US20070197460A1 - Rnai inhibition of influenza virus replication - Google Patents

Abstract

The invention relates to compositions and methods for modulating the expression of influenza viral genes, and more particularly to the downregulation of influenza viral genes by chemically modified oligonucleotides.

Description

CROSS-REFERENCE TO RELATED APPLICATIONS
• This application claims priority to U.S. Application Ser. No. 60/732,243, filed Nov. 1, 2005; U.S. Ser. No. 60/748,317, filed Dec. 7, 2005; and U.S. Ser. No. 60/799,000, filed May 9, 2006. The contents of each of these provisional applications are hereby incorporated by reference in their entirety.
TECHNICAL FIELD
• The invention relates to the field of influenza viral therapy and compositions and methods for modulating viral replication, and more particularly to the down-regulation of a gene(s) of an influenza virus by oligonucleotides via RNA interference which are administered locally to the lungs and nasal passage via inhalation/intranasal administration, or are administered systemically, e.g. by via intravenous injection.
BACKGROUND
• RNA interference or “RNAi” is a term initially coined by Fire and co-workers to describe the observation that double-stranded RNA (dsRNA) can block gene expression when it is introduced into worms (Fire et al., Nature 391:806-811, 1998). Short dsRNA directs gene-specific, post-transcriptional silencing in many organisms, including vertebrates, and has provided a new tool for studying gene function. This technology has been reviewed numerous times recently, see, for example Novina, C. D:, and Sharp, P., Nature 2004, 430:161, and Sandy, P., et al., Biotechniques 2005, 39:215, hereby incorporated by reference.
• Influenza is one of the most widely spread infections worldwide. It can be deadly: an estimated 20 to 40 million people died during the 1918 influenza A virus pandemic. In the United States between 20 and 40 thousand people die from influenza A virus infection or its complications each year. During epidemics the number of influenza related hospitalizations may reach over 300,000 in a single winter season.
• Several properties contribute to the epidemiological success of influenza virus. First, it is spread easily from person to person by aerosol (droplet infection). Second, small changes in influenza virus antigens are frequent (antigenic drift) so that the virus readily escapes protective immunity induced by a previous exposure to a different variant of the virus. Third, new strains of influenza virus can be easily generated by reassortment or mixing of genetic material between different strains (antigenic shift). In the case of influenza A virus, such mixing can occur between subtypes or strains that affect different species. The 1918 pandemic is thought to have been caused by a hybrid strain of virus derived from reassortment between a swine and a human influenza A virus. At present, there is a spreading concern about the potential emergence of novel influenza strains infective to humans, particularly from avian influenza variants, and more particularly from strain H5N1, by mixing in humans concurrently exposed to human and avian influenza virus. The close contact between agricultural birds and their human breeders familiar in most asian societies has experts convinced that it is not a question of whether but only when such a mixed strain will arise. A world-wide pandemic could swiftly ensue, with even graver consequences than in 1918.
• Despite intensive efforts, there is still no effective therapy for influenza virus infection and existing vaccines are limited in value in part because of the properties of antigenic shift and drift described above. For these reasons, global surveillance of influenza A virus has been underway for many years, and the National Institutes of Health designates it as one of the top priority pathogens for biodefense. Although current vaccines based upon inactivated virus are able to prevent illness in approximately 70-80% of healthy individuals under age 65, this percentage is far lower in the elderly or immunocompromised. In addition, the expense and potential side effects associated with vaccine administration make this approach less than optimal. Although the antiviral drugs currently approved in the United States for treatment and/or prophylaxis of influenza are helpful, their use is limited due to concerns about side effects, compliance, and possible emergence of resistant strains.
• US patent application 20040242518 and corresponding WO 04/028471, both filed Sep. 29, 2003, propose a limited number of RNAi agents for the treatment of influenza. Their efficacy in humans is not disclosed.
• Therefore, there still remains a need for the development of effective therapies for the treatment and prevention of influenza infection in humans and animals, and particularly for therapies with high efficiency that allow the targeting of a broad range of influenza subtypes. One prerequisite for high efficiency is that the active ingredient is not degraded quickly in a physiological environment.
SUMMARY
• The present invention is based on the in vitro and in vivo demonstration that influenza virus infection can be inhibited through intranasal administration of iRNA agents, as well as by parenteral administration of such agents and the identification of potent iRNA agents from the MP, NP, PB1, PB2, or PA gene of influenza virus that can reduce RNA levels of several subtypes of influenza virus. Based on these findings, the present invention provides specific compositions and methods that are useful in reducing influenza virus mRNA levels, influenza virus protein levels and influenza virus viral titers in a subject, e.g., a mammal, such as a human.
• The present invention specifically provides iRNA agents consisting of, consisting essentially of or comprising at least 15 or more contiguous nucleotides of one of the genes of influenza virus, particularly the MP, NP, PB1, PB2 and PA genes of influenza virus, and more particularly agents that comprising 15 or more contiguous nucleotides from one of the sequences provided in Tables 1A-1H. The iRNA agent preferably comprises less than 30 nucleotides per strand, e.g., 21-23 nucleotides, such as those provided in Tables 1A-1H. The double stranded iRNA agent can either have blunt ends or more preferably have overhangs of 1-4 nucleotides from one or both 3′ ends of the agent.
• Further, the iRNA agent can either contain only naturally occurring ribonucleotide subunits, or can be synthesized so as to contain one or more modifications to the sugar or base of one or more of the ribonucleotide subunits that is included in the agent. The iRNA agent can be further modified so as to be attached to a ligand that is selected to improve stability, distribution or cellular uptake of the agent, e.g. cholesterol. The iRNA agents can further be in isolated form or can be part of a pharmaceutical composition used for the methods described herein, particularly as a pharmaceutical composition formulated for delivery to the lungs or nasal passage or formulated for parental administration. The pharmaceutical compositions can contain one or more iRNA agents, and in some embodiments, will contain two or more iRNA agents, each one directed to a different segment of a influenza virus gene or a different influenza virus gene.
• One aspect of the present invention relates to a double-stranded oligonucleotide comprising at least one non-natural nucleobase. In certain embodiments, the non-natural nucleobase is difluorotolyl, nitroindolyl, nitropyrrolyl, or nitroimidazolyl. In a preferred embodiment, the non-natural nucleobase is difluorotolyl. In certain embodiments, only one of the two oligonucleotide strands comprising the double-stranded oligonucleotide contains a non-natural nucleobase. In certain embodiments, both of the oligonucleotide strands comprising the double-stranded oligonucleotide independently contain a non-natural nucleobase.
• The present invention further provides methods for reducing the level of influenza virus viral RNA in a cell. Such methods comprise the step of administering one of the iRNA agents of the present invention to a subject as further described below. The present methods utilize the cellular mechanisms involved in RNA interference to selectively degrade the viral RNA in a cell and are comprised of the step of contacting a cell with one of the antiviral iRNA agents of the present invention. Such methods can be performed directly on a cell or can be performed on a mammalian subject by administering to a subject one of the iRNA agents/pharmaceutical compositions of the present invention. Reduction of viral RNA in a cells results in a reduction in the amount of viral protein produced, and in an organism, results in a decrease in replicating viral titer (as shown in the Examples).
• The methods and compositions of the invention, e.g., the methods and iRNA agent compositions can be used with any dosage and/or formulation described herein, as well as with any route of administration described herein. Particularly important is the showing herein of intranasal administration of an iRNA agent and its ability to inhibit viral replication in respiratory tissues.
• The details of one or more embodiments of the invention are set forth in the accompanying drawings and the description below. Other features, objects, and advantages of the invention will be apparent from this description, the drawings, and from the claims. This application incorporates all cited references, patents, and patent applications by references in their entirety for all purposes.
BRIEF DESCRIPTION OF DRAWINGS
• FIGS. 1A-1I: Dose-response curves for the inhibition of target gene expression for selected RNAi agents. The respective target gene was recombinantly cloned into Cos-7 cells in a plasmid resulting in expression of an mRNA encoding the target gene and Renilla luciferase, the cells treated with the RNAi agent, and Renilla luciferase was quantified. Cells were treated with the RNAi agent at concentrations of 100 nM, 25 nM, 6.3 nM, 1.6 nM, 400 pM, 100 pM, 24 pM, 6 pM, 1.5 pM, and 380 fM, and IC₅₀ values determined by parametrized curve fitting using the program XLfit.
DETAILED DESCRIPTION
• The term “influenza virus” is used here to refer to any strain of influenza virus that is capable of causing disease in an animal or human subject, or that is an interesting candidate for experimental analysis. Influenza viruses are described in Fields, B., et al., Fields' Virology, 4^th ed. 2001, Lippincott Williams and Wilkins; Philadelphia, ISBN: 0781718325. In particular, the term encompasses any strain of influenza A virus that is capable of causing disease in an animal or human subject, or that is an interesting candidate for experimental analysis. A large number of influenza A isolates have been partially or completely sequenced. Table 6 presents merely a partial list of complete sequences for influenza A genome segments that have been deposited in a public database (The influenza Sequence Database (ISD), see Macken, C., Lu, H., Goodman, J., & Boykin, L., “The value of a database in surveillance and vaccine selection.” in Options for the Control of influenza IV. A. D. M. E. Osterhaus, N. Cox & A. W. Hampson (Eds.) 2001, Elsevier Science, Amsterdam, pp 103-106). This database also contains complete sequences for influenza B and C genome segments. The database is available on the World Wide Web and includes a convenient search engine that allows the user to search by genome segment, by species infected by the virus, and by year of isolation. Influenza sequences are also available on Genbank. Sequences of influenza genes are therefore readily available to, or determinable by, those of ordinary skill in the art.
• For ease of exposition the term “nucleotide” or “ribonucleotide” is sometimes used herein in reference to one or more monomeric subunits of an RNA agent. It will be understood that the usage of the term “ribonucleotide” or “nucleotide” herein can, in the case of a modified RNA or nucleotide surrogate, also refer to a modified nucleotide, or surrogate replacement moiety, as further described below, at one or more positions.
• An “RNA agent” as used herein, is an unmodified RNA, modified RNA, or nucleoside surrogate, each of which is described herein or is well known in the RNA synthetic art. While numerous modified RNAs and nucleoside surrogates are described, preferred examples include those which have greater resistance to nuclease degradation than do unmodified RNAs. Preferred examples include those that have a 2′ sugar modification, a modification in a single strand overhang, preferably a 3′ single strand overhang, or, particularly if single stranded, a 5′-modification which includes one or more phosphate groups or one or more analogs of a phosphate group.
• An “iRNA agent” (abbreviation for “interfering RNA agent”) as used herein, is an RNA agent, which can downregulate the expression of a target gene, e.g., influenza virus. While not wishing to be bound by theory, an iRNA agent may act by one or more of a number of mechanisms, including post-transcriptional cleavage of a target mRNA sometimes referred to in the art as RNAi, or pre-transcriptional or pre-translational mechanisms. An iRNA agent can be a double stranded iRNA agent.
• A “ds iRNA agent” (abbreviation for “double stranded iRNA agent”), as used herein, is an iRNA agent which includes more than one, and preferably two, strands in which interstrand hybridization can form a region of duplex structure. A “strand” herein refers to a contigouous sequence of nucleotides (including non-naturally occurring or modified nucleotides). The two or more strands may be, or each form a part of, separate molecules, or they may be covalently interconnected, e.g., by a linker, e.g., a polyethyleneglycol linker, to form one molecule. At least one strand can include a region which is sufficiently complementary to a target RNA. Such strand is termed the “antisense strand.” A second strand of the dsRNA agent, which comprises a region complementary to the antisense strand, is termed the “sense strand.” However, a ds iRNA agent can also be formed from a single RNA molecule which is at least partly self-complementary, forming, e.g., a hairpin or panhandle structure, including a duplex region. The latter are herein referred to as short hairpin RNAs or shRNAs. In such case, the term “strand” refers to one of the regions of the RNA molecule that is complementary to another region of the same RNA molecule.
• Although, in mammalian cells, long ds iRNA agents can induce the interferon response which is frequently deleterious, short ds iRNA agents do not trigger the interferon response, at least not to an extent that is deleterious to the cell and/or host (Manche et al., Mol. Cell. Biol. 12:5238, 1992; Lee et al., Virology 199:491, 1994; Castelli et al., J. Exp. Med. 186:967, 1997; Zheng et al, RNA 10:1934, 2004; Heidel et al., “Lack of interferon response in animals to naked siRNAs” Nature Biotechn. advance online publication doi:10.1038/nbt1038, Nov. 21, 2004). The iRNA agents of the present invention include molecules which are sufficiently short that they do not trigger a deleterious non-specific interferon response in normal mammalian cells. Thus, the administration of a composition including an iRNA agent (e.g., formulated as described herein) to a subject can be used to decreased expression of the influenza virus genes in influenza virus expressing cells in the subject, while circumventing an interferon response. Molecules that are short enough that they do not trigger a deleterious interferon response are termed siRNA agents or siRNAs herein. “siRNA agent” or “siRNA” as used herein, refers to an iRNA agent, e.g., a ds iRNA agent, that is sufficiently short that it does not induce a deleterious interferon response in a mammalian, and particularly a human, cell, e.g., it has a duplexed region of less than 60 but preferably less than 50, 40, or 30 nucleotide pairs.
• The isolated iRNA agents described herein, including ds iRNA agents and siRNA agents, can mediate the decreased expression of a influenza virus nucleic acid, e.g., by RNA degradation. For convenience, such RNA is also referred to herein as the RNA to be silenced. Such a nucleic acid is also referred to as a target gene. Preferably, the RNA to be silenced is a gene product of a influenza virus gene that is part of an influenzy virus strain that is pathogenic to humans.
• As used herein, the phrase “mediates RNAi” refers to the ability of an agent to silence, in a sequence specific manner, a target gene. “Silencing a target gene” means the process whereby a cell containing and/or expressing a certain product of the target gene when not in contact with the agent, will contain and/or express at least 10%, 20%, 30%, 40%, 50%, 60%, 70%, 80%, or 90% less of such gene product when contacted with the agent, as compared to a similar cell which has not been contacted with the agent. Such product of the target gene can, for example, be a messenger RNA (mRNA), a protein, or a regulatory element.
• As used herein, the term “complementary” is used to indicate a sufficient degree of complementarity such that stable and specific binding occurs between a compound of the invention and a target RNA molecule, e.g., a influenza virus mRNA. Specific binding requires a sufficient degree of complementarity to avoid non-specific binding of the oligomeric compound to non-target sequences under conditions in which specific binding is desired, i.e., under physiological conditions in the case of in vivo assays or therapeutic treatment, or in the case of in vitro assays, under conditions in which the assays are performed. The non-target sequences typically differ from the target sequences by at least 2, 3 or 4 nucleotides.
• As used herein, an iRNA agent is “sufficiently complementary” to a target RNA, e.g., a target mRNA (e.g., a target influenza virus mRNA) if the iRNA agent reduces the production of a protein encoded by the target RNA in a cell. The iRNA agent may also be “exactly complementary” to the target RNA, e.g., the target RNA and the iRNA agent anneal, preferably to form a hybrid made exclusively of Watson-Crick basepairs in the region of exact complementarity. A “sufficiently complementary” iRNA agent can include an internal region (e.g., of at least 10 nucleotides) that is exactly complementary to a target influenza virus RNA. Moreover, in some embodiments, the iRNA agent specifically discriminates a single-nucleotide difference. In this case, the iRNA agent only mediates RNAi if exact complementarity is found in the region (e.g., within 7 nucleotides of) the single-nucleotide difference. Preferred iRNA agents will be based on or consist of or comprise the sense and antisense sequences provided in Table 1A-1H.
• As used herein, “essentially identical” when used referring to a first nucleotide sequence in comparison to a second nucleotide sequence means that the first nucleotide sequence is identical to the second nucleotide sequence except for up to one, two or three nucleotide substitutions (e.g., adenosine replaced by uracil). “Essentially retaining the ability to inhibit influenza virus expression in cultured human influenza virus expressing cells,” as used herein referring to an iRNA agent not identical to but derived from one of the iRNA agents of Tables 1A-1H by deletion, addition or substitution of nucleotides, means that the derived iRNA agent possesses an inhibitory activity not less than 20% of the inhibitory activity of the iRNA agent of Tables 1A-1H from which it was derived. For example, an iRNA agent derived from an iRNA agent of Tables 1A-1H which lowers the amount of influenza virus mRNA present in cultured human cells infected with influenza virus by 70% may itself lower the amount of influenza virus mRNA present in cultured human cells infected with influenza virus by at least 50% in order to be considered as essentially retaining the ability to inhibit influenza virus replication in cultured human cells infected with influenza virus. Optionally, an iRNA agent of the invention may lower the amount of influenza virus mRNA present in cultured human cells infected with influenza virus by at least 50%.
• As used herein, a “subject” refers to a mammalian organism undergoing treatment for a disorder mediated by infection with an influenza virus. The subject can be any mammal, such as a cow, horse, mouse, rat, dog, pig, goat, or a primate. In the preferred embodiment, the subject is a human.
• Influenza Viral Characteristics
• Influenza viruses are enveloped, negative-stranded RNA viruses of the Orthomyxoviridae family. They are classified as influenza types A, B, and C, of which influenza A is the most pathogenic and is believed to be the only type able to undergo reassortment with animal strains. Influenza types A, B, and C can be distinguished by differences in their nucleoprotein and matrix proteins. As discussed further below, influenza A subtypes are defined by variation in their hemagglutinin (HA) and neuraminidase (NA) genes and usually distinguished by antibodies that bind to the corresponding proteins.
• The influenza A viral genome consists of ten genes distributed in eight RNA segments. The genes encode 10 proteins: the envelope glycoproteins hemagglutinin (HA) and neuraminidase (NA); matrix protein (referred to as M1 or MP herein); nucleoprotein (NP); three polymerases (PB1, PB2, and PA) which are components of an RNA-dependent RNA transcriptase also referred to as a polymerase or polymerase complex herein; ion channel protein (M2), and nonstructural proteins (NS1 and NS2). See Julkunen, I., et al., Cytokine and Growth Factor Reviews, 12: 171-180, 2001 for further details regarding the influenza A virus and its molecular pathogenesis. See also Fields, B., et al., Fields' Virology, 4.sup.th. ed., Philadelphia: Lippincott Williams and Wilkins; ISBN: 0781718325, 2001. The organization of the influenza B viral genome is extremely similar to that of influenza A whereas the influenza C viral genome contains seven RNA segments and lacks the NA gene.
• Influenza A virus classification is based on the hemagglutinin (H1-H15) and neuraminidase (N1-N9) genes. World Health Organization (WHO) nomenclature defines each virus strain by its animal host of origin (specified unless human), geographical origin, strain number, year of isolation, and antigenic description of HA and NA. For example, A/Puerto Rico/8/34 (H1N1) designates strain A, isolate 8, that arose in humans in Puerto Rico in 1934 and has antigenic subtypes 1 of HA and NA. As another example, A/Chicken/Hong Kong/258/97 (H5N1) designates strain A, isolate 258, that arose in chickens in Hong Kong in 1997 and has antigenic subtype 5 of HA and 1 of NA. Human epidemics have been caused by viruses with HA types H1, H2, and H3 and NA types N1 and N2.
• As mentioned above, genetic variation occurs by two primary mechanisms in influenza virus A. Antigenic drift occurs via point mutations, which often occur at antigenically significant positions due to selective pressure from host immune responses, and antigenic shift (also referred to as reassortment), involving substitution of a whole viral genome segment of one subtype by another. Many different types of animal species including humans, swine, birds, horses, aquatic mammals, and others, may become infected with influenza A viruses. Some influenza A viruses are restricted to a particular species and will not normally infect a different species. However, some influenza A viruses may infect several different animal species, principally birds (particularly migratory water fowl), swine, and humans. This capacity is considered to be responsible for major antigenic shifts in influenza A virus. For example, suppose a swine becomes infected with an influenza A virus from a human and at the same time becomes infected with a different influenza A virus from a duck. When the two different viruses reproduce in the swine cells, the genes of the human strain and duck strain may “mix,” resulting in a new virus with a unique combination of RNA segments. This process is called genetic reassortment. (Note that this type of genetic reassortment is distinct from the exchange of genetic information that occurs between chromosomes during meiosis.)
• Like other viruses and certain bacterial species, influenza viruses replicate intracellularly. Influenza A viruses replicate in epithelial cells of the upper respiratory tract. However, monocytes/macrophages and other white blood cells can also be infected. Numerous other cell types with cell surface glycoproteins containing sialic acid are susceptible to infection in vitro since the virus uses these molecules as a receptor.
• Design and Selection of iRNA Agents
• As used herein, “disorders associated with influenza virus expression” refers to any biological or pathological state that (1) is mediated at least in part by the presence of an influenza virus and (2) whose outcome can be affected by reducing the level of the influenza virus present. Specific disorders associated with influenza virus expression are noted below.
• The present invention is based on the design, synthesis and generation of iRNA agents that target viral genes of influenza virus, and the demonstration of silencing of a viral gene in vitro in cultured cells after incubation with an iRNA agent, and the resulting protective effect towards viral infection.
• An iRNA agent can be rationally designed based on sequence information and desired characteristics. For example, an iRNA agent can be designed according to the relative melting temperature of the candidate duplex. Generally, the duplex should have a lower melting temperature at the 5′ end of the antisense strand than at the 3′ end of the antisense strand.
• The present invention provides compositions containing siRNA(s) and/or shRNA(s) targeted to one or more influenza virus transcripts. As the description of the influenza virus replicative cycle presented above demonstrates, various types of viral RNA transcripts (primary and secondary vRNA, primary and secondary viral mRNA, and viral cRNA) are present within cells infected with influenza virus and play important roles in the viral life cycle. Any of these transcripts are appropriate targets for siRNA mediated inhibition by either a direct or an indirect mechanism in accordance with the present invention. siRNAs and shRNAs that target any viral mRNA transcript will specifically reduce the level of the transcript itself in a direct manner, i.e., by causing degradation of the transcript. In addition, as discussed below, siRNAs and shRNAs that target certain viral transcripts (e.g., MP, PA, PB1) will indirectly cause reduction in the levels of viral transcripts to which they are not specifically targeted. In situations where alternative splicing is possible, as for the mRNA that encodes MP and M2 and the mRNA that encodes NS1 and NS2, the unspliced transcript or the spliced transcript may serve as a target transcript.
• Potential viral transcripts that may serve as a target for RNAi based therapy according to the present invention include, for example, 1) any influenza virus genomic segment; 2) transcripts that encode any viral proteins including transcripts encoding the proteins PB1, PB2, PA, NP, NS1, NS2, MP, M2, HA, or NA. As will be appreciated, transcripts may be targeted in their vRNA, cRNA, and/or mRNA form(s) by a single siRNA or shRNA. However, it may be that viral mRNA is the sole or primary target of RNAi as suggested by Ge et al., WO 04/028471.
• For any particular gene target that is selected, the design of siRNAs or shRNAs for use in accordance with the present invention will preferably follow certain guidelines. In general, it is desirable to target sequences that are specific to the virus (as compared with the host), and that, preferably, are important or essential for viral function. Although certain viral genes, particularly those encoding HA and NA are characterized by a high mutation rate and are capable of tolerating mutations, certain regions and/or sequences tend to be conserved. According to certain embodiments of the invention such sequences may be particularly appropriate targets. As described further below, such conserved regions can be identified, for example, through review of the literature and/or comparisons of influenza gene sequences, a large number of which are publicly available. Also, in many cases, the agent that is delivered to a cell according to the present invention may undergo one or more processing steps before becoming an active suppressing agent (see below for further discussion); in such cases, those of ordinary skill in the art will appreciate that the relevant agent will preferably be designed to include sequences that may be necessary for its processing. One aspect of the present invention is the recognition that when multiple strains, subtypes, etc. (referred to collectively as variants), of an infectious agent exist, whose genomes vary in sequence, it will often be desirable to select and/or design siRNAs and shRNAs that target regions that are highly conserved among different variants. In particular, by comparing a sufficient number of sequences and selecting highly conserved regions, it will be possible to target multiple variants with a single siRNA whose duplex portion includes such a highly conserved region. Generally such regions should be of sufficient length to include the entire duplex portion of the siRNA (e.g., 19 nucleotides) and, optionally, one or more 3′ overhangs, though regions shorter than the full length of the duplex can also be used (e.g., 15, 16, 17, or 18 nucleotides). According to certain embodiments of the invention a region is highly conserved among multiple variants if it is identical among the variants. According to certain embodiments of the invention a region (of whatever length is to be included in the duplex portion of the siRNA, e.g., 15, 16, 17, 18, or, preferably, 19 nucleotides) is highly conserved if it differs by at most one nucleotide (i.e., 0 or 1 nucleotide) among the variants. According to certain embodiments of the invention such a region is highly conserved among multiple variants if it differs by at most two nucleotides (i.e., 0, 1, or 2 nucleotides) among the variants. According to certain embodiments of the invention a region is highly conserved among multiple variants if it differs by at most three nucleotides or (i.e., 0, 1, 2, or 3 nucleotides) among the variants. According to certain embodiments of the invention an siRNA includes a duplex portion that targets a region that is highly conserved among at least 5 variants, at least variants, at least 15 variants, at least 20 variants, at least 25 variants, at least 30 variants, at least 40 variants, or at least 50 or more variants.
• In order to determine whether a region is highly conserved among a set of multiple variants, the following procedure may be used. One member of the set of sequences is selected as the base sequence, i.e., the sequence to which other sequences are to be compared. Typically the length of the base sequence will be the length desired for the duplex portion of the siRNA, e.g, 15, 16, 17, 18, or, preferably 19 nucleotides. According to different embodiments of the invention the base sequence may be either one of the sequences in the set being compared or may be a consensus sequence derived, e.g., by determining for each position the most frequently found nucleotide at that position among the sequences in the set.
• Having selected a base sequence, the sequence of each member of the set of multiple variants is compared with the base sequence. The number of differences between the base sequence and any member of the set of multiple variants over a region of the sequence is used to determine whether the base sequence and that member are highly conserved over the particular region of interest. As noted above, in various embodiments of the invention if the number of sequence differences between two regions is either 0; 0 or 1, 0, 1, or 2; or 0, 1, 2, or 3, the regions are considered highly conserved. At the positions where differences occur, the siRNA sequence may be selected to be identical to the base sequence or to one of the other sequences. Generally the nucleotide present in the base sequence will be selected. However in certain embodiments of the invention, particularly if a nucleotide present at a particular position in a second sequence in the set being compared is found in more of the sequences being compared than the nucleotide in the base sequence, then the siRNA sequence may be selected to be identical to the second sequence. In addition according to certain embodiments of the invention, if the consensus nucleotide (most commonly occurring nucleotide) at the position where the difference occurs is different to that found in the base sequence, the consensus nucleotide may be used. Note that this may result in a sequence that is not identical to any of the sequences being compared (as may the use of a consensus sequence as the base sequence).
• The inventors have found that a significant proportion of the sequences selected using the design parameters described hereinbelow (see Example 1) prove to be efficient in suppressing viral replication when included in an siRNA or shRNA and tested as described below.
• Based on the results shown herein, the present invention provides iRNA agents that reduce influenza virus replication in cultured cells infected with influenza virus and in a subject, e.g. a mammalian, for example a human. Tables 1A-1H provide exemplary iRNA agents targeting influenza virus. Table 1A, C, D, and E list siRNAs that do not comprise nucleotide modifications except for one phosphorothioate linkage between the 3′-terminal and the penultimate thymidines. Table 1B and H list siRNAs wherein all nucleotides comprising pyrimidine bases are 2′-O-methyl-modified nucleotides in the sense strand, and all uridines in a sequence context of 5′-ua-3′ as well as all cytidines in a sequence context of or 5′-ca-3′ are 2′-O-methyl-modified nucleotides in the antisense strand, except for the iRNA agents with duplex identified AL-DP-2295, AL-DP-2301, and AL-DP-2302, in which all uridines in a sequence context of 5′-ug-3′ are 2′-O-methyl-modified nucleotides in the antisense strand. These latter siRNAs had no occurrences of the sequence motifs 5′-ua-3′ or 5′-ca-3′, and an analysis of degradation fragments after incubation of these agents in mouse serum revealed that the sequence motif 5′-ug-3′ was the primary point of endonucleolytic attack.
• Based on these results, the invention specifically provides an iRNA agent that includes a sense strand having at least 15 contiguous nucleotides of the sense strand sequences of the agents provided in Tables 1A-1H, and an antisense strand having at least 15 contiguous nucleotides of the antisense sequences of the agents provided in Tables 1A-1H.
• The iRNA agents shown in Tables 1A-1H are composed of two strands of 19 nucleotides in length which are complementary or identical to the target sequence, plus a 3′-TT overhang. The present invention provides agents that comprise at least 15, or at least 16, 17, or 18, or 19 contiguous nucleotides from these sequences. However, while these lengths may potentially be optimal, the iRNA agents are not meant to be limited to these lengths. The skilled person is well aware that shorter or longer iRNA agents may be similarly effective, since, within certain length ranges, the efficacy is rather a function of the nucleotide sequence than strand length. For example, Yang, et al., PNAS 99:9942-9947 (2002), demonstrated similar efficacies for iRNA agents of lengths between 21 and 30 base pairs. Others have shown effective silencing of genes by iRNA agents down to a length of approx. 15 base pairs (Byrom, et al., “Inducing RNAi with siRNA Cocktails Generated by RNase III” Tech Notes 10(1), Ambion, Inc., Austin, Tex.).
• Therefore, it is possible and contemplated by the instant invention to select from the sequences provided in Tables 1A-1H a partial sequence of between 15 to 19 nucleotides for the generation of an iRNA agent derived from one of the sequences provided in Tables 1A-1H. Alternatively, one may add one or several nucleotides to one of the sequences provided in Tables 1A-1H, or an agent comprising 15 contiguous nucleotides from one of these agents, preferably, but not necessarily, in such a fashion that the added nucleotides are complementary to the respective sequence of the target gene, e.g., an influenza virus gene. For example, the first 15 nucleotides from one of the agents can be combined with the 8 nucleotides found 5′ to these sequence in the influenza virus mRNA to obtain an agent with 23 nucleotides in the sense and antisense strands. All such derived iRNA agents are included in the iRNA agents of the present invention, provided they essentially retain the ability to inhibit influenza virus replication in cultured human cells infected with influenza virus.

  TABLE 1A
  Exemplary iRNA agents for targeting influenza virus having 80% target coverage (criterium 1,
  see example 1) and 79.9% target efficiency (criterium 2, see example 1), and having an off
  target score of less than 16.8 (see example 1)

  							ELISA	ELISA	Plasmid
  					Target	%	(MDCK	(Vero	expres-
  		SEQ		SEQ	influ-	remaining	cells),	cells),	sion,
  Duplex	Sense strand sequence	ID	Antisense strand	ID	enza	infec-	% inhi-	% inhi-	% inhi-
  identifier	(5′-3′)	NO:	sequence (5′-3′)	NO	gene	tivity1	bition2	bition3	bition4

  AL-DP-2241	uggaagcaauggcuuuccuTT	1	aggaaagccauugcuuccaTT	2	PB1		3	−31
  AL-DP-2242	ggcaccaaacgaucuuaugTT	3	cauaagaucguuuggugccTT	4	NP		−10	28	63
  AL-DP-2243	aggcaccaaacgaucuuauTT	5	auaagaucguuuggugccuTT	6	NP		−34	15	51
  AL-DE-2244	gcaccaaacgaucuuaugaTT	7	ucauaagaucguuuggugcTT	8	NP	<50	−26	74	76
  AL-DE-2245	cuucuaaccgaggucgaaaTT	9	uuucgaccucgguuagaagTT	10	MP		−20	−72
  AL-DP-2246	gucgaaacguacguucucuTT	11	agagaacguacguuucgacTT	12	MP		−2	−70
  AL-DE-2247	cucaaagccgagaucgcgcTT	13	gcgcgaucucggcuuugagTT	14	MP		−4	−95
  AL-DE-2248	uucuaaccgaggucgaaacTT	15	guuucgaccucgguuagaaTT	16	MP		−23	−37
  AL-DE-2249	ucuaaccgaggucgaaacgTT	17	cguuucgaccucgguuagaTT	18	MP		−1	18
  AL-DE-2250	ucgaaacguacguucucucTT	19	gagagaacguacguuucgaTT	20	MP		−27	15
  AL-DE-2251	cgaaacguacguucucucuTT	21	agagagaacguacguuucgTT	22	MP		−16	12
  AL-DE-2252	aaacguacguucucucuauTT	23	auagagagaacguacguuuTT	24	MP		−21	−24
  AL-DE-2253	cccccucaaagccgagaucTT	25	gaucucggcuuugagggggTT	26	MP		−14	6
  AL-DE-2254	cccucaaagccgagaucgcTT	27	gcgaucucggcuuugagggTT	28	MP		−22	−24
  AL-DE-2255	ccucaaagccgagaucgcgTT	29	cgcgaucucggcuuugaggTT	30	MP		−11	−14
  AL-DE-2256	acaagaccaauccugucacTT	31	gugacaggauuggucuuguTT	32	MP		17	−22
  AL-DE-2257	agcgaggacugcagcguagTT	33	cuacgcugcaguccucgcuTT	34	MP		1	−124
  AL-DE-2258	cgaggacugcagcguagacTT	35	gucuacgcugcaguccucgTT	36	MP		26	−37
  AL-DE-2259	uugcacuugauauuguggaTT	37	uccacaauaucaagugcaaTT	38	MP		12	−18
  AL-DE-2260	ugcacuugauauuguggauTT	39	auccacaauaucaagugcaTT	40	MP		−5	−76
  AL-DE-2261	auacgguuugaaaagagggTT	41	cccucuuuucaaaccguauTT	42	MP		−1	5
  AL-DE-2262	uacgguuugaaaagagggcTT	43	gcccucuuuucaaaccguaTT	44	MP		−6	−6
  AL-DE-2263	acgguuugaaaagagggccTT	45	ggcccucuuuucaaaccguTT	46	MP		3	−22
  AL-DE-2264	cgguuugaaaagagggccuTT	47	aggcccucuuuucaaaccgTT	48	MP		4	1
  AL-DE-2265	cuaaccgaggucgaaacguTT	49	acguuucgaccucgguuagTT	50	MP		13	−52
  AL-DE-2266	uaaccgaggucgaaacguaTT	51	uacguuucgaccucgguuaTT	52	MP		27	−107
  AL-DE-2267	aaccgaggucgaaacguacTT	53	guacguuucgaccucgguuTT	54	MP	<25	42	−73
  AL-DE-2268	accgaggucgaaacguacgTT	55	cguacguuucgaccucgguTT	56	MP		−16	−18
  AL-DE-2269	ccgaggucgaaacguacguTT	57	acguacguuucgaccucggTT	58	MP		−21	−43
  AL-DE-2270	cgaggucgaaacguacguuTT	59	aacguacguuucgaccucgTT	60	MP		−6	−25
  AL-DE-2271	gaggucgaaacguacguucTT	61	gaacguacguuucgaccucTT	62	MP		−29	−29
  AL-DE-2272	aggucgaaacguacguucuTT	63	agaacguacguuucgaccuTT	64	MP		−23	−59
  AL-DE-2273	ggucgaaacguacguucucTT	65	gagaacguacguuucgaccTT	66	MP		−9	−36
  AL-DE-2274	gcuaaagacaagaccaaucTT	67	gauuggucuugucuuuagcTT	68	MP		−24	−17
  AL-DE-2275	aauccugucaccucugacuTT	69	agucagaggugacaggauuTT	70	MP		−33	−36
  AL-DE-2276	uccugucaccucugacuaaTT	71	uuagucagaggugacaggaTT	72	MP	30%	−20	−10
  AL-DE-2277	cacgcucaccgugcccaguTT	73	acugggcacggugagcgugTT	74	MP		−38	−32
  AL-DE-2278	acgcucaccgugcccagugTT	75	cacugggcacggugagcguTT	76	MP		−26	−17
  AL-DE-2279	cgcucaccgugcccagugaTT	77	ucacugggcacggugagcgTT	78	MP		−36	−7
  AL-DE-2280	gcucaccgugcccagugagTT	79	cucacugggcacggugagcTT	80	MP		−37	−34
  AL-DE-2281	caccgugcccagugagcgaTT	81	ucgcucacugggcacggugTT	82	MP		−46	−52
  AL-DE-2282	gagcgaggacugcagcguaTT	83	uacgcugcaguccucgcucTT	84	MP		−31	−62
  AL-DE-2283	uauuguggauucuugaucgTT	85	cgaucaagaauccacaauaTT	86	MP	45%	−52	−26
  AL-DE-2284	uuguggauucuugaucgucTT	87	gacgaucaagaauccacaaTT	88	MP	61%	39	−60
  AL-DE-2285	uguggauucuugaucgucuTT	89	agacgaucaagaauccacaTT	90	MP	41%	3	−49
  AL-DE-2286	guggauucuugaucgucuuTT	91	aagacgaucaagaauccacTT	92	MP	36%	9	−50
  AL-DE-2287	ucaaaugcauuuaucgucgTT	93	cgacgauaaaugcauuugaTT	94	MP	38%	−17	−11
  AL-DE-2288	caaaugcauuuaucgucgcTT	95	gcgacgauaaaugcauuugTT	96	MP	39%	23	−58
  1in vitro plaque forming assay in MCDK cells as described in Example 3.1;
  2in in vitro ELISA assay in MCDK cells as described in Example 3.2:
  3in in vitro ELISA assay in MCDK cells as described in Example 3.2;
  4in in vitro ELISA assay in MCDK cells as described in Example 3.2; negative values indicate that target gene expression was enhanced in treated cells compared to controls

• TABLE 1B
  Exemplary iRNA agents for targeting influenza virus derived from agents listed in Table 1A
  by stabilization towards nucleolytic degradation by nucleotide modifications

  	Corre-					Target
  	sponding		SEQ		SEQ	influ-
  Duplex	unmodified	Sense strand sequence	ID	Antisense strand	ID	enza
  identifier	duplex1	(5′-3′)	NO:	sequence (5′-3′)	NO:	gene

  AL-DP-2289	AL-DP-2241	umggaagcmaaumggcmumumumcmcmumTT	97	aggaaagccmauugcuuccmaTT	98	PB1
  AL-DP-2290	AL-DP-2242	ggcmacmcmaaacmgaumcmumumaumgTT	99	cmaumaagaucguuuggugccTT	100	NP
  AL-DP-2291	AL-DP-2243	aggcmacmcmaaacmgaumcmumumaumTT	101	aumaagaucguuuggugccuTT	102	NP
  AL-DP-2292	AL-DP-2244	gcmacmcmaaacmgaumcmumumaumgaTT	103	ucmaumaagaucguuuggugcTT	104	NP
  AL-DP-2293	AL-DP-2245	cmumumcmumaacmcmgaggumcmgaaaTT	105	uuucgaccucgguumagaagTT	106	MP
  AL-DP-2294	AL-DP-2246	gumcmgaaacmgumacmgumumcmumcmumTT	107	agagaacgumacguuucgacTT	108	MP
  AL-DP-2295	AL-DP-2247	cmumcmaaagcmcmgagaumcmgcmgcmTT	109	gcgcgaucucggcuuumgagTT	110	MP
  AL-DP-2296	AL-DP-2248	umumcmumaacmcmgaggumcmgaaacmTT	111	guuucgaccucgguumagaaTT	112	MP
  AL-DP-2297	AL-DP-2249	umcmumaacmcmgaggumcmgaaacmgTT	113	cguuucgaccucgguumagaTT	114	MP
  AL-DP-2298	AL-DP-2250	umcmgaaacmgumacmgumumcmumcmumcmTT	115	gagagaacgumacguuucgaTT	116	MP
  AL-DP-2299	AL-DP-2251	cmgaaacmgumacmgumumcmumcmumcmumTT	117	agagagaacgumacguuucgTT	118	MP
  AL-DP-2300	AL-DP-2252	aaacmgumacmgumumcmumcmumcmumaumTT	119	aumagagagaacgumacguuuTT	120	MP
  AL-DP-2301	AL-DP-2254	cmcmcmumcmaaagcmcmgagaumcmgcmTT	121	gcgaucucggcuuumgagggTT	122	MP
  AL-DP-2302	AL-DP-2255	cmcmumcmaaagcmcmgagaumcmgcmgTT	123	cgcgaucucggcuuumgaggTT	124	MP
  AL-DP-2303	AL-DP-2256	acmaagacmcmaaumcmcmumgumcmacmTT	125	gugacmaggauuggucuuguTT	126	MP
  AL-DP-2304	AL-DP-2257	agcmgaggacmumgcmagcmgumagTT	127	cumacgcugcmaguccucgcuTT	128	MP
  AL-DP-2305	AL-DP-2258	cmgaggacmumgcmagcmgumagacmTT	129	gucumacgcugcmaguccuucgTT	130	MP
  AL-DP-2306	AL-DP-2259	umumgcmacmumumgaumaumumgumggaTT	131	uccmacmaaumaucmaagugcmaaTT	132	MP
  AL-DP-2307	AL-DP-2260	umgcmacmumumgaumaumumgumggaumTT	133	auccmacmaaumaucmaagugcmaTT	134	MP
  AL-DP-2308	AL-DP-2265	cmumaacmcmgaggumcmgaaacmgumTT	135	acguuucgaccucgguumagTT	136	MP
  AL-DP-2309	AL-DP-2266	umaacmcmgaggumcmgaaacmgumaTT	137	umacguuucgaccucgguumaTT	138	MP
  AL-DP-2310	AL-DP-2267	aacmcmgaggumcmgaaacmgumacmTT	139	gumacguuucgaccucgguuTT	140	MP
  AL-DP-2311	AL-DP-2268	acmcmgaggumcmgaaacmgumacmgTT	141	cgumacguuucgaccucgguTT	142	MP
  AL-DP-2312	AL-DP-2269	cmcmgaggumcmgaaacmgumacmgumTT	143	acgumacguuucgaccucggTT	144	MP
  1duplex identifier of siRNA agent of Table 1A having an identical nucleotide sequence when nucleotide modifications are disregarded

• TABLE 1C
  Additional exemplary iRNA agents for targeting influenza virus not listed in Table 1A having
  at least 50% target coverage (criterium 1, see Example 1) and at least 80% target efficiency
  (criterium 2, see Example 1), and having an off target score of less than 16.8 (see Example 1)

  							ELISA	ELISA	Plasmid
  					Target	%	(MDCK	(Vero	expres-
  		SEQ		SEQ	influ-	remaining	cells),	cells),	sion,
  Duplex	Sense strand sequence	ID	Antisense strand	ID	enza	infec-	% inhi-	% inhi-	% inhi-
  identifier	(5′-3′)	NO:	sequence (5′-3′)	NO	gene	tivity1	bition2	bition3	bition4

  AL-DP-2313	augagucuucuaaccgaggTT	145	ccucgguuagaagacucauTT	146	MP		−29	10
  AL-DP-2314	ucuucuaaccgaggucgaaTT	147	uucgaccucgguuagaagaTT	148	MP		−51	−53
  AL-DP-2315	gucuucuaaccgaggucgaTT	149	ucgaccucgguuagaagacTT	150	MP		−39	−74
  AL-DP-2316	cuucagaucgaacggucuaTT	151	uagaccguucgaucugaagTT	152	EB1		−63	−34
  AL-DP-2317	cagaucgaacggucuaacaTT	153	uguuagaccguucgaucugTT	154	EB1		−50	−33
  AL-DP-2318	agaucgaacggucuaacagTT	155	cuguuagaccguucgaucuTT	156	EB1		−43	−13
  AL-DP-2319	caaaaugcuauaaguaccaTT	157	ugguacuuauagcauuuugTT	158	EB1		−42	−65
  AL-DP-2320	uucagaucgaacggucuaaTT	159	uuagaccguucgaucugaaTT	160	EB1		−50	−51
  AL-DP-2321	uaccacauucccuuauacuTT	161	aguauaagggaaugugguaTT	162	EB1		−35	1
  AL-DP-2322	ucuuacauaaaucggacagTT	163	cuguccgauuuauguaagaTT	164	EB1		12	0
  AL-DP-2323	gucuuacauaaaucggacaTT	165	uguccgauuuauguaagacTT	166	EB1		21	−31
  AL-DP-2324	agucuuacauaaaucggacTT	167	guccgauuuauguaagacuTT	168	EB1		20	−6
  AL-DP-2325	ccucugaugauuucgcucuTT	169	agagcgaaaucaucagaggTT	170	EB1		35	−36
  AL-DP-2326	ggaugucaauccgacuuuaTT	171	uaaagucggauugacauccTT	172	EB1		40	12
  AL-DP-2327	uuugagagagaaggguacuTT	173	aguacccuucucucucaaaTT	174	NP		38	−14	33
  AL-DP-2328	aggcaacgaacccgaucguTT	175	acgaucggguucguugccuTT	176	NP		36	−44	65
  AL-DP-2329	ggcaacgaacccgaucgugTT	177	cacgaucggguucguugccTT	178	NP		31	−55	58
  AL-DP-2330	caacgaacccgaucgugccTT	179	ggcacgaucggguucguugTT	180	NP		33	−43	56
  AL-DP-2331	gcaacgaacccgaucgugcTT	181	gcacgaucggguucguugcTT	182	NP	<75	24	44	67
  AL-DP-2332	gaaaaggcaacgaacccgaTT	183	ucggguucguugccuuuucTT	184	NP		32	10	78
  AL-DP-2333	ucgagcucucggacgaaaaTT	185	uuuucguccgagagcucgaTT	186	NP	<50	18	53	69
  AL-DP-2334	aacgaacccgaucgugccuTT	187	aggcacgaucggguucguuTT	188	NP		35	−19	30
  AL-DP-2335	uauuucuucggagacaaugTT	189	cauugucuccgaagaaauaTT	190	NP		2	−20	41
  AL-DP-2348	ugcaugauaaaggcaguccTT	191	ggacugccuuuaucaugcaTT	192	PB2		−45	−65	4
  AL-DP-2349	auggggaugaucggaauauTT	193	auauuccgaucauccccauTT	194	PB2		0	32	55
  AL-DP-2350	uggggaugaucggaauauuTT	195	aauauuccgaucauccccaTT	196	PB2		−41	5	52
  AL-DP-2351	gaaacgggacucuagcauaTT	197	uaugcuagagucccguuucTT	198	PB2	<25	−33	68	76
  AL-DP-2356	agacuuugugcgacaaugcTT	199	gcauugucgcacaaagucuTT	200	PA		19	−22	77
  AL-DP-2357	gacuuugugcgacaaugcuTT	201	agcauugucgcacaaagucTT	202	PA		−84	13	86
  AL-DP-2358	ucuaugggauuccuuucguTT	203	acgaaaggaaucccauagaTT	204	PA		−33	−81	30
  AL-DP-2359	cuaugggauuccuuucgucTT	205	gacgaaaggaaucccauagTT	206	PA		−59	−109	80
  AL-DP-2360	auguggauggauucgaaccTT	207	gguucgaauccauccacauTT	208	PA		1	4	16
  AL-DP-2361	uguggauggauucgaaccgTT	209	cgguucgaauccauccacaTT	210	PA		−10	28	−7
  AL-DP-2362	guggauggauucgaaccgaTT	211	ucgguucgaauccauccacTT	212	PA	<25	−28	59	88
  AL-DP-2363	uggauggauucgaaccgaaTT	213	uucgguucgaauccauccaTT	214	PA	<25	−7	50	89
  AL-DP-2364	ggauggauucgaaccgaacTT	215	guucgguucgaauccauccTT	216	PA	<25	55	65	89
  AL-DP-2365	gauggauucgaaccgaacgTT	217	cguucgguucgaauccaucTT	218	PA		−3	27	60
  AL-DP-2366	auggauucgaaccgaacggTT	219	ccguucgguucgaauccauTT	220	PA		32	19	31
  AL-DP-2367	uggauucgaaccgaacggcTT	221	gccguucgguucgaauccaTT	222	PA		0	−52	14
  AL-DP-2368	aucuccacaacucgaggggTT	223	ccccucgaguuguggagauTT	224	PA		22	0	20
  1in in vitro plaque forming assay in MCDK cells as described in Example 3.1;
  2in in vitro ELISA assay in MCDK cells as described in Example 3.2:
  3in in vitro ELISA assay in MCDK cells as described in Example 3.2;
  4in in vitro ELISA assay in MCDK cells as described in Example 3.2; negative values indicate that target gene expression was enhanced in treated cells compared to controls

• TABLE 1D
  Additional exemplary iRNA agents for targeting influenza virus not listed in Table 1A or C,
  and having at least 80% target coverage (criterium 1, see Example 1) and at least 80% target
  efficiency (criterium 2, see Example 1)

  							ELISA	ELISA	Plasmid
  					Target	%	(MDCK	(Vero	expres-
  		SEQ		SEQ	influ-	remaining	cells),	cells),	sion,
  Duplex	Sense strand sequence	ID	Antisense strand	ID	enza	infec-	% inhi-	% inhi-	% inhi-
  identifier	(5′-3′)	NO:	sequence (5′-3′)	NO	gene	tivity1	bition2	bition3	bition4

  AL-DP-7614	uaacaauagagagaaugguTT	225	accauucucucuauuguuaTT	226	NP		17	+80	35
  AL-DP-7635	gaaacguacguucucucuaTT	227	uagagagaacguacguuucTT	228	MP		7	19
  AL-DP-7636	aacguacguucucucuaucTT	229	gauagagagaacguacguuTT	230	MP		1	24
  AL-DP-7637	uggcuaaagacaagaccaaTT	231	uuggucuugucuuuagccaTT	232	MP	<25	42	8
  AL-DP-7638	ggcuaaagacaagaccaauTT	233	auuggucuugucuuuagccTT	234	MP		19	5
  AL-DP-7639	cuaaagacaagaccaauccTT	235	ggauuggucuugucuuuagTT	236	MP		22	24
  AL-DP-7640	uaaagacaagaccaauccuTT	237	aggauuggucuugucuuuaTT	238	MP		11	43
  AL-DP-7641	aaagacaagaccaauccugTT	239	caggauuggucuugucuuuTT	240	MP		13	33
  AL-DP-7642	aagacaagaccaauccuguTT	241	acaggauuggucuugucuuTT	242	MP		−12	39
  AL-DP-7643	agacaagaccaauccugucTT	243	gacaggauuggucuugucuTT	244	MP		4	5
  AL-DP-7644	gacaagaccaauccugucaTT	245	ugacaggauuggucuugucTT	246	MP		3	26
  AL-DP-7645	caagaccaauccugucaccTT	247	ggugacaggauuggucuugTT	248	MP		2	2
  AL-DP-7646	aagaccaauccugucaccuTT	249	aggugacaggauuggucuuTT	250	MP		12	9
  AL-DP-7647	agaccaauccugucaccucTT	251	gaggugacaggauuggucuTT	252	MP		8	−5
  AL-DP-7648	gaccaauccugucaccucuTT	253	agaggugacaggauuggucTT	254	MP		−27	2
  AL-DP-7649	accaauccugucaccucugTT	255	cagaggugacaggauugguTT	256	MP		8	0
  AL-DP-7650	ccaauccugucaccucugaTT	257	ucagaggugacaggauuggTT	258	MP		−1	11
  AL-DP-7651	caauccugucaccucugacTT	259	gucagaggugacaggauugTT	260	MP	<50	30	16
  AL-DP-7652	auccugucaccucugacuaTT	261	uagucagaggugacaggauTT	262	MP	<50	69	9
  AL-DP-7653	uucacgcucaccgugcccaTT	263	ugggcacggugagcgugaaTT	264	MP	<75	31	6
  AL-DP-7654	ucacgcucaccgugcccagTT	265	cugggcacggugagcgugaTT	266	MP	<75	57	12
  AL-DP-7655	cucaccgugcccagugagcTT	267	gcucacugggcacggugagTT	268	MP			22
  AL-DP-7656	ucaccgugcccagugagcgTT	269	cgcucacugggcacggugaTT	270	MP	<75	69	10
  AL-DP-7657	accgugcccagugagcgagTT	271	cucgcucacugggcacgguTT	272	MP		1	22
  AL-DP-7658	ccgugcccagugagcgaggTT	273	ccucgcucacugggcacggTT	274	MP	<75	34	20
  AL-DP-7659	cgugcccagugagcgaggaTT	275	uccucgcucacugggcacgTT	276	MP		4	35
  AL-DP-7660	gugcccagugagcgaggacTT	277	guccucgcucacugggcacTT	278	MP	<75	33	49
  AL-DP-7661	ugcccagugagcgaggacuTT	279	aguccucgcucacugggcaTT	280	MP	<50	−10	58
  AL-DP-7662	gcccagugagcgaggacugTT	281	caguccucgcucacugggcTT	282	MP		−16	−44
  AL-DP-7663	cccagugagcgaggacugcTT	283	gcaguccucgcucacugggTT	284	MP		11	−8
  AL-DP-7664	ccagugagcgaggacugcaTT	285	ugcaguccucgcucacuggTT	286	MP		24	−20
  AL-DP-7665	cagugagcgaggacugcagTT	287	cugcaguccucgcucacugTT	288	MP		7	−24
  AL-DP-7666	agugagcgaggacugcagcTT	289	gcugcaguccucgcucacuTT	290	MP	<50	42	−22
  AL-DP-7667	gugagcgaggacugcagcgTT	291	cgcugcaguccucgcucacTT	292	MP		20	−17
  AL-DP-7668	ugagcgaggacugcagcguTT	293	acgcugcaguccucgcucaTT	294	MP	<50	51	−54
  AL-DP-7669	gcgaggacugcagcguagaTT	295	ucuacgcugcaguccucgcTT	296	MP	<25	32	37
  AL-DP-7670	gaggacugcagcguagacgTT	297	cgucuacgcugcaguccucTT	298	MP	<75	35	20
  AL-DP-7671	gcacuugauauuguggauuTT	299	aauccacaauaucaagugcTT	300	MP		−19	4
  AL-DP-7672	cacuugauauuguggauucTT	301	gaauccacaauaucaagugTT	302	MP		12	−10
  AL-DP-7673	acuugauauuguggauucuTT	303	agaauccacaauaucaaguTT	304	MP		0	−1
  AL-DP-7674	cuugauauuguggauucuuTT	305	aagaauccacaauaucaagTT	306	MP		−8	−36
  AL-DP-7675	uugauauuguggauucuugTT	307	caagaauccacaauaucaaTT	308	MP	<75	2	−27
  AL-DP-7676	ugauauuguggauucuugaTT	309	ucaagaauccacaauaucaTT	310	MP		−29	−40
  AL-DP-7677	gauauuguggauucuugauTT	311	aucaagaauccacaauaucTT	312	MP		−14	−24
  AL-DP-7678	auauuguggauucuugaucTT	313	gaucaagaauccacaauauTT	314	MP		24	−22
  AL-DP-7679	ggauucuugaucgucuuuuTT	315	aaaagacgaucaagaauccTT	316	MP		3	−34
  AL-DP-7684	ccgucaggcccccucaaagTT	317	cuuugagggggccugacggTT	318	MP		−1	23
  AL-DP-7685	cgucaggcccccucaaagcTT	319	gcuuugagggggccugacgTT	320	MP		−12	36
  AL-DP-7686	gucaggcccccucaaagccTT	321	ggcuuugagggggccugacTT	322	MP		−4	14
  AL-DP-7687	ucaggcccccucaaagccgTT	323	cggcuuugagggggccugaTT	324	MP	<75	32	−11
  AL-DP-7688	caggcccccucaaagccgaTT	325	ucggcuuugagggggccugTT	326	MP	<25	56	−14
  AL-DP-7689	aggcccccucaaagccgagTT	327	cucggcuuugagggggccuTT	328	MP	<50	83	−21
  AL-DP-7690	ggcccccucaaagccgagaTT	329	ucucggcuuugagggggccTT	330	MP	<50	89	−29
  AL-DP-7691	gcccccucaaagccgagauTT	331	aucucggcuuugagggggcTT	332	MP		8	−21
  AL-DP-7692	ccccucaaagccgagaucgTT	333	cgaucucggcuuugaggggTT	334	MP		5	−86
  1in in vitro plaque forming assay in MCDK cells as described in Example 3.1;
  2in in vitro ELISA assay in MCDK cells as described in Example 3.2:
  3in in vitro ELISA assay in MCDK cells as described in Example 3.2;
  4in in vitro ELISA assay in MCDK cells as described in Example 3.2; negative values indicate that target gene expression was enhanced in treated cells compared to controls

• TABLE 1E
  Additional exemplary iRNA agents for targeting influenza virus not listed in Table 1A, C, or
  D,and having at least 50% target coverage (criterium 1, see Example 1) and at least 80%
  target efficiency (criterium 2, see Example 1)

  							ELISA	ELISA	Plasmid
  					Target	%	(MDCK	(Vero	expres-
  		SEQ		SEQ	influ-	remaining	cells),	cells),	sion,
  Duplex	Sense strand sequence	ID	Antisense strand	ID	enza	infec-	% inhi-	% inhi-	% inhi-
  identifier	(5′-3′)	NO:	sequence (5′-3′)	NO	gene	tivity1	bition2	bition3	bition4

  AL-DP-7565	cgagagaggcgaagagacaTT	335	ugucucuucgccucucucgTT	336	PA	<50	−29	71	59
  AL-DP-7566	gaagagacaauugaagaaaTT	337	uuucuucaauugucucuucTT	338	PA	<75	−15	61	57
  AL-DP-7567	uuuagagccuauguggaugTT	339	cauccacauaggcucuaaaTT	340	PA	<75	−64	49	13
  AL-DP-7568	uuagagccuauguggauggTT	341	ccauccacauaggcucuaaTT	342	PA	<75	−24	60	19
  AL-DP-7569	uagagccuauguggauggaTT	343	uccauccacauaggcucuaTT	344	PA	<75	−47	67	26
  AL-DP-7570	agagccuauguggauggauTT	345	auccauccacauaggcucuTT	346	PA	<50	−23	87	72
  AL-DP-7571	gagccuauguggauggauuTT	347	aauccauccacauaggcucTT	348	PA	<25	2	94	84
  AL-DP-7572	agccuauguggauggauucTT	349	gaauccauccacauaggcuTT	350	PA	<25	−14	82	76
  AL-DP-7573	uaugaagcaauugaggaguTT	351	acuccucaauugcuucauaTT	352	PA	<75	−58	48	6
  AL-DP-7574	augaagcaauugaggagugTT	353	cacuccucaauugcuucauTT	354	PA		−69	16	4
  AL-DP-7575	ugaagcaauugaggagugcTT	355	gcacuccucaauugcuucaTT	356	PA		−65	99	2
  AL-DP-7576	gaagcaauugaggagugccTT	357	ggcacuccucaauugcuucTT	358	PA	<25	−23	99	63
  AL-DP-7577	aagcaauugaggagugccuTT	359	aggcacuccucaauugcuuTT	360	PA	<25	−27	99	60
  AL-DP-7578	gaucccuggguuuugcuuaTT	361	uaagcaaaacccagggaucTT	362	PA	<50	−50	96	80
  AL-DP-7579	aucccuggguuuugcuuaaTT	363	uuaagcaaaacccagggauTT	364	PA	<25	−51	98	87
  AL-DP-7580	ucccuggguuuugcuuaauTT	365	auuaagcaaaacccagggaTT	366	PA	<75	15	95	60
  AL-DP-7581	cccuggguuuugcuuaaugTT	367	cauuaagcaaaacccagggTT	368	PA	<50	−55	100	75
  AL-DP-7582	ccuggguuuugcuuaaugcTT	369	gcauuaagcaaaacccaggTT	370	PA	<25	3	74	87
  AL-DP-7583	ucuugguucaacuccuuccTT	371	ggaaggaguugaaccaagaTT	372	PA	<75	43	14	19
  AL-DP-7584	cuugguucaacuccuuccuTT	373	aggaaggaguugaaccaagTT	374	PA		−19	22	74
  AL-DP-7585	aaacgggacucuagcauacTT	375	guaugcuagagucccguuuTT	376	PB2		6	35	66
  AL-DP-7586	aacgggacucuagcauacuTT	377	aguaugcuagagucccguuTT	378	PB2	<25	43	35	58
  AL-DP-7587	acgggacucuagcauacuuTT	379	aaguaugcuagagucccguTT	380	PB2	<25	14	52	71
  AL-DP-7588	cgggacucuagcauacuuaTT	381	uaaguaugcuagagucccgTT	382	PB2	<25	34	36	72
  AL-DP-7589	gggacucuagcauacuuacTT	383	guaaguaugcuagagucccTT	384	PB2		−28	32	69
  AL-DP-7590	ggacucuagcauacuuacuTT	385	aguaaguaugcuagaguccTT	386	PB2		−10	36	75
  AL-DP-7591	gacucuagcauacuuacugTT	387	caguaaguaugcuagagucTT	388	PB2		−20	22	61
  AL-DP-7592	acucuagcauacuuacugaTT	389	ucaguaaguaugcuagaguTT	390	PB2	<25	−25	48	77
  AL-DP-7593	cucuagcauacuuacugacTT	391	gucaguaaguaugcuagagTT	392	PB2	<75	−14	50	64
  AL-DP-7594	ucuagcauacuuacugacaTT	393	ugucaguaaguaugcuagaTT	394	PB2		−40	9	44
  AL-DP-7595	cuagcauacuuacugacagTT	395	cugucaguaaguaugcuagTT	396	PB2	<25	59	48	66
  AL-DP-7596	uagcauacuuacugacagcTT	397	gcugucaguaaguaugcuaTT	398	PB2		−33	−14	44
  AL-DP-7597	agcauacuuacugacagccTT	399	ggcugucaguaaguaugcuTT	400	PB2		−13	−27	29
  AL-DP-7598	gcauacuuacugacagccaTT	401	uggcugucaguaaguaugcTT	402	PB2	<25	8	65	73
  AL-DP-7599	cauacuuacugacagccagTT	403	cuggcugucaguaaguaugTT	404	PB2	<25	−39	43	69
  AL-DP-7600	auacuuacugacagccagaTT	405	ucuggcugucaguaaguauTT	406	PB2	<25	−33	48	74
  AL-DP-7601	uacuuacugacagccagacTT	407	gucuggcugucaguaaguaTT	408	PB2		−28	−40	35
  AL-DP-7602	acuuacugacagccagacaTT	409	ugucuggcugucaguaaguTT	410	PB2		6	17	60
  AL-DP-7603	cuuacugacagccagacagTT	411	cugucuggcugucaguaagTT	412	PB2	<25	16	73	77
  AL-DP-7604	uuacugacagccagacagcTT	413	gcugucuggcugucaguaaTT	414	PB2		18	−26	37
  AL-DP-7605	uacugacagccagacagcgTT	415	cgcugucuggcugucaguaTT	416	PB2		20	−133	41
  AL-DP-7606	acugacagccagacagcgaTT	417	ucgcugucuggcugucaguTT	418	PB2	<25	34	0	80
  AL-DP-7607	cugacagccagacagcgacTT	419	gucgcugucuggcugucagTT	420	PB2	<25	38	51	74
  AL-DP-7608	ugacagccagacagcgaccTT	421	ggucgcugucuggcugucaTT	422	PB2	<25	64	−155 34
  AL-DP-7609	gacagccagacagcgaccaTT	423	uggucgcugucuggcugucTT	424	PB2	<25	88	−16	71
  AL-DP-7610	acagccagacagcgaccaaTT	425	uuggucgcugucuggcuguTT	426	PB2	<25	55	29	72
  AL-DP-7611	cagccagacagcgaccaaaTT	427	uuuggucgcugucuggcugTT	428	PB2	<25	33	88	78
  AL-DP-7612	agccagacagcgaccaaaaTT	429	uuuuggucgcugucuggcuTT	430	PB2	<25	37	73	74
  AL-DP-7613	gccagacagcgaccaaaagTT	431	cuuuuggucgcugucuggcTT	432	PB2	<25	57	−4	79
  AL-DP-7615	cccgaucgugccuuccuuuTT	433	aaaggaaggcacgaucgggTT	434	NP		17	−80	35
  AL-DP-7616	ccgaucgugccuuccuuugTT	435	caaaggaaggcacgaucggTT	436	NP		11	−40	47
  AL-DP-7617	cgaucgugccuuccuuugaTT	437	ucaaaggaaggcacgaucgTT	438	NP		22	−81	47
  AL-DP-7618	gaucgugccuuccuuugacTT	439	gucaaaggaaggcacgaucTT	440	NP	<25	87	86	73
  AL-DP-7619	aucgugccuuccuuugacaTT	441	ugucaaaggaaggcacgauTT	442	NP	<25	86	82	50
  AL-DP-7620	ucgugccuuccuuugacauTT	443	augucaaaggaaggcacgaTT	444	NP	<25	3	43	53
  AL-DP-7621	cgugccuuccuuugacaugTT	445	caugucaaaggaaggcacgTT	446	NP		−22	7	47
  AL-DP-7622	gugccuuccuuugacaugaTT	447	ucaugucaaaggaaggcacTT	448	NP	<25	17	78	53
  AL-DP-7623	ggaucuuauuucuucggagTT	449	cuccgaagaaauaagauccTT	450	NP	<25	66	95	58
  AL-DP-7624	gaucuuauuucuucggagaTT	451	ucuccgaagaaauaagaucTT	452	NP	<25	95	96	75
  AL-DP-7625	aucuuauuucuucggagacTT	453	gucuccgaagaaauaagauTT	454	NP	<25	33	78	77
  AL-DP-7626	ucuuauuucuucggagacaTT	455	ugucuccgaagaaauaagaTT	456	NP		8	17	7
  AL-DP-7627	cuuauuucuucggagacaaTT	457	uugucuccgaagaaauaagTT	458	NP	<25	32	66	54
  AL-DP-7628	uuauuucuucggagacaauTT	459	auugucuccgaagaaauaaTT	460	NP	<25	24	81	72
  AL-DP-7629	auuucuucggagacaaugcTT	461	gcauugucuccgaagaaauTT	462	NP	<50	11	44	61
  AL-DP-7630	gggcggggagucuucgagcTT	463	gcucgaagacuccccgcccTT	464	NP		15	24	9
  AL-DP-7631	ggcggggagucuucgagcuTT	465	agcucgaagacuccccgccTT	466	NP		5	33	30
  AL-DP-7632	gcggggagucuucgagcucTT	467	gagcucgaagacuccccgcTT	468	NP	<25	16	41	33
  AL-DP-7633	cggggagucuucgagcucuTT	469	agagcucgaagacuccccgTT	470	NP	<25	33	55	50
  AL-DP-7634	ggggagucuucgagcucucTT	471	gagagcucgaagacuccccTT	472	NP	<25	41	82	44
  AL-DP-7680	ugacgauggucauuuugucTT	473	gacaaaaugaccaucgucaTT	474	MP	<25	58	72	49
  AL-DP-7681	gacgauggucauuuugucaTT	475	ugacaaaaugaccaucgucTT	476	MP		−1	23
  AL-DP-7682	ucccgucaggcccccucaaTT	477	uugagggggccugacgggaTT	478	MP		−12	36
  AL-DP-7683	cccgucaggcccccucaaaTT	479	uuugagggggccugacgggTT	480	MP		−4	14
  AL-DP-8102	ugagucuucuaaccgagguTT	481	accucgguuagaagacucaTT	482	MP
  AL-DP-8103	gagucuucuaaccgaggucTT	483	gaccucgguuagaagacucTT	484	MP
  AL-DP-8104	agucuucuaaccgaggucgTT	485	cgaccucgguuagaagacuTT	486	MP
  AL-DP-8107	auuguggauucuugaucguTT	487	acgaucaagaauccacaauTT	488	MP
  AL-DP-8108	uggauucuugaucgucuuuTT	489	aaagacgaucaagaauccaTT	490	MP
  AL-DP-8109	gauucuugaucgucuuuucTT	491	gaaaagacgaucaagaaucTT	492	MP
  AL-DP-8110	auucuugaucgucuuuucuTT	493	agaaaagacgaucaagaauTT	494	MP
  AL-DP-8111	uucuugaucgucuuuucuuTT	495	aagaaaagacgaucaagaaTT	496	MP
  AL-DP-8112	ucuugaucgucuuuucuucTT	497	gaagaaaagacgaucaagaTT	498	MP
  AL-DP-8113	cuugaucgucuuuucuucaTT	499	ugaagaaaagacgaucaagTT	500	MP
  AL-DP-8114	uugaucgucuuuucuucaaTT	501	uugaagaaaagacgaucaaTT	502	MP
  AL-DP-8115	ugaucgucuuuucuucaaaTT	503	uuugaagaaaagacgaucaTT	504	MP
  AL-DP-8116	gaucgucuuuucuucaaauTT	505	auuugaagaaaagacgaucTT	506	MP
  AL-DP-8117	aucgucuuuucuucaaaugTT	507	cauuugaagaaaagacgauTT	508	MP
  AL-DP-8118	ucgucuuuucuucaaaugcTT	509	gcauuugaagaaaagacgaTT	510	MP
  AL-DP-8119	cgucuuuucuucaaaugcaTT	511	ugcauuugaagaaaagacgTT	512	MP
  AL-DP-8120	gucuuuucuucaaaugcauTT	513	augcauuugaagaaaagacTT	514	MP
  AL-DP-8121	ucuuuucuucaaaugcauuTT	515	aaugcauuugaagaaaagaTT	516	MP
  AL-DP-8122	cuuuucuucaaaugcauuuTT	517	aaaugcauuugaagaaaagTT	518	MP
  AL-DP-8123	uuuucuucaaaugcauuuaTT	519	uaaaugcauuugaagaaaaTT	520	MP
  AL-DP-8124	uuucuucaaaugcauuuauTT	521	auaaaugcauuugaagaaaTT	522	MP
  AL-DP-8125	uucuucaaaugcauuuaucTT	523	gauaaaugcauuugaagaaTT	524	MP
  AL-DP-8126	ucuucaaaugcauuuaucgTT	525	cgauaaaugcauuugaagaTT	526	MP
  AL-DP-8127	cuucaaaugcauuuaucguTT	527	acgauaaaugcauuugaagTT	528	MP
  AL-DP-8128	uucaaaugcauuuaucgucTT	529	gacgauaaaugcauuugaaTT	530	MP
  AL-DP-8129	uuaaauacgguuugaaaagTT	531	cuuuucaaaccguauuuaaTT	532	MP
  AL-DP-8130	uaaauacgguuugaaaagaTT	533	ucuuuucaaaccguauuuaTT	534	MP
  AL-DP-8131	aaauacgguuugaaaagagTT	535	cucuuuucaaaccguauuuTT	536	MP
  AL-DP-8132	aauacgguuugaaaagaggTT	537	ccucuuuucaaaccguauuTT	538	MP
  AL-DP-8133	uugaaaagagggccuucuaTT	539	uagaaggcccucuuuucaaTT	540	MP
  AL-DP-8134	ugaaaagagggccuucuacTT	541	guagaaggcccucuuuucaTT	542	MP
  AL-DP-8135	gaaaagagggccuucuacgTT	543	cguagaaggcccucuuuucTT	544	MP
  AL-DP-8136	ccugagucuaugagggaagTT	545	cuucccucauagacucaggTT	546	MP
  AL-DP-8137	cugagucuaugagggaagaTT	547	ucuucccucauagacucagTT	548	MP
  AL-DP-8138	ugcuguggauguugacgauTT	549	aucgucaacauccacagcaTT	550	MP
  AL-DP-8139	gcuguggauguugacgaugTT	551	caucgucaacauccacagcTT	552	MP
  AL-DP-8140	cuguggauguugacgauggTT	553	ccaucgucaacauccacagTT	554	MP
  AL-DP-8141	uguggauguugacgaugguTT	555	accaucgucaacauccacaTT	556	MP
  AL-DP-8142	guggauguugacgauggucTT	557	gaccaucgucaacauccacTT	558	MP
  AL-DP-8143	uggauguugacgauggucaTT	559	ugaccaucgucaacauccaTT	560	MP
  AL-DP-8144	ggauguugacgauggucauTT	561	augaccaucgucaacauccTT	562	MP
  AL-DP-8145	gauguugacgauggucauuTT	563	aaugaccaucgucaacaucTT	564	MP
  AL-DP-8146	auguugacgauggucauuuTT	565	aaaugaccaucgucaacauTT	566	MP
  AL-DP-8147	uguugacgauggucauuuuTT	567	aaaaugaccaucgucaacaTT	568	MP
  AL-DP-8148	guugacgauggucauuuugTT	569	caaaaugaccaucgucaacTT	570	MP
  AL-DP-8149	uugacgauggucauuuuguTT	571	acaaaaugaccaucgucaaTT	572	MP
  AL-DP-8152	acgauggucauuuugucaaTT	573	uugacaaaaugaccaucguTT	574	MP
  AL-DP-8153	cgauggucauuuugucaacTT	575	guugacaaaaugaccaucgTT	576	MP
  AL-DP-8154	gauggucauuuugucaacaTT	577	uguugacaaaaugaccaucTT	578	MP
  AL-DP-8155	auggucauuuugucaacauTT	579	auguugacaaaaugaccauTT	580	MP
  AL-DP-8156	uggucauuuugucaacauaTT	581	uauguugacaaaaugaccaTT	582	MP
  AL-DP-8157	ggucauuuugucaacauagTT	583	cuauguugacaaaaugaccTT	584	MP
  AL-DP-8158	gucauuuugucaacauagaTT	585	ucuauguugacaaaaugacTT	586	MP
  AL-DP-8159	ucaaggcaccaaacgaucuTT	587	agaucguuuggugccuugaTT	588	NP
  AL-DP-8160	caaggcaccaaacgaucuuTT	589	aagaucguuuggugccuugTT	590	NP
  AL-DP-8161	aaggcaccaaacgaucuuaTT	591	uaagaucguuuggugccuuTT	592	NP
  AL-DP-8162	aacagcauaacaauagagaTT	593	ucucuauuguuaugcuguuTT	594	NP
  AL-DP-8163	acagcauaacaauagagagTT	595	cucucuauuguuaugcuguTT	596	NP
  AL-DP-8164	cagcauaacaauagagagaTT	597	ucucucuauuguuaugcugTT	598	NP
  AL-DP-8165	agcauaacaauagagagaaTT	599	uucucucuauuguuaugcuTT	600	NP
  AL-DP-8166	gcauaacaauagagagaauTT	601	auucucucuauuguuaugcTT	602	NP
  AL-DP-8167	cauaacaauagagagaaugTT	603	cauucucucuauuguuaugTT	604	NP
  AL-DP-8168	auugcauaugagagaauguTT	605	acauucucucauaugcaauTT	606	NP
  AL-DP-8169	uugcauaugagagaaugugTT	607	cacauucucucauaugcaaTT	608	NP
  AL-DP-8170	gcauaugagagaaugugcaTT	609	ugcacauucucucauaugcTT	610	NP
  AL-DP-8171	cauaugagagaaugugcaaTT	611	uugcacauucucucauaugTT	612	NP
  AL-DP-8177	gggagucuucgagcucucgTT	613	cgagagcucgaagacucccTT	614	NP
  AL-DP-8178	ggagucuucgagcucucggTT	615	ccgagagcucgaagacuccTT	616	NP
  AL-DP-8179	gagucuucgagcucucggaTT	617	uccgagagcucgaagacucTT	618	NP
  AL-DP-8180	agucuucgagcucucggacTT	619	guccgagagcucgaagacuTT	620	NP
  AL-DP-8181	gucuucgagcucucggacgTT	621	cguccgagagcucgaagacTT	622	NP
  AL-DP-8182	ucuucgagcucucggacgaTT	623	ucguccgagagcucgaagaTT	624	NP
  AL-DP-8183	cuucgagcucucggacgaaTT	625	uucguccgagagcucgaagTT	626	NP
  AL-DP-8184	uucgagcucucggacgaaaTT	627	uuucguccgagagcucgaaTT	628	NP
  AL-DP-8185	cgagcucucggacgaaaagTT	629	cuuuucguccgagagcucgTT	630	NP
  AL-DP-8186	gagcucucggacgaaaaggTT	631	ccuuuucguccgagagcucTT	632	NP
  AL-DP-8187	agcucucggacgaaaaggcTT	633	gccuuuucguccgagagcuTT	634	NP
  AL-DP-8188	gcucucggacgaaaaggcaTT	635	ugccuuuucguccgagagcTT	636	NP
  AL-DP-8189	cucucggacgaaaaggcaaTT	637	uugccuuuucguccgagagTT	638	NP
  AL-DP-8190	ucucggacgaaaaggcaacTT	639	guugccuuuucguccgagaTT	640	NP
  AL-DP-8191	cucggacgaaaaggcaacgTT	641	cguugccuuuucguccgagTT	642	NP
  AL-DP-8192	ucggacgaaaaggcaacgaTT	643	ucguugccuuuucguccgaTT	644	NP
  AL-DP-8193	cggacgaaaaggcaacgaaTT	645	uucguugccuuuucguccgTT	646	NP
  AL-DP-8194	ggacgaaaaggcaacgaacTT	647	guucguugccuuuucguccTT	648	NP
  AL-DP-8195	gacgaaaaggcaacgaaccTT	649	gguucguugccuuuucgucTT	650	NP
  AL-DP-8196	acgaaaaggcaacgaacccTT	651	ggguucguugccuuuucguTT	652	NP
  AL-DP-8197	cgaaaaggcaacgaacccgTT	653	cggguucguugccuuuucgTT	654	NP
  AL-DP-8198	aaaaggcaacgaacccgauTT	655	aucggguucguugccuuuuTT	656	NP
  AL-DP-8199	aaaggcaacgaacccgaucTT	657	gaucggguucguugccuuuTT	658	NP
  AL-DP-8200	aaggcaacgaacccgaucgTT	659	cgaucggguucguugccuuTT	660	NP
  AL-DP-8201	acgaacccgaucgugccuuTT	661	aaggcacgaucggguucguTT	662	NP
  AL-DP-8202	cgaacccgaucgugccuucTT	663	gaaggcacgaucggguucgTT	664	NP
  AL-DP-8203	gaacccgaucgugccuuccTT	665	ggaaggcacgaucggguucTT	666	NP
  AL-DP-8204	aacccgaucgugccuuccuTT	667	aggaaggcacgaucggguuTT	668	NP
  AL-DP-8205	acccgaucgugccuuccuuTT	669	aaggaaggcacgaucggguTT	670	NP
  AL-DP-8221	auggaugucaauccgacuuTT	671	aagucggauugacauccauTT	672	PB1
  AL-DP-8222	uggaugucaauccgacuuuTT	673	aaagucggauugacauccaTT	674	PB1
  AL-DP-8223	gaugucaauccgacuuuacTT	675	guaaagucggauugacaucTT	676	PB1
  AL-DP-8224	augucaauccgacuuuacuTT	677	aguaaagucggauugacauTT	678	PB1
  AL-DP-8225	ugucaauccgacuuuacuuTT	679	aaguaaagucggauugacaTT	680	PB1
  AL-DP-8226	ccauacagccauggaacagTT	681	cuguuccauggcuguauggTT	682	PB1
  AL-DP-8227	cauacagccauggaacaggTT	683	ccuguuccauggcuguaugTT	684	PB1
  AL-DP-8228	acaggauacaccauggacaTT	685	uguccaugguguauccuguTT	686	PB1
  AL-DP-8229	caggauacaccauggacacTT	687	guguccaugguguauccugTT	688	PB1
  AL-DP-8230	uuggaagcaauggcuuuccTT	689	ggaaagccauugcuuccaaTT	690	PB1
  AL-DP-8231	ggaagcaauggcuuuccuuTT	691	aaggaaagccauugcuuccTT	692	PB1
  AL-DP-8232	agcaauggcuuuccuugaaTT	693	uucaaggaaagccauugcuTT	694	PB1
  AL-DP-8233	augaugacuaacucacaagTT	695	cuugugaguuagucaucauTT	696	PB1
  AL-DP-8234	ugaugacuaacucacaagaTT	697	ucuugugaguuagucaucaTT	698	PB1
  AL-DP-8235	accaaauggaaugagaaucTT	699	gauucucauuccauuugguTT	700	PB1
  AL-DP-8236	ccaaauggaaugagaaucaTT	701	ugauucucauuccauuuggTT	702	PB1
  AL-DP-8237	ggaaugaugaugggcauguTT	703	acaugcccaucaucauuccTT	704	PB1
  AL-DP-8238	gaaugaugaugggcauguuTT	705	aacaugcccaucaucauucTT	706	PB1
  AL-DP-8239	cuccaauccucugaugauuTT	707	aaucaucagaggauuggagTT	708	PB1
  AL-DP-8240	uccaauccucugaugauuuTT	709	aaaucaucagaggauuggaTT	710	PB1
  AL-DP-8241	aucaugagggaauacaagcTT	711	gcuuguauucccucaugauTT	712	PB1
  AL-DP-8242	uuugugcgacaaugcuucaTT	713	ugaagcauugucgcacaaaTT	714	PA
  AL-DP-8243	uaugggauuccuuucgucaTT	715	ugacgaaaggaaucccauaTT	716	PA
  AL-DP-8244	uccgagagaggcgaagagaTT	717	ucucuucgccucucucggaTT	718	PA
  AL-DP-8245	ccgagagaggcgaagagacTT	719	gucucuucgccucucucggTT	720	PA
  AL-DP-8247	gagagaggcgaagagacaaTT	721	uugucucuucgccucucucTT	722	PA
  AL-DP-8248	agagaggcgaagagacaauTT	723	auugucucuucgccucucuTT	724	PA
  AL-DP-8249	gagaggcgaagagacaauuTT	725	aauugucucuucgccucucTT	726	PA
  AL-DP-8250	agaggcgaagagacaauugTT	727	caauugucucuucgccucuTT	728	PA
  AL-DP-8251	gaggcgaagagacaauugaTT	729	ucaauugucucuucgccucTT	730	PA
  AL-DP-8252	aggcgaagagacaauugaaTT	731	uucaauugucucuucgccuTT	732	PA
  AL-DP-8253	ggcgaagagacaauugaagTT	733	cuucaauugucucuucgccTT	734	PA
  AL-DP-8254	gcgaagagacaauugaagaTT	735	ucuucaauugucucuucgcTT	736	PA
  AL-DP-8255	cgaagagacaauugaagaaTT	737	uucuucaauugucucuucgTT	738	PA
  AL-DP-8257	uucuccagccuugaaaacuTT	739	aguuuucaaggcuggagaaTT	740	PA
  AL-DP-8258	ucuccagccuugaaaacuuTT	741	aaguuuucaaggcuggagaTT	742	PA
  AL-DP-8259	cuccagccuugaaaacuuuTT	743	aaaguuuucaaggcuggagTT	744	PA
  AL-DP-8260	uccagccuugaaaacuuuaTT	745	uaaaguuuucaaggcuggaTT	746	PA
  AL-DP-8261	ccagccuugaaaacuuuagTT	747	cuaaaguuuucaaggcuggTT	748	PA
  AL-DP-8262	cagccuugaaaacuuuagaTT	749	ucuaaaguuuucaaggcugTT	750	PA
  AL-DP-8263	agccuugaaaacuuuagagTT	751	cucuaaaguuuucaaggcuTT	752	PA
  AL-DP-8264	gccuugaaaacuuuagagcTT	753	gcucuaaaguuuucaaggcTT	754	PA
  AL-DP-8265	ccuugaaaacuuuagagccTT	755	ggcucuaaaguuuucaaggTT	756	PA
  AL-DP-8266	cuugaaaacuuuagagccuTT	757	aggcucuaaaguuuucaagTT	758	PA
  AL-DP-8267	uugaaaacuuuagagccuaTT	759	uaggcucuaaaguuuucaaTT	760	PA
  AL-DP-8268	ugaaaacuuuagagccuauTT	761	auaggcucuaaaguuuucaTT	762	PA
  AL-DP-8269	gaaaacuuuagagccuaugTT	763	cauaggcucuaaaguuuucTT	764	PA
  AL-DP-8270	aaaacuuuagagccuauguTT	765	acauaggcucuaaaguuuuTT	766	PA
  AL-DP-8271	aaacuuuagagccuaugugTT	767	cacauaggcucuaaaguuuTT	768	PA
  AL-DP-8272	aacuuuagagccuauguggTT	769	ccacauaggcucuaaaguuTT	770	PA
  AL-DP-8273	acuuuagagccuauguggaTT	771	uccacauaggcucuaaaguTT	772	PA
  AL-DP-8274	cuuuagagccuauguggauTT	773	auccacauaggcucuaaagTT	774	PA
  AL-DP-8281	aaccgaacggcugcauugaTT	775	ucaaugcagccguucgguuTT	776	PA
  AL-DP-8282	accgaacggcugcauugagTT	777	cucaaugcagccguucgguTT	778	PA
  AL-DP-8283	ccgaacggcugcauugaggTT	779	ccucaaugcagccguucggTT	780	PA
  AL-DP-8284	cgaacggcugcauugagggTT	781	cccucaaugcagccguucgTT	782	PA
  AL-DP-8285	gaacggcugcauugagggcTT	783	gcccucaaugcagccguucTT	784	PA
  AL-DP-8286	aacggcugcauugagggcaTT	785	ugcccucaaugcagccguuTT	786	PA
  AL-DP-8287	acggcugcauugagggcaaTT	787	uugcccucaaugcagccguTT	788	PA
  AL-DP-8288	cggcugcauugagggcaagTT	789	cuugcccucaaugcagccgTT	790	PA
  AL-DP-8289	ggcugcauugagggcaagcTT	791	gcuugcccucaaugcagccTT	792	PA
  AL-DP-8290	gcugcauugagggcaagcuTT	793	agcuugcccucaaugcagcTT	794	PA
  AL-DP-8291	cugcauugagggcaagcuuTT	795	aagcuugcccucaaugcagTT	796	PA
  AL-DP-8292	ugcauugagggcaagcuuuTT	797	aaagcuugcccucaaugcaTT	798	PA
  AL-DP-8293	gcauugagggcaagcuuucTT	799	gaaagcuugcccucaaugcTT	800	PA
  AL-DP-8294	cauugagggcaagcuuucuTT	801	agaaagcuugcccucaaugTT	802	PA
  AL-DP-8295	auugagggcaagcuuucucTT	803	gagaaagcuugcccucaauTT	804	PA
  AL-DP-8296	uugagggcaagcuuucucaTT	805	ugagaaagcuugcccucaaTT	806	PA
  AL-DP-8297	ugagggcaagcuuucucaaTT	807	uugagaaagcuugcccucaTT	808	PA
  AL-DP-8298	gagggcaagcuuucucaaaTT	809	uuugagaaagcuugcccucTT	810	PA
  AL-DP-8299	agggcaagcuuucucaaauTT	811	auuugagaaagcuugcccuTT	812	PA
  AL-DP-8300	gggcaagcuuucucaaaugTT	813	cauuugagaaagcuugcccTT	814	PA
  AL-DP-8301	ggcaagcuuucucaaauguTT	815	acauuugagaaagcuugccTT	816	PA
  AL-DP-8302	gcaagcuuucucaaaugucTT	817	gacauuugagaaagcuugcTT	818	PA
  AL-DP-8303	augauaagcaaaugcagaaTT	819	uucugcauuugcuuaucauTT	820	PA
  AL-DP-8304	ugauaagcaaaugcagaacTT	821	guucugcauuugcuuaucaTT	822	PA
  AL-DP-8305	cuuagggacaaccuggaacTT	823	guuccagguugucccuaagTT	824	PA
  AL-DP-8306	uuagggacaaccuggaaccTT	825	gguuccagguugucccuaaTT	826	PA
  AL-DP-8307	uagggacaaccuggaaccuTT	827	agguuccagguugucccuaTT	828	PA
  AL-DP-8308	agggacaaccuggaaccugTT	829	cagguuccagguugucccuTT	830	PA
  AL-DP-8309	gggacaaccuggaaccuggTT	831	ccagguuccagguugucccTT	832	PA
  AL-DP-8315	agcaauugaggagugccugTT	833	caggcacuccucaauugcuTT	834	PA
  AL-DP-8316	gcaauugaggagugccugaTT	835	ucaggcacuccucaauugcTT	836	PA
  AL-DP-8317	caauugaggagugccugauTT	837	aucaggcacuccucaauugTT	838	PA
  AL-DP-8318	aauugaggagugccugauuTT	839	aaucaggcacuccucaauuTT	840	PA
  AL-DP-8319	auugaggagugccugauuaTT	841	uaaucaggcacuccucaauTT	842	PA
  AL-DP-8320	uugaggagugccugauuaaTT	843	uuaaucaggcacuccucaaTT	844	PA
  AL-DP-8328	uugguucaacuccuuccucTT	845	gaggaaggaguugaaccaaTT	846	PA
  AL-DP-8329	gaaugaaauggaugauggcTT	847	gccaucauccauuucauucTT	848	PB2
  AL-DP-8330	ugguaaugaaacggaaacgTT	849	cguuuccguuucauuaccaTT	850	PB2
  AL-DP-8331	augaaacggaaacgggacuTT	851	agucccguuuccguuucauTT	852	PB2
  AL-DP-8332	ugaaacggaaacgggacucTT	853	gagucccguuuccguuucaTT	854	PB2
  AL-DP-8333	gaaacggaaacgggacucuTT	855	agagucccguuuccguuucTT	856	PB2
  AL-DP-8334	aaacggaaacgggacucuaTT	857	uagagucccguuuccguuuTT	858	PB2
  AL-DP-8335	aacggaaacgggacucuagTT	859	cuagagucccguuuccguuTT	860	PB2
  AL-DP-8336	acggaaacgggacucuagcTT	861	gcuagagucccguuuccguTT	862	PB2
  AL-DP-8337	cggaaacgggacucuagcaTT	863	ugcuagagucccguuuccgTT	864	PB2
  AL-DP-8338	ggaaacgggacucuagcauTT	865	augcuagagucccguuuccTT	866	PB2
  1in in vitro plaque forming assay in MCDK cells as described in Example 3.1;
  2in in vitro ELISA assay in MCDK cells as described in Example 3.2:
  3in in vitro ELISA assay in MCDK cells as described in Example 3.2;
  4in in vitro ELISA assay in MCDK cells as described in Example 3.2; negative values indicate that target gene expression was enhanced in treated cells compared to controls

• TABLE 1F
  Exemplary iRNA agents for targeting influenza virus,and having 100%
  target coverage (criterium 1, see example 1) and 100% target
  efficiency (criterium 2, see example 1), but allowing for up to 3
  universal bases in the non-seed region of the iRNA agent; x stands
  for the position of a universal base

  		SEQ		SEQ	Target
  Duplex	Sense strand sequence	ID	Antisense strand	ID	influenza
  identifier	(5′-3′)	NO:	sequence (5′-3′)	NO:	gene
  AL-DP-8368	ucxgcxgaxaugagcauugTT	867	caaugcucauxucxgcxgaTT	868	PB1
  AL-DP-8369	cxgcxgaxaugagcauuggTT	869	ccaaugcucauxucxgcxgTT	870	PB1
  AL-DP-8370	xaagaucugxuccaccauuTT	871	aaugguggaxcagaucuuxTT	872	PB1
  AL-DP-8371	aagaucugxuccaccauugTT	873	caaugguggaxcagaucuuTT	874	PB1
  AL-DP-8372	agaucugxuccaccauugxTT	875	xcaaugguggaxcagaucuTT	876	PB1
  AL-DP-8373	xugaauuuxxcuuguccuuTT	877	aaggacaagxxaaauucaxTT	878	PB1
  AL-DP-8374	ugaauuuxxcuuguccuucTT	879	gaaggacaagxxaaauucaTT	880	PB1
  AL-DP-8375	gaauuuxxcuuguccuucxTT	881	xgaaggacaagxxaaauucTT	882	PB1
  AL-DP-8376	uuguccuucxugaaaaaauTT	883	auuuuuucaxgaaggacaaTT	884	PB1
  AL-DP-8377	uguccuucxugaaaaaaugTT	885	cauuuuuucaxgaaggacaTT	886	PB1
  AL-DP-8378	guccuucxugaaaaaaugcTT	887	gcauuuuuucaxgaaggacTT	888	PB1
  AL-DP-8379	uccuucxugaaaaaaugcxTT	889	xgcauuuuuucaxgaaggaTT	890	PB1
  AL-DP-8380	aaxggxugxauugagggcaTT	891	ugcccucaauxcaxccxuuTT	892	PA
  AL-DP-8381	axggxugxauugagggcaaTT	893	uugcccucaauxcaxccxuTT	894	PA
  AL-DP-8382	xggxugxauugagggcaagTT	895	cuugcccucaauxcaxccxTT	896	PA
  AL-DP-8383	ggxugxauugagggcaagcTT	897	gcuugcccucaauxcaxccTT	898	PA
  AL-DP-8384	gxugxauugagggcaagcuTT	899	agcuugcccucaauxcaxcTT	900	PA
  AL-DP-8385	xugxauugagggcaagcuwTT	901	wagcuugcccucaauxcaxTT	902	PA
  AL-DP-8386	aaxgcuacuxuuugcuaucTT	903	gauagcaaaxaguagcxuuTT	904	PA
  AL-DP-8387	axgcuacuxuuugcuauccTT	905	ggauagcaaaxaguagcxuTT	906	PA
  AL-DP-8388	xgcuacuxuuugcuauccaTT	907	uggauagcaaaxaguagcxTT	908	PA
  AL-DP-8389	gcuacuxuuugcuauccauTT	909	auggauagcaaaxaguagcTT	910	PA
  AL-DP-8390	cuacuxuuugcuauccauaTT	911	uauggauagcaaaxaguagTT	912	PA
  AL-DP-8391	uacuxuuugcuauccauacTT	913	guauggauagcaaaxaguaTT	914	PA
  AL-DP-8392	acuxuuugcuauccauacuTT	915	aguauggauagcaaaxaguTT	916	PA
  AL-DP-8393	cuxuuugcuauccauacugTT	917	caguauggauagcaaaxagTT	918	PA
  AL-DP-8394	uxuuugcuauccauacuguTT	919	acaguauggauagcaaaxaTT	920	PA
  AL-DP-8395	xuuugcuauccauacugucTT	921	gacaguauggauagcaaaxTT	922	PA
  AL-DP-8396	uuugcuauccauacugucxTT	923	xgacaguauggauagcaaaTT	924	PA
  AL-DP-8397	ucggccxxcxaaagcagguTT	925	accugcuuuxgxxggccgaTT	926	PB2
  AL-DP-8398	cggccxxcxaaagcaggucTT	927	gaccugcuuuxgxxggccgTT	928	PB2
  AL-DP-8399	ggccxxcxaaagcaggucaTT	929	ugaccugcuuuxgxxggccTT	930	PB2
  AL-DP-8400	gccxxcxaaagcaggucaaTT	931	uugaccugcuuuxgxxggcTT	932	PB2
  AL-DP-8401	gacagxcagxcagcgaccaTT	933	uggucgcugxcugxcugucTT	934	PB2
  AL-DP-8402	acagxcagxcagcgaccaxTT	935	xuggucgcugxcugxcuguTT	936	PB2
  AL-DP-8403	xuxuhgaauxguuuaaaaaTT	937	uuuuuaaacxauuchaxaxTT	938	PB2
  AL-DP-8404	uguxgaauxguuuaaaaacTT	939	guuuuuaaacxauucxacaTT	940	PB2
  AL-DP-8405	guxgaauxguuuaaaaacsTT	941	sguuuuuaaacxauucxacTT	942	PB2
  AL-DP-8406	uguuucuxxxauauggcgcTT	943	gcgccauauxxxagaaacaTT	944	PB2
  AL-DP-8407	guuucuxxxauauggcgcaTT	945	ugcgccauauxxxagaaacTT	946	PB2
  AL-DP-8408	uuucuxxxauauggcgcauTT	947	augcgccauauxxxagaaaTT	948	PB2
  AL-DP-8409	uucuxxxauauggcgcauaTT	949	uaugcgccauauxxxagaaTT	950	PB2
  AL-DP-8410	ucuxxxauauggcgcauacTT	951	guaugcgccauauxxxagaTT	952	PB2
  AL-DP-8411	cuxxxauauggcgcauacuTT	953	aguaugcgccauauxxxagTT	954	PB2
  AL-DP-8412	uxxxauauggcgcauacucTT	955	gaguaugcgccauauxxxaTT	956	PB2
  AL-DP-8413	xxxuauggcgcauacucgTT		957	cgaguaugcgccauaxxxTT	958	PB2
  AL-DP-8414	xxauauggcgcauacucggTT	959	ccgaguaugcgccauauxxTT	960	PB2
  AL-DP-8415	xauauggcgcauacucgggTT	961	cccgaguaugcgccauauxTT	962	PB2
  AL-DP-8416	auauggcgcauacucgggcTT	963	gcccgaguaugcgccauauTT	964	PB2
  AL-DP-8417	uauggcgcauacucgggcaTT	965	ugcccgaguaugcgccauaTT	966	PB2
  AL-DP-8418	auggcgcauacucgggcauTT	967	augcccgaguaugcgccauTT	968	PB2
  AL-DP-8419	uggcgcauacucgggcaugTT	969	caugcccgaguaugcgccaTT	970	PB2
  AL-DP-8420	ggcgcauacucgggcauguTT	971	acaugcccgaguaugcgccTT	972	PB2
  AL-DP-8421	xxggcccccxcaaagccgaTT	973	ucggcuuugxgggggccxxTT	974	MP
  AL-DP-8422	xggcccccxcaaagccgaxTT	975	xucggcuuugxgggggccxTT	976	MP
  AL-DP-8423	xuuxacgcuxaccgugcccTT	977	gggcacgguxagcguxaaxTT	978	MP
  AL-DP-8424	uuxacgcuxaccgugcccaTT	979	ugggcacgguxagcguxaaTT	980	MP
  AL-DP-8425	uxacgcuxaccgugcccagTT	981	cugggcacgguxagcguxaTT	982	MP
  AL-DP-8426	xacgcuxaccgugcccagxTT	983	xcugggcacgguxagcguxTT	984	MP
  1in in vitro plaque forming assay in MCDK cells as described in Example 3.1

• TABLE 1G
  Exemplary iRNA agents for targeting influenza virus,and having 80%
  target coverage (criterium 1, see example 1) and 80% target
  efficiency (criterium 2, see example 1), but allowing for 1
  universal base in the non-seed region of the iRNA agent; x
  stands for the position of a universal base

  		SEQ		SEQ	Target
  Duplex	Sense strand sequence	ID	Antisense strand	ID	influenza
  identifier	(5′-3′)	NO:	sequence (5′-3′)	NO:	gene

  AL-DP-8427	acguacguucucucuaucxTT	985	xgauagagagaacguacguTT	986	MP
  AL-DP-8428	cucucuaucxucccgucagTT	987	cugacgggaxgauagagagTT	988	MP
  AL-DP-8429	ucucuaucxucccgucaggTT	989	ccugacgggaxgauagagaTT	990	MP
  AL-DP-8430	cucuaucxucccgucaggcTT	991	gccugacgggaxgauagagTT	992	MP
  AL-DP-8431	ucuaucxucccgucaggccTT	993	ggccugacgggaxgauagaTT	994	MP
  AL-DP-8432	cuaucxucccgucaggcccTT	995	gggccugacgggaxgauagTT	996	MP
  AL-DP-8433	uaucxucccgucaggccccTT	997	ggggccugacgggaxgauaTT	998	MP
  AL-DP-8434	aucxucccgucaggcccccTT	999	gggggccugacgggaxgauTT	1000	MP
  AL-DP-8435	ucxucccgucaggcccccuTT	1001	agggggccugacgggaxgaTT	1002	MP
  AL-DP-8436	cxucccgucaggcccccucTT	1003	gagggggccugacgggaxgTT	1004	MP
  AL-DP-8437	xucccgucaggcccccucaTT	1005	ugagggggccugacgggaxTT	1006	MP
  AL-DP-8438	aagccgagaucgcgcagaxTT	1007	xucugcgcgaucucggcuuTT	1008	MP
  AL-DP-8439	gaucuxgaggcucucauggTT	1009	ccaugagagccucxagaucTT	1010	MP
  AL-DP-8440	aucuxgaggcucucauggaTT	1011	uccaugagagccucxagauTT	1012	MP
  AL-DP-8441	ucucauggaxuggcuaaagTT	1013	cuuuagccaxuccaugagaTT	1014	MP
  AL-DP-8442	cucauggaxuggcuaaagaTT	1015	ucuuuagccaxuccaugagTT	1016	MP
  AL-DP-8443	ucauggaxuggcuaaagacTT	1017	gucuuuagccaxuccaugaTT	1018	MP
  AL-DP-8444	cauggaxuggcuaaagacaTT	1019	ugucuuuagccaxuccaugTT	1020	MP
  AL-DP-8445	auggaxuggcuaaagacaaTT	1021	uugucuuuagccaxuccauTT	1022	MP
  AL-DP-8446	uggaxuggcuaaagacaagTT	1023	cuugucuuuagccaxuccaTT	1024	MP
  AL-DP-8447	ggaxuggcuaaagacaagaTT	1025	ucuugucuuuagccaxuccTT	1026	MP
  AL-DP-8448	gaxuggcuaaagacaagacTT	1027	gucuugucuuuagccaxucTT	1028	MP
  AL-DP-8449	axuggcuaaagacaagaccTT	1029	ggucuugucuuuagccaxuTT	1030	MP
  AL-DP-8450	xuggcuaaagacaagaccaTT	1031	uggucuugucuuuagccaxTT	1032	MP
  AL-DP-8451	ccugucaccucugacuaaxTT	1033	xuuagucagaggugacaggTT	1034	MP
  AL-DP-8452	uuuguxuucacgcucaccgTT	1035	cggugagcgugaaxacaaaTT	1036	MP
  AL-DP-8453	uuguxuucacgcucaccguTT	1037	acggugagcgugaaxacaaTT	1038	MP
  AL-DP-8454	uguxuucacgcucaccgugTT	1039	cacggugagcgugaaxacaTT	1040	MP
  AL-DP-8455	guxuucacgcucaccgugcTT	1041	gcacggugagcgugaaxacTT	1042	MP
  AL-DP-8456	uxuucacgcucaccgugccTT	1043	ggcacggugagcgugaaxaTT	1044	MP
  AL-DP-8457	xuucacgcucaccgugcccTT	1045	gggcacggugagcgugaaxTT	1046	MP
  AL-DP-8458	aggacugcagcguagacgxTT	1047	xcgucuacgcugcaguccuTT	1048	MP
  AL-DP-8459	ugxaugggucucauauacaTT	1049	uguauaugagacccauxcaTT	1050	MP
  AL-DP-8460	gxaugggucucauauacaaTT	1051	uuguauaugagacccauxcTT	1052	MP
  AL-DP-8461	xaugggucucauauacaacTT	1053	guuguauaugagacccauxTT	1054	MP
  AL-DP-8462	augggucucauauacaacxTT	1055	xguuguauaugagacccauTT	1056	MP
  AL-DP-8463	ugugccacxugugagcagaTT	1057	ucugcucacaxguggcacaTT	1058	MP
  AL-DP-8464	gugccacxugugagcagauTT	1059	aucugcucacaxguggcacTT	1060	MP
  AL-DP-8465	gccacxugugagcagauugTT	1061	caaucugcucacaxguggcTT	1062	MP
  AL-DP-8466	ccacxugugagcagauugcTT	1063	gcaaucugcucacaxguggTT	1064	MP
  AL-DP-8467	cuaggcaxauggugcaggcTT	1065	gccugcaccauxugccuagTT	1066	MP
  AL-DP-8468	augagxacaauugggacucTT	1067	gagucccaauuguxcucauTT	1068	MP
  AL-DP-8469	ugagxacaauugggacucaTT	1069	ugagucccaauuguxcucaTT	1070	MP
  AL-DP-8470	uuugcaggcxuaccagaaaTT	1071	uuucugguaxgccugcaaaTT	1072	MP
  AL-DP-8471	uugcaggcxuaccagaaacTT	1073	guuucugguaxgccugcaaTT	1074	MP
  AL-DP-8472	ugcaggcxuaccagaaacgTT	1075	cguuucugguaxgccugcaTT	1076	MP
  AL-DP-8473	augcagcgxuucaagugauTT	1077	aucacuugaaxcgcugcauTT	1078	MP
  AL-DP-8474	ugcagcgxuucaagugaucTT	1079	gaucacuugaaxcgcugcaTT	1080	MP
  AL-DP-8475	gcagcgxuucaagugauccTT	1081	ggaucacuugaaxcgcugcTT	1082	MP
  AL-DP-8476	cagcgxuucaagugauccuTT	1083	aggaucacuugaaxcgcugTT	1084	MP
  AL-DP-8477	agcgxuucaagugauccucTT	1085	gaggaucacuugaaxcgcuTT	1086	MP
  AL-DP-8478	gcgxuucaagugauccucuTT	1087	agaggaucacuugaaxcgcTT	1088	MP
  AL-DP-8479	cauugggauxuugcacuugTT	1089	caagugcaaxaucccaaugTT	1090	MP
  AL-DP-8480	auugggauxuugcacuugaTT	1091	ucaagugcaaxaucccaauTT	1092	MP
  AL-DP-8481	uugggauxuugcacuugauTT	1093	aucaagugcaaxaucccaaTT	1094	MP
  AL-DP-8482	ugggauxuugcacuugauaTT	1095	uaucaagugcaaxaucccaTT	1096	MP
  AL-DP-8483	gggauxuugcacuugauauTT	1097	auaucaagugcaaxaucccTT	1098	MP
  AL-DP-8484	ggauxuugcacuugauauuTT	1099	aauaucaagugcaaxauccTT	1100	MP
  AL-DP-8485	gauxuugcacuugauauugTT	1101	caauaucaagugcaaxaucTT	1102	MP
  AL-DP-8486	auxuugcacuugauauuguTT	1103	acaauaucaagugcaaxauTT	1104	MP
  AL-DP-8487	uxuugcacuugauauugugTT	1105	cacaauaucaagugcaaxaTT	1106	MP
  AL-DP-8488	xuugcacuugauauuguggTT	1107	ccacaauaucaagugcaaxTT	1108	MP
  AL-DP-8489	aaaugcauuuaucgucgcxTT	1109	xgcgacgauaaaugcauuuTT	1110	MP
  AL-DP-8490	uaucgucgcxuuaaauacgTT	1111	cguauuuaaxgcgacgauaTT	1112	MP
  AL-DP-8491	aucgucgcxuuaaauacggTT	1113	ccguauuuaaxgcgacgauTT	1114	MP
  AL-DP-8492	ucgucgcxuuaaauacgguTT	1115	accguauuuaaxgcgacgaTT	1116	MP
  AL-DP-8493	cgucgcxuuaaauacgguuTT	1117	aaccguauuuaaxgcgacgTT	1118	MP
  AL-DP-8494	gucgcxuuaaauacgguuuTT	1119	aaaccguauuuaaxgcgacTT	1120	MP
  AL-DP-8495	ucgcxuuaaauacgguuugTT	1121	caaaccguauuuaaxgcgaTT	1122	MP
  AL-DP-8496	cgcxuuaaauacgguuugaTT	1123	ucaaaccguauuuaaxgcgTT	1124	MP
  AL-DP-8497	gcxuuaaauacgguuugaaTT	1125	uucaaaccguauuuaaxgcTT	1126	MP
  AL-DP-8498	cxuuaaauacgguuugaaaTT	1127	uuucaaaccguauuuaaxgTT	1128	MP
  AL-DP-8499	xuuaaauacgguuugaaaaTT	1129	uuuucaaaccguauuuaaxTT	1130	MP
  AL-DP-8500	gguuugaaaagagggccuxTT	1131	xaggcccucuuuucaaaccTT	1132	MP
  AL-DP-8501	xuugaaaagagggccuucuTT	1133	agaaggcccucuuuucaaxTT	1134	MP
  AL-DP-8502	aaaaxagggccuucuacggTT	1135	ccguagaaggcccuxuuuuTT	1136	MP
  AL-DP-8503	aaagagggccuucuacggxTT	1137	xccguagaaggcccucuuuTT	1138	MP
  AL-DP-8504	guxccugagucuaugagggTT	1139	cccucauagacucaggxacTT	1140	MP
  AL-DP-8505	uxccugagucuaugagggaTT	1141	ucccucauagacucaggxaTT	1142	MP
  AL-DP-8506	xccugagucuaugagggaaTT	1143	uucccucauagacucaggxTT	1144	MP
  AL-DP-8507	ugagucuaugagggaagaxTT	1145	xucuucccucauagacucaTT	1146	MP
  AL-DP-8508	cagaxugcuguggauguugTT	1147	caacauccacagcaxucugTT	1148	MP
  AL-DP-8509	agaxugcuguggauguugaTT	1149	ucaacauccacagcaxucuTT	1150	MP
  AL-DP-8510	gaxugcuguggauguugacTT	1151	gucaacauccacagcaxucTT	1152	MP
  AL-DP-8511	axugcuguggauguugacgTT	1153	cgucaacauccacagcaxuTT	1154	MP
  AL-DP-8512	xugcuguggauguugacgaTT	1155	ucgucaacauccacagcaxTT	1156	MP
  AL-DP-8513	xucaaggcaccaaacgaucTT	1157	gaucguuuggugccuugaxTT	1158	NP
  AL-DP-8514	aggcaccaaacgaucuuaxTT	1159	xuaagaucguuuggugccuTT	1160	NP
  AL-DP-8515	uaugaxcagauggaaacugTT	1161	caguuuccaucugxucauaTT	1162	NP
  AL-DP-8516	augaxcagauggaaacuggTT	1163	ccaguuuccaucugxucauTT	1164	NP
  AL-DP-8517	ugaxcagauggaaacugguTT	1165	accaguuuccaucugxucaTT	1166	NP
  AL-DP-8518	gaxcagauggaaacuggugTT	1167	caccaguuuccaucugxucTT	1168	NP
  AL-DP-8519	axcagauggaaacugguggTT	1169	ccaccaguuuccaucugxuTT	1170	NP
  AL-DP-8520	aacugguggxgaacgccagTT	1171	cuggcguucxccaccaguuTT	1172	NP
  AL-DP-8521	acugguggxgaacgccagaTT	1173	ucuggcguucxccaccaguTT	1174	NP
  AL-DP-8522	cugguggxgaacgccagaaTT	1175	uucuggcguucxccaccagTT	1176	NP
  AL-DP-8523	ugguggxgaacgccagaauTT	1177	auucuggcguucxccaccaTT	1178	NP
  AL-DP-8524	gguggxgaacgccagaaugTT	1179	cauucuggcguucxccaccTT	1180	NP
  AL-DP-8525	guggxgaacgccagaaugcTT	1181	gcauucuggcguucxccacTT	1182	NP
  AL-DP-8526	ccagaaugcxacugagaucTT	1183	gaucucaguxgcauucuggTT	1184	NP
  AL-DP-8527	cagaaugcxacugagaucaTT	1185	ugaucucaguxgcauucugTT	1186	NP
  AL-DP-8528	agaaugcxacugagaucagTT	1187	cugaucucaguxgcauucuTT	1188	NP
  AL-DP-8529	gaugugcacxgaacucaaaTT	1189	uuugaguucxgugcacaucTT	1190	NP
  AL-DP-8530	augugcacxgaacucaaacTT	1191	guuugaguucxgugcacauTT	1192	NP
  AL-DP-8531	ugugcacxgaacucaaacuTT	1193	aguuugaguucxgugcacaTT	1194	NP
  AL-DP-8532	gugcacxgaacucaaacucTT	1195	gaguuugaguucxgugcacTT	1196	NP
  AL-DP-8533	ugcacxgaacucaaacucaTT	1197	ugaguuugaguucxgugcaTT	1198	NP
  AL-DP-8534	gcacxgaacucaaacucagTT	1199	cugaguuugaguucxgugcTT	1200	NP
  AL-DP-8535	caxaacagcauaacaauagTT	1201	cuauuguuaugcuguuxugTT	1202	NP
  AL-DP-8536	axaacagcauaacaauagaTT	1203	ucuauuguuaugcuguuxuTT	1204	NP
  AL-DP-8537	xaacagcauaacaauagagTT	1205	cucuauuguuaugcuguuxTT	1206	NP
  AL-DP-8538	aacaauagagagaaugguxTT	1207	xaccauucucucuauuguuTT	1208	NP
  AL-DP-8539	ugaugauxuggcauuccaaTT	1209	uuggaaugccaxaucaucaTT	1210	NP
  AL-DP-8540	augugxucucugaugcaagTT	1211	cuugcaucagagaxcacauTT	1212	NP
  AL-DP-8541	ugugxucucugaugcaaggTT	1213	ccuugcaucagagaxcacaTT	1214	NP
  AL-DP-8542	agxauugcauaugagagaaTT	1215	uucucucauaugcaauxcuTT	1216	NP
  AL-DP-8543	gxauugcauaugagagaauTT	1217	auucucucauaugcaauxcTT	1218	NP
  AL-DP-8544	xauugcauaugagagaaugTT	1219	cauucucucauaugcaauxTT	1220	NP
  AL-DP-8545	ugcxuaugagagaaugugcTT	1221	gcacauucucucauaxgcaTT	1222	NP
  AL-DP-8546	auaugagagaaugugcaaxTT	1223	xuugcacauucucucauauTT	1224	NP
  AL-DP-8547	uaugaxagaaugugcaacaTT	1225	uguugcacauucuxucauaTT	1226	NP
  AL-DP-8548	augaxagaaugugcaacauTT	1227	auguugcacauucuxucauTT	1228	NP
  AL-DP-8549	aaugugcaaxauccucaaaTT	1229	uuugaggauxuugcacauuTT	1230	NP
  AL-DP-8550	augugcaaxauccucaaagTT	1231	cuuugaggauxuugcacauTT	1232	NP
  AL-DP-8551	ugugcaaxauccucaaaggTT	1233	ccuuugaggauxuugcacaTT	1234	NP
  AL-DP-8552	agggaaauuxcaaacagcaTT	1235	ugcuguuugxaauuucccuTT	1236	NP
  AL-DP-8553	gggaaauuxcaaacagcagTT	1237	cugcuguuugxaauuucccTT	1238	NP
  AL-DP-8554	ggaaauuxcaaacagcagcTT	1239	gcugcuguuugxaauuuccTT	1240	NP
  AL-DP-8555	gaaauuxcaaacagcagcaTT	1241	ugcugcuguuugxaauuucTT	1242	NP
  AL-DP-8556	aaauuxcaaacagcagcacTT	1243	gugcugcuguuugxaauuuTT	1244	NP
  AL-DP-8557	aauuxcaaacagcagcacaTT	1245	ugugcugcuguuugxaauuTT	1246	NP
  AL-DP-8558	auuxcaaacagcagcacaaTT	1247	uugugcugcuguuugxaauTT	1248	NP
  AL-DP-8559	gcacaaxgagcaaugauggTT	1249	ccaucauugcucxuugugcTT	1250	NP
  AL-DP-8560	cacaaxgagcaaugauggaTT	1251	uccaucauugcucxuugugTT	1252	NP
  AL-DP-8561	acauucccxuauacuggagTT	1253	cuccaguauaxgggaauguTT	1254	PB1
  AL-DP-8562	cauucccxuauacuggagaTT	1255	ucuccaguauaxgggaaugTT	1256	PB1
  AL-DP-8563	ggagaxccuccauacagccTT	1257	ggcuguauggaggxucuccTT	1258	PB1
  AL-DP-8564	gagaxccuccauacagccaTT	1259	uggcuguauggaggxucucTT	1260	PB1
  AL-DP-8565	agaxccuccauacagccauTT	1261	auggcuguauggaggxucuTT	1262	PB1
  AL-DP-8566	gaxccuccauacagccaugTT	1263	cauggcuguauggaggxucTT	1264	PB1
  AL-DP-8567	ccxccauacagccauggaaTT	1265	uuccauggcuguauggxggTT	1266	PB1
  AL-DP-8568	cxccauacagccauggaacTT	1267	guuccauggcuguauggxgTT	1268	PB1
  AL-DP-8569	xccauacagccauggaacaTT	1269	uguuccauggcuguauggxTT	1270	PB1
  AL-DP-8570	auacagccauggaacaggxTT	1271	xccuguuccauggcuguauTT	1272	PB1
  AL-DP-8571	uggaacaggxacaggauacTT	1273	guauccuguxccuguuccaTT	1274	PB1
  AL-DP-8572	ggaacaggxacaggauacaTT	1275	uguauccuguxccuguuccTT	1276	PB1
  AL-DP-8573	gaacaggxacaggauacacTT	1277	guguauccuguxccuguucTT	1278	PB1
  AL-DP-8574	aacaggxacaggauacaccTT	1279	gguguauccuguxccuguuTT	1280	PB1
  AL-DP-8575	acaggxacaggauacaccaTT	1281	ugguguauccuguxccuguTT	1282	PB1
  AL-DP-8576	caggxacaggauacaccauTT	1283	augguguauccuguxccugTT	1284	PB1
  AL-DP-8577	aggxacaggauacaccaugTT	1285	caugguguauccuguxccuTT	1286	PB1
  AL-DP-8578	ggxacaggauacaccauggTT	1287	ccaugguguauccuguxccTT	1288	PB1
  AL-DP-8579	gxacaggauacaccauggaTT	1289	uccaugguguauccuguxcTT	1290	PB1
  AL-DP-8580	xacaggauacaccauggacTT	1291	guccaugguguauccuguxTT	1292	PB1
  AL-DP-8581	aggauacaccauggacacxTT	1293	xguguccaugguguauccuTT	1294	PB1
  AL-DP-8582	acacxgucaacagaacacaTT	1295	uguguucuguugacxguguTT	1296	PB1
  AL-DP-8583	guxuuggaagcaauggcuuTT	1297	aagccauugcuuccaaxacTT	1298	PB1
  AL-DP-8584	uxuuggaagcaauggcuuuTT	1299	aaagccauugcuuccaaxaTT	1300	PB1
  AL-DP-8585	xuuggaagcaauggcuuucTT	1301	gaaagccauugcuuccaaxTT	1302	PB1
  AL-DP-8586	gcaauggcuuuccuugaaxTT	1303	xuucaaggaaagccauugcTT	1304	PB1
  AL-DP-8587	caauggcxuuccuugaagaTT	1305	ucuucaaggaaxgccauugTT	1306	PB1
  AL-DP-8588	ugaaaacucxugucuugaaTT	1307	uucaagacaxgaguuuucaTT	1308	PB1
  AL-DP-8589	gaaaacucxugucuugaaaTT	1309	uuucaagacaxgaguuuucTT	1310	PB1
  AL-DP-8590	aaaacucxugucuugaaacTT	1311	guuucaagacaxgaguuuuTT	1312	PB1
  AL-DP-8591	cgccagacxuaugacuggaTT	1313	uccagucauaxgucuggcgTT	1314	PB1
  AL-DP-8592	gccagacxuaugacuggacTT	1315	guccagucauaxgucuggcTT	1316	PB1
  AL-DP-8593	ccagacxuaugacuggacaTT	1317	uguccagucauaxgucuggTT	1318	PB1
  AL-DP-8594	caugaccaaxaaaauggucTT	1319	gaccauuuuxuuggucaugTT	1320	PB1
  AL-DP-8595	augaccaaxaaaauggucaTT	1321	ugaccauuuuxuuggucauTT	1322	PB1
  AL-DP-8596	ugaccaaxaaaauggucacTT	1323	gugaccauuuuxuuggucaTT	1324	PB1
  AL-DP-8597	gaccaaxaaaauggucacaTT	1325	ugugaccauuuuxuuggucTT	1326	PB1
  AL-DP-8598	accaaxaaaauggucacacTT	1327	gugugaccauuuuxuugguTT	1328	PB1
  AL-DP-8599	ccaaxaaaauggucacacaTT	1329	ugugugaccauuuuxuuggTT	1330	PB1
  AL-DP-8600	caaxaaaauggucacacaaTT	1331	uugugugaccauuuuxuugTT	1332	PB1
  AL-DP-8601	axaaaauggucacacaaagTT	1333	cuuugugugaccauuuuxuTT	1334	PB1
  AL-DP-8602	ugacaxugaacacaaugacTT	1335	gucauuguguucaxugucaTT	1336	PB1
  AL-DP-8603	aaxaugaugacuaacucacTT	1337	gugaguuagucaucauxuuTT	1338	PB1
  AL-DP-8604	axaugaugacuaacucacaTT	1339	ugugaguuagucaucauxuTT	1340	PB1
  AL-DP-8605	xaugaugacuaacucacaaTT	1341	uugugaguuagucaucauxTT	1342	PB1
  AL-DP-8606	gaugacuaacucacaagaxTT	1343	xucuugugaguuagucaucTT	1344	PB1
  AL-DP-8607	gacaaxaccaaauggaaugTT	1345	cauuccauuugguxuugucTT	1346	PB1
  AL-DP-8608	acaaxaccaaauggaaugaTT	1347	ucauuccauuugguxuuguTT	1348	PB1
  AL-DP-8609	caaxaccaaauggaaugagTT	1349	cucauuccauuugguxuugTT	1350	PB1
  AL-DP-8610	aaxaccaaauggaaugagaTT	1351	ucucauuccauuugguxuuTT	1352	PB1
  AL-DP-8611	axaccaaauggaaugagaaTT	1353	uucucauuccauuugguxuTT	1354	PB1
  AL-DP-8612	xaccaaauggaaugagaauTT	1355	auucucauuccauuugguxTT	1356	PB1
  AL-DP-8613	caaauggaaugagaaucaxTT	1357	xugauucucauuccauuugTT	1358	PB1
  AL-DP-8614	auugcxccuauaauguucuTT	1359	agaacauuauaggxgcaauTT	1360	PB1
  AL-DP-8615	uugcxccuauaauguucucTT	1361	gagaacauuauaggxgcaaTT	1362	PB1
  AL-DP-8616	gcxccuauaauguucucaaTT	1363	uugagaacauuauaggxgcTT	1364	PB1
  AL-DP-8617	cxccuauaauguucucaaaTT	1365	uuugagaacauuauaggxgTT	1366	PB1
  AL-DP-8618	uacgxacacaaauaccagcTT	1367	gcugguauuuguguxcguaTT	1368	PB1
  AL-DP-8619	cgxacacaaauaccagcagTT	1369	cugcugguauuuguguxcgTT	1370	PB1
  AL-DP-8620	gxacacaaauaccagcagaTT	1371	ucugcugguauuuguguxcTT	1372	PB1
  AL-DP-8621	acacaxauaccagcagaaaTT	1373	uuucugcugguauxuguguTT	1374	PB1
  AL-DP-8622	cacaxauaccagcagaaauTT	1375	auuucugcugguauxugugTT	1376	PB1
  AL-DP-8623	acaaauaccxgcagaaaugTT	1377	cauuucugcxgguauuuguTT	1378	PB1
  AL-DP-8624	caaauaccxgcagaaaugcTT	1379	gcauuucugcxgguauuugTT	1380	PB1
  AL-DP-8625	aaauaccxgcagaaaugcuTT	1381	agcauuucugcxgguauuuTT	1382	PB1
  AL-DP-8626	aauaccagcxgaaaugcuuTT	1383	aagcauuucxgcugguauuTT	1384	PB1
  AL-DP-8627	auaccagcxgaaaugcuugTT	1385	caagcauuucxgcugguauTT	1386	PB1
  AL-DP-8628	uaccagcxgaaaugcuugcTT	1387	gcaagcauuucxgcugguaTT	1388	PB1
  AL-DP-8629	accagcxgaaaugcuugcaTT	1389	ugcaagcauuucxgcugguTT	1390	PB1
  AL-DP-8630	ccagcxgaaaugcuugcaaTT	1391	uugcaagcauuucxgcuggTT	1392	PB1
  AL-DP-8631	agaaaauxgagaaaauaagTT	1393	cuuauuuucucxauuuucuTT	1394	PB1

• TABLE 1H
  Exemplary iRNA agents for targeting influenza virus derived from agents listed in Table
  1C by stabilization towards nucleolytic degradation by nucleotide modifications

  	Corre-					Target
  	sponding		SEQ		SEQ	influ-
  Duplex	unmodified		ID	Antisense strand	ID	enza
  identifier	duplex1	Sense strand sequence (5′-3′)	NO:	sequence (5′-3′)	NO:	gene
  AL-DP-2336	AL-DP-2316	cmumumcmagaumcmgaacmggumcmumaTT	1395	umagaccguucgaucugaagTT	1396	PB2
  AL-DP-2337	AL-DP-2317	cmagaumcmgaacmggumcmumaacmaTT	1397	uguumagaccguucgaucugTT	1398	PB2
  AL-DP-2338	AL-DP-2318	agaumcmgaacmggumcmumaacmagTT	1399	cuguumagaccguucgaucuTT	1400	PB2
  AL-DP-2339	AL-DP-2319	cmaaaaumgcmumaumaagumacmcmaTT	1401	uggumacuumaumagcmauuuugTT	1402	PB2
  AL-DP-2340	AL-DP-2320	umumcmagaumcmgaacmggumcmumaaTT	1403	uumagaccguucgaucugaaTT	1404	PB2
  AL-DP-2341	AL-DP-2321	umacmcmacmaumumcmcmcmumumaumacmumTT	1405	agumaumaagggaauguggumaTT	1406	PB2
  AL-DP-2342	AL-DP-2327	umumumgagagagaagggumacmumTT	1407	agumacccuucucucucmaaaTT	1408	NP
  AL-DP-2343	AL-DP-2328	aggcmaacmgaacmcmcmgaumcmgumTT	1409	acgaucggguucguumgccuTT	1410	NP
  AL-DP-2344	AL-DP-2329	ggcmaacmgaacmcmcmgaumcmgumgTT	1411	cmacgaucggguucguugccTT	1412	NP
  AL-DP-2345	AL-DP-2330	cmaacmgaacmcmcmgaumcmgumgcmcmTT	1413	ggcmacgaucggguucguugTT	1414	NP
  AL-DP-2346	AL-DP-2331	gcmaacmgaacmcmcmgaumcmgumgcmTT	1415	gcmacgaucggguucguugcTT	1416	NP
  AL-DP-2347	AL-DP-2332	gaaaaggcmaacmgaacmcmcmgaTT	1417	ucggguucguumgccuuuucTT	1418	NP
  AL-DP-2352	AL-DP-2348	umgcmaumgaumaaaggcmagumcmcmTT	1419	ggacugccuuumaucmaugcmaTT	1420	PB2
  AL-DP-2353	AL-DP-2349	aumggggaumgaumcmggaaumaumTT	1421	aumauuccgaucmauccccmauTT	1422	PB2
  AL-DP-2354	AL-DP-2350	umggggaumgaumcmggaaumaumumTT	1423	aaumauuccgaucmauccccmaTT	1424	PB2
  AL-DP-2355	AL-DP-2351	gaaacmgggacmumcmumagcmaumaTT	1425	umaugcumagagucccguuucTT	1426	PB2
  AL-DP-2369	AL-DP-2356	agacmumumumgumgcmgacmaaumgcmTT	1427	gcmauugucgcmacmaaagucuTT	1428	PA
  AL-DP-2370	AL-DP-2357	gacmumumumgumgcmgacmaaumgcmumTT	1429	agcmauugucgcmacmaaagucTT	1430	PA
  AL-DP-2371	AL-DP-2358	umcmumaumgggaumumcmcmumumumcmgumTT	1431	acgaaaggaaucccmaumagaTT	1432	PA
  AL-DP-2372	AL-DP-2359	cmumaumgggaumumcmcmumumumcmgumcmTT	1433	gacgaaaggaaucccmaumagTT	1434	PA
  AL-DP-2373	AL-DP-2360	aumgumggaumggaumumcmgaacmcmTT	1435	gguucgaauccmauccmacmauTT	1436	PA
  AL-DP-2374	AL-DP-2361	umgumggaumggaumumcmgaacmcmgTT	1437	cgguucgaauccmauccmacmaTT	1438	PA
  AL-DP-2375	AL-DP-2362	gumggaumggaumumcmgaacmcmgaTT	1439	ucgguucgaauccmauccmacTT	1440	PA
  AL-DP-2376	AL-DP-2363	umggaumggaumumcmgaacmcmgaaTT	1441	uucgguucgaauccmauccmaTT	1442	PA
  AL-DP-2377	AL-DP-2364	ggaumggaumumcmgaacmcmgaacmTT	1443	guucgguucgaauccmauccTT	1444	PA
  AL-DP-2378	AL-DP-2365	gaumggaumumcmgaacmcmgaacmgTT	1445	cguucgguucgaauccmaucTT	1446	PA
  AL-DP-2379	AL-DP-2366	aumggaumumcmgaacmcmgaacmggTT	1447	ccguucgguucgaauccmauTT	1448	PA
  AL-DP-2380	AL-DP-2367	umggaumumcmgaacmcmgaacmggcmTT	1449	gccguucgguucgaauccmaTT	1450	PA
  AL-DP-2381	AL-DP-2368	aumcmumcmcmacmaacmumcmgaggggTT	1451	ccccucgaguumgumggagauTT	1452	PA
  1duplex identifier of siRNA agent of Table 1C having an identical nucleotide sequence when nucleotide modifications are disregarded

• TABLE 1I
  Activity of the modified RNAi agents listed in Table 1B and H towards inhibition
  of influenza gene expression in the assays described in Example 3

  	Target		ELISA (MDCK	ELISA (Vero	Plasmid
  Duplex	influenza	% remaining	cells),	cells),	expression,
  identifier	gene	infectivity1	% inhibition2	% inhibition3	% inhibition4

  AL-DP-2289	PB1	104%	17	−31
  AL-DP-2290	NP	29%	−8	−36	61
  AL-DP-2291	NP	34%	−28	−30	5
  AL-DP-2292	NP	34%	−25	−14	36
  AL-DP-2293	MP	40%	−7	−74
  AL-DP-2294	MP	78%	−19	−53
  AL-DP-2295	MP	67%	−39	−85
  AL-DP-2296	MP	61%	−21
  AL-DP-2297	MP		−15	−27
  AL-DP-2298	MP		−21	11
  AL-DP-2299	MP		−23	12
  AL-DP-2300	MP		−37	−62
  AL-DP-2301	MP		−13	−62
  AL-DP-2302	MP		−30	−51
  AL-DP-2303	MP		1	−44
  AL-DP-2304	MP		−16	−38
  AL-DP-2305	MP	45%	28	−42
  AL-DP-2306	MP	46%	−1	−46
  AL-DP-2307	MP	39%	11	−18
  AL-DP-2308	MP		−5	15
  AL-DP-2309	MP		19	−42
  AL-DP-2310	MP		−1	−29
  AL-DP-2311	MP		−46	−45
  AL-DP-2312	MP		−66	−31
  AL-DP-2336	PB2		11	−15
  AL-DP-2337	PB2		6	−23
  AL-DP-2338	PB2		5	5
  AL-DP-2339	PB2		33	−38
  AL-DP-2340	PB2		19	−46
  AL-DP-2341	PB2		14	−5
  AL-DP-2342	NP		9	3	42
  AL-DP-2343	NP		−32	−20	29
  AL-DP-2344	NP		−27	−10	22
  AL-DP-2345	NP		15	−29	39
  AL-DP-2346	NP		−22	−32	29
  AL-DP-2347	NP		−9	−24	65
  AL-DP-2352	PB2		3	17	5
  AL-DP-2353	PB2		−44	9	28
  AL-DP-2354	PB2		−54	−9	27
  AL-DP-2355	PB2	<25	13	45	59
  AL-DP-2369	PA	<75	40	3	2
  AL-DP-2370	PA		28	27	67
  AL-DP-2371	PA		15	−24	12
  AL-DP-2372	PA		18	−29	73
  AL-DP-2373	PA	<25	37	27	71
  AL-DP-2374	PA	<75	27	−48	9
  AL-DP-2375	PA	<25	44	53	87
  AL-DP-2376	PA		4	−40	38
  AL-DP-2377	PA	<25	21	39	65
  AL-DP-2378	PA		−50	−75	11
  AL-DP-2379	PA		−39	−20	19
  AL-DP-2380	PA		0	−27	31
  AL-DP-2381	PA		−52	−54	43
  1in in vitro plaque forming assay in MCDK cells as described in Example 3.1;
  2in in vitro ELISA assay in MCDK cells as described in Example 3.2:
  3in in vitro ELISA assay in MCDK cells as described in Example 3.2;
  4in in vitro ELISA assay in MCDK cells as described in Example 3.2; negative values indicate that target gene expression was enhanced in treated cells compared to controls

• TABLE 2
  Concentration at 50% inhibition (IC50) for selected
  RNAi agents of Table 1

  		Target
  	Duplex	influenza
  	identifier	gene	IC50 (nM)

  	AL-DP-2364	PA	0.22
  	AL-DP-2377	PA	2.15
  	AL-DP-7595	PB2	0.54
  	AL-DP-7611	PB2	0.075
  	AL-DP-7617	NP	0.57
  	AL-DP-7622	NP	0.74
  	AL-DP-7633	NP	˜90
  	AL-DP-7660	M	261
  	AL-DP-7669	M	0.79

• The antisense strand of an iRNA agent should be equal to or at least, 14, 15, 16 17, 18, 19, 25, 29, 40, or 50 nucleotides in length. It should be equal to or less than 60, 50, 40, or 30, nucleotides in length. Preferred ranges are 15-30, 17 to 25, 19 to 23, and 19 to 21 nucleotides in length.
• The sense strand of an iRNA agent should be equal to or at least 14, 15, 16 17, 18, 19, 25, 29, 40, or 50 nucleotides in length. It should be equal to or less than 60, 50, 40, or 30 nucleotides in length. Preferred ranges are 15-30, 17 to 25, 19 to 23, and 19 to 21 nucleotides in length.
• The double stranded portion of an iRNA agent should be equal to or at least, 15, 16 17, 18, 19, 20, 21, 22, 23, 24, 25, 29, 40, or 50 nucleotide pairs in length. It should be equal to or less than 60, 50, 40, or 30 nucleotides pairs in length. Preferred ranges are 15-30, 17 to 25, 19 to 23, and 19 to 21 nucleotides pairs in length.
• Generally, the iRNA agents of the instant invention include a region of sufficient complementarity to the respective influenza virus gene, and are of sufficient length in terms of nucleotides, that the iRNA agent, or a fragment thereof, can mediate down regulation of the influenza virus gene. It is not necessary that there be perfect complementarity between the iRNA agent and the target gene, but the correspondence must be sufficient to enable the iRNA agent, or a cleavage product thereof, to direct sequence specific silencing, e.g., by RNAi cleavage of an influenza virus RNA.
• Therefore, the iRNA agents of the instant invention include agents comprising a sense strand and antisense strand each comprising a sequence of at least 16, 17 or 18 nucleotides which is essentially identical, as defined below, to one of the sequences of Tables 1A-1H, except that not more than 1, 2 or 3 nucleotides per strand, respectively, have been substituted by other nucleotides (e.g. adenosine replaced by uracil), while essentially retaining the ability to inhibit influenza virus replication in cultured human cells infected with influenza virus, respectively. These agents will therefore possess at least 15 nucleotides identical to one of the sequences of Tables 1A-1H, but 1, 2 or 3 base mismatches with respect to either the target influenza virus RNA sequence or between the sense and antisense strand are introduced. Mismatches to the target influenza virus RNA sequence, particularly in the antisense strand, are most tolerated in the terminal regions and if present are preferably in a terminal region or regions, e.g., within 6, 5, 4, or 3 nucleotides of a 5′ and/or 3′ terminus, most preferably within 6, 5, 4, or 3 nucleotides of the 5′-terminus of the sense strand or the 3′-terminus of the antisense strand. The sense strand need only be sufficiently complementary with the antisense strand to maintain the overall double stranded character of the molecule.
• It is preferred that the sense and antisense strands be chosen such that the iRNA agent includes a single strand or unpaired region at one or both ends of the molecule. Thus, an iRNA agent contains sense and antisense strands, preferably paired to contain an overhang, e.g., one or two 5′ or 3′ overhangs but preferably a 3′ overhang of 2-3 nucleotides. Most embodiments will have a 3′ overhang. Preferred siRNA agents will have single-stranded overhangs, preferably 3′ overhangs, of 1 to 4, or preferably 2 or 3 nucleotides, in length, at one or both ends of the iRNA agent. The overhangs can be the result of one strand being longer than the other, or the result of two strands of the same length being staggered. The unpaired nucleotides forming the overhang can be ribonucleotides, or they can be deoxyribonucleotides, preferably thymidine. 5′-ends are preferably phosphorylated, or they may be unphosphorylated.
• Preferred lengths for the duplexed region are between 15 and 30, most preferably 18, 19, 20, 21, 22, and 23 nucleotides in length, e.g., in the siRNA agent range discussed above. siRNA agents can resemble in length and structure the natural Dicer processed products from long dsRNAs. Embodiments in which the two strands of the siRNA agent are linked, e.g., covalently linked, are also included. Hairpin, or other single strand structures which provide the required double stranded region, and preferably a 3′ overhang are also within the invention.
• Evaluation of Candidate iRNA Agents
• As noted above, the present invention provides a system for identifying siRNAs that are useful as inhibitors of influenza virus infection and/or replication. Since, as noted above, shRNAs are processed intracellularly to produce siRNAs having duplex portions with the same sequence as the stem structure of the shRNA, the system is equally useful for identifying shRNAs that are useful as inhibitors of influenza virus infection. For purposes of description this section will refer to siRNAs, but the system also encompasses corresponding shRNAs. Specifically, the present invention demonstrates the successful preparation of siRNAs targeted to viral genes to block or inhibit viral infection and/or replication. The techniques and reagents described herein can readily be applied to design potential new siRNAs, targeted to other genes or gene regions, and tested for their activity in inhibiting influenza virus infection and/or replication as discussed herein. It is expected that influenza viruses will continue to mutate and undergo reassortment and that it may be desirable to continue to develop and test new, differently targeted siRNAs.
• In various embodiments of the invention potential influenza virus inhibitors can be tested by introducing candidate siRNA(s) into cells (e.g., by exogenous administration or by introducing a vector or construct that directs endogenous synthesis of siRNA into the cell), or laboratory animals, prior to, simultaneously with, or after transfection with an influenza genome or portion thereof (e.g., within minutes, hours, or at most a few days) or prior to, simultaneously with, or after infection with influenza virus. Alternately, potential influenza virus inhibitors can be tested by introducing candidate siRNA(s) into cells or laboratory animals that are productively infected with influenza virus (i.e., cells that are producing progeny virus). The ability of the candidate siRNA(s) to reduce target transcript levels and/or to inhibit or suppress one or more aspects or features of the viral life cycle such as viral replication, pathogenicity, and/or infectivity is then assessed. For example, production of viral particles and/or production of viral proteins, etc., can be assessed either directly or indirectly using methods well known in the art.
• Cells or laboratory animals to which inventive siRNA compositions have been delivered (test cells/animals) may be compared with similar or comparable cells or laboratory animals that have not received the inventive composition (control cells/animals, e.g., cells/animals that have received either no siRNA or a control siRNA such as an siRNA targeted to a non-viral transcript such as GFP). The susceptibility of the test cells/animals to influenza virus infection can be compared with the susceptibility of control cells/animals to infection. Production of viral protein(s) and/or progeny virus may be compared in the test cells/animals relative to the control cells/animals. Other indicia of viral infectivity, replication, pathogenicity, etc., can be similarly compared. Standard in vitro antiviral assays may utilize inhibition of viral plaques, viral cytopathic effect (CPE), and viral hemagglutinin or other protein, inhibition of viral yield, etc. The CPE can be determined visually and by dye uptake. See, e.g., Sidwell, R. W. and Smee, D. F, “In vitro and in vivo assay systems for study of influenza virus inhibitors” Antiviral Res 2000, 48:1. Generally, test cells/animals and control cells/animals would be from the same species and, for cells, of similar or identical cell type. For example, cells from the same cell line could be compared. When the test cell is a primary cell, typically the control cell would also be a primary cell. Typically the same influenza virus strain would be used to compare test cells/animals and control cells/animals.
• For example, the ability of a candidate siRNA to inhibit influenza virus production may conveniently be determined by (i) delivering the candidate siRNA to cells (either prior to, at the same time as, or after exposure to influenza virus); (ii) assessing the production of viral hemagglutinin using a hemagglutinin assay, and (iii) comparing the amount of hemagglutinin produced in the presence of the siRNA with the amount produced in the absence of the siRNA. (The test need not include a control in which the siRNA is absent but may make use of previous information regarding the amount of hemagglutinin produced in the absence of inhibition.) A reduction in the amount of hemagglutinin strongly suggests a reduction in virus production. This assay may be used to test siRNAs that target any viral transcript and is not limited to siRNAs that target the transcript that encodes the viral hemagglutinin.
• The ability of a candidate siRNA to reduce the level of the target transcript may also be assessed by measuring the amount of the target transcript using, for example, Northern blots, nuclease protection assays, reverse transcription (RT)-PCR, real-time RT-PCR, microarray analysis, etc. The ability of a candidate siRNA to inhibit production of a polypeptide encoded by the target transcript (either at the transcriptional or post-transcriptional level) may be measured using a variety of antibody-based approaches including, but not limited to, Western blots, immunoassays, ELISA, flow cytometry, protein microarrays, etc. In general, any method of measuring the amount of either the target transcript or a polypeptide encoded by the target transcript may be used.
• In general, certain preferred influenza virus inhibitors reduce the target transcript level at least about 2 fold, preferably at least about 4 fold, more preferably at least about 8 fold, at least about 16 fold, at least about 64 fold or to an even greater degree relative to the level that would be present in the absence of the inhibitor (e.g., in a comparable control cell lacking the inhibitor). In general, certain preferred influenza virus inhibitors inhibit viral replication, so that the level of replication is lower in a cell containing the inhibitor than in a control cell not containing the inhibitor by at least about 2 fold, preferably at least about 4 fold, more preferably at least about 8 fold, at least about 16 fold, at least about 64 fold, at least about 100 fold, at least about 200 fold, or to an even greater degree.
• Certain preferred influenza virus inhibitors inhibit viral replication so that development of detectable viral titer is prevented for at least 24 hours, at least 36 hours, at least 48 hours, or at least 60 hours following administration of the siRNA and infection of the cells. Certain preferred influenza virus inhibitors prevent (i.e., reduce to undetectable levels) or significantly reduce viral replication for at least 24 hours, at least 36 hours, at least 48 hours, or at least 60 hours following administration of the siRNA. According to various embodiments of the invention a significant reduction in viral replication is a reduction to less than approximately 90% of the level that would occur in the absence of the siRNA, a reduction to less than approximately 75% of the level that would occur in the absence of the siRNA, a reduction to less than approximately 50% of the level that would occur in the absence of the siRNA, a reduction to less than approximately 25% of the level that would occur in the absence of the siRNA, or a reduction to less than approximately 10% of the level that would occur in the absence of the siRNA. Reduction in viral replication may be measured using any suitable method including, but not limited to, measurement of HA titer.
• Stability Testing, Modification, and Retesting of iRNA Agents
• A candidate iRNA agent can be evaluated with respect to stability, e.g., its susceptibility to cleavage by an endonuclease or exonuclease, such as when the iRNA agent is introduced into the body of a subject. Methods can be employed to identify sites that are susceptible to modification, particularly cleavage, e.g., cleavage by a component found in the body of a subject. Such methods may include the isolation and identification of most abundant fragments formed by degradation of the candidate iRNA agent after its incubation with isolated biological media in vitro, e.g. serum, plasma, sputum, cerebrospinal fluid, or cell or tissue homogenates, or after contacting a subject with the candidate iRNA agent in vivo, thereby identifying sites prone to cleavage. Such methods are, for example, without limitation, in co-owned International Application No. PCT/US2005/018931, filed on May 27, 2005.
• When sites susceptible to cleavage are identified, a further iRNA agent can be designed and/or synthesized wherein the potential cleavage site is made resistant to cleavage, e.g. by introduction of a 2′-modification on the site of cleavage, e.g. a 2′-O-methyl group. This further iRNA agent can be retested for stability, and this process may be iterated until an iRNA agent is found exhibiting the desired stability.
• In Vivo Testing
• An iRNA agent identified as being capable of inhibiting influenza virus gene expression can be tested for functionality in vivo in an animal model (e.g., in a mammal, such as in mouse or rat). For example, the iRNA agent can be administered to an animal, and the iRNA agent evaluated with respect to its biodistribution, stability, and its ability to inhibit influenza virus replication or reduce a biological or pathological process mediated at least in part by influenza virus.
• The iRNA agent can be administered directly to the target tissue, such as by injection, or the iRNA agent can be administered to the animal model in the same manner that it would be administered to a human. Preferably, the iRNA agent is delivered to the subject's airways, such as intranasally.
• The iRNA agent can also be evaluated for its intracellular distribution. The evaluation can include determining whether the iRNA agent was taken up into the cell. The evaluation can also include determining the stability (e.g., the half-life) of the iRNA agent. Evaluation of an iRNA agent in vivo can be facilitated by use of an iRNA agent conjugated to a traceable marker (e.g., a fluorescent marker such as fluorescein; a radioactive label, such as ³⁵S, ³²P, ³³P, or ³H; gold particles; or antigen particles for immunohistochemistry).
• The iRNA agent can be evaluated with respect to its ability to down regulate influenza virus replication. Levels of influenza virus gene expression in vivo can be measured, for example, by in situ hybridization, or by the isolation of RNA from tissue prior to and following exposure to the iRNA agent. Where the animal needs to be sacrificed in order to harvest the tissue, an untreated control animal will serve for comparison. Influenza virus RNA can be detected by any desired method, including but not limited to RT-PCR, Northern blot, branched-DNA assay, or RNAase protection assay. Alternatively, or additionally, influenza virus gene expression can be monitored by performing Western blot analysis or plaque forming assays on tissue extracts treated with the iRNA agent.
• Potential influenza virus inhibitors can be tested using any of variety of animal models that have been developed. Compositions comprising candidate siRNA(s), constructs or vectors capable of directing synthesis of such siRNAs within a host cell, or cells engineered or manipulated to contain candidate siRNAs may be administered to an animal prior to, simultaneously with, or following infection with an influenza virus. The ability of the composition to prevent viral infection and/or to delay or prevent appearance of influenza-related symptoms and/or lessen their severity relative to influenza-infected animals that have not received the potential influenza inhibitor is assessed. Such models include, but are not limited to, murine, chicken, ferret, and non-human primate models for influenza infection, all of which are known in the art and are used for testing the efficacy of potential influenza therapeutics and vaccines. See, e.g, Sidwell, R. W. and Smee, D. F, referenced above. Such models may involve use of naturally occurring influenza virus strains and/or strains that have been modified or adapted to existence in a particular host (e.g., the WSN or PR8 strains, which are adapted for replication in mice). The above animal models may also be used to establish the concentration necessary to achieve a certain desired effect (e.g., EC50).
• IRNA Chemistry
• Described herein are isolated iRNA agents, e.g., ds RNA agents that mediate RNAi to inhibit expression of a influenza virus gene.
• RNA agents discussed herein include otherwise unmodified RNA as well as RNA which has been modified, e.g., to improve efficacy, and polymers of nucleoside surrogates. Unmodified RNA refers to a molecule in which the components of the nucleic acid, namely sugars, bases, and phosphate moieties, are the same or essentially the same as that which occur in nature, preferably as occur naturally in the human body. The art has referred to rare or unusual, but naturally occurring, RNAs as modified RNAs, see, e.g., Limbach et al. Nucleic Acids Res. 22: 2183-2196, 1994. Such rare or unusual RNAs, often termed modified RNAs (apparently because they are typically the result of a post-transcriptional modification) are within the term unmodified RNA, as used herein. Modified RNA as used herein refers to a molecule in which one or more of the components of the nucleic acid, namely sugars, bases, and phosphate moieties, are different from that which occurs in nature, preferably different from that which occurs in the human body. While they are referred to as modified “RNAs,” they will of course, because of the modification, include molecules which are not RNAs. Nucleoside surrogates are molecules in which the ribophosphate backbone is replaced with a non-ribophosphate construct that allows the bases to the presented in the correct spatial relationship such that hybridization is substantially similar to what is seen with a ribophosphate backbone, e.g., non-charged mimics of the ribophosphate backbone. Examples of the above are discussed herein.
• Modifications described herein can be incorporated into any double-stranded RNA and RNA-like molecule described herein, e.g., an iRNA agent. It may be desirable to modify one or both of the antisense and sense strands of an iRNA agent. As nucleic acids are polymers of subunits or monomers, many of the modifications described below occur at a position which is repeated within a nucleic acid, e.g., a modification of a base, or a phosphate moiety, or the non-linking 0 of a phosphate moiety. In some cases the modification will occur at all of the subject positions in the nucleic acid but in many, and in fact in most, cases it will not. By way of example, a modification may only occur at a 3′ or 5′ terminal position, may only occur in a terminal region, e.g. at a position on a terminal nucleotide or in the last 2, 3, 4, 5, or 10 nucleotides of a strand. A modification may occur in a double strand region, a single strand region, or in both. E.g., a phosphorothioate modification at a non-linking O position may only occur at one or both termini, may only occur in a terminal regions, e.g., at a position on a terminal nucleotide or in the last 2, 3, 4, 5, or 10 nucleotides of a strand, or may occur in double strand and single strand regions, particularly at termini. Similarly, a modification may occur on the sense strand, antisense strand, or both. In some cases, the sense and antisense strand will have the same modifications or the same class of modifications, but in other cases the sense and antisense strand will have different modifications, e.g., in some cases it may be desirable to modify only one strand, e.g. the sense strand.
• Two prime objectives for the introduction of modifications into iRNA agents is their stabilization towards degradation in biological environments and the improvement of pharmacological properties, e.g. pharmacodynamic properties, which are further discussed below. Other suitable modifications to a sugar, base, or backbone of an iRNA agent are described in co-owned PCT Application No. PCT/US2004/01193, filed Jan. 16, 2004. An iRNA agent can include a non-naturally occurring base, such as the bases described in co-owned PCT Application No. PCT/US2004/011822, filed Apr. 16, 2004. An iRNA agent can include a non-naturally occurring sugar, such as a non-carbohydrate cyclic carrier molecule. Exemplary features of non-naturally occurring sugars for use in iRNA agents are described in co-owned PCT Application No. PCT/US2004/11829, filed Apr. 16, 2003.
• An iRNA agent can include an internucleotide linkage (e.g., the chiral phosphorothioate linkage) useful for increasing nuclease resistance. In addition, or in the alternative, an iRNA agent can include a ribose mimic for increased nuclease resistance. Exemplary internucleotide linkages and ribose mimics for increased nuclease resistance are described in co-owned PCT Application No. PCT/US2004/07070, filed on Mar. 8, 2004.
• An iRNA agent can include ligand-conjugated monomer subunits and monomers for oligonucleotide synthesis. Exemplary monomers are described in co-owned U.S. application Ser. No. 10/916,185, filed on Aug. 10, 2004.
• An iRNA agent can have a ZXY structure, such as is described in co-owned PCT Application No. PCT/US2004/07070, filed on Mar. 8, 2004.
• An iRNA agent can be complexed with an amphipathic moiety. Exemplary amphipathic moieties for use with iRNA agents are described in co-owned PCT Application No. PCT/US2004/07070, filed on Mar. 8, 2004.
• In another embodiment, the iRNA agent can be complexed to a delivery agent that features a modular complex. The complex can include a carrier agent linked to one or more of (preferably two or more, more preferably all three of): (a) a condensing agent (e.g., an agent capable of attracting, e.g., binding, a nucleic acid, e.g., through ionic or electrostatic interactions); (b) a fusogenic agent (e.g., an agent capable of fusing and/or being transported through a cell membrane); and (c) a targeting group, e.g., a cell or tissue targeting agent, e.g., a lectin, glycoprotein, lipid or protein, e.g., an antibody, that binds to a specified cell type. iRNA agents complexed to a delivery agent are described in co-owned PCT Application No. PCT/US2004/07070, filed on Mar. 8, 2004.
• An iRNA agent can have non-canonical pairings, such as between the sense and antisense sequences of the iRNA duplex. Exemplary features of non-canonical iRNA agents are described in co-owned PCT Application No. PCT/US2004/07070, filed on Mar. 8, 2004.
• Enhanced Nuclease Resistance
• An iRNA agent, e.g., an iRNA agent that targets influenza virus, can have enhanced resistance to nucleases.
• One way to increase resistance is to identify cleavage sites and modify such sites to inhibit cleavage, as described in co-owned U.S. Application No. 60/559,917, filed on May 4, 2004. For example, the dinucleotides 5′-ua-3′,5′-ca-3′,5′-ug-3′,5′-uu-3′, or 5′-ca-3′ can serve as cleavage sites. In certain embodiments, all the pyrimidines of an iRNA agent carry a 2′-modification in either the sense strand, the antisense strand, or both strands, and the iRNA agent therefore has enhanced resistance to endonucleases. Enhanced nuclease resistance can also be achieved by modifying the 5′ nucleotide, resulting, for example, in at least one 5′-uridine-adenine-3′ (5′-ua-3′) dinucleotide wherein the uridine is a 2′-modified nucleotide; at least one 5′-cytidine-adenine-3′ (5′-ca-3′) dinucleotide, wherein the 5′-cytidine is a 2′-modified nucleotide; at least one 5′-uridine-guanine-3′ (5′-ug-3′) dinucleotide, wherein the 5′-uridine is a 2′-modified nucleotide; at least one 5′-uridine-uridine-3′ (5′-uu-3′) dinucleotide, wherein the 5′-uridine is a 2′-modified nucleotide; or at least one 5′-cytidine-cytidine-3′ (5′-ca-3′) dinucleotide, wherein the 5′-cytidine is a 2′-modified nucleotide, as described in co-owned International Application No. PCT/US2005/018931, filed on May 27, 2005. The iRNA agent can include at least 2, at least 3, at least 4 or at least 5 of such dinucleotides. In a particularly preferred embodiment, the 5′ nucleotide in all occurrences of the sequence motifs 5′-ua-3′ and 5′-ca-3′ in either the sense strand, the antisense strand, or both strands is a modified nucleotide. Preferably, the 5′ nucleotide in all occurrences of the sequence motifs 5′-ua-3′,5′-ca-3′ and 5′-ug-3′ in either the sense strand, the antisense strand, or both strands is a modified nucleotide. More preferably, all pyrimidine nucleotides in the sense strand are modified nucleotides, and the 5′ nucleotide in all occurrences of the sequence motifs 5′-ua-3′ and 5′-ca-3′ in the antisense strand are modified nucleotides, or where the antisense strand does comprise neither of a 5′-ua-3′ and a 5′-ca-3′ motif, in all occurrences of the sequence motif 5′-ug-3′.
• Preferably, the 2′-modified nucleotides include, for example, a 2′-modified ribose unit, e.g., the 2′-hydroxyl group (OH) can be modified or replaced with a number of different “oxy” or “deoxy” substituents.
• Examples of “oxy”-2′ hydroxyl group modifications include alkoxy or aryloxy (OR, e.g., R═H, alkyl, cycloalkyl, aryl, aralkyl, heteroaryl or sugar); polyethyleneglycols (PEG), O(CH₂CH₂O)_nCH₂CH₂OR; “locked” nucleic acids (LNA) in which the 2′ hydroxyl is connected, e.g., by a methylene bridge, to the 4′ carbon of the same ribose sugar; O-AMINE and aminoalkoxy, O(CH₂)_nAMINE, (e.g., AMINE=NH₂; alkylamino, dialkylamino, heterocyclyl amino, arylamino, diaryl amino, heteroaryl amino, or diheteroaryl amino, ethylene diamine, polyamino). It is noteworthy that oligonucleotides containing only the methoxyethyl group (MOE), (OCH₂CH₂OCH₃, a PEG derivative), exhibit nuclease stabilities comparable to those modified with the robust phosphorothioate modification.
• “Deoxy” modifications include hydrogen (i.e. deoxyribose sugars, which are of particular relevance to the overhang portions of partially ds RNA); halo (e.g., fluoro); amino (e.g. NH₂; alkylamino, dialkylamino, heterocyclyl, arylamino, diaryl amino, heteroaryl amino, diheteroaryl amino, or amino acid); NH(CH₂CH₂NH)_nCH₂CH₂-AMINE (AMINE=NH₂; alkylamino, dialkylamino, heterocyclyl amino, arylamino, diaryl amino, heteroaryl amino, or diheteroaryl amino), —NHC(O)R (R=alkyl, cycloalkyl, aryl, aralkyl, heteroaryl or sugar), cyano; mercapto; alkyl-thio-alkyl; thioalkoxy; and alkyl, cycloalkyl, aryl, alkenyl and alkynyl, which may be optionally substituted with e.g., an amino functionality.
• Preferred substitutents are 2′-methoxyethyl, 2′-OCH₃, 2′-O-allyl, 2′-C-allyl, and 2′-fluoro.
• The inclusion of furanose sugars in the oligonucleotide backbone can also decrease endonucleolytic cleavage. An iRNA agent can be further modified by including a 3′ cationic group, or by inverting the nucleoside at the 3′-terminus with a 3′-3′ linkage. In another alternative, the 3′-terminus can be blocked with an aminoalkyl group, e.g., a 3′ C5-aminoalkyl dT. Other 3′ conjugates can inhibit 3′-5′ exonucleolytic cleavage. While not being bound by theory, a 3′ conjugate, such as naproxen or ibuprofen, may inhibit exonucleolytic cleavage by sterically blocking the exonuclease from binding to the 3′-end of oligonucleotide. Even small alkyl chains, aryl groups, or heterocyclic conjugates or modified sugars (D-ribose, deoxyribose, glucose etc.) can block 3′-5′-exonucleases.
• Nucleolytic cleavage can also be inhibited by the introduction of phosphate linker modifications, e.g., phosphorothioate linkages. Thus, preferred iRNA agents include nucleotide dimers enriched or pure for a particular chiral form of a modified phosphate group containing a heteroatom at a nonbridging position normally occupied by oxygen. The heteroatom can be S, Se, Nr₂, or Br₃. When the heteroatom is S, enriched or chirally pure Sp linkage is preferred. Enriched means at least 70, 80, 90, 95, or 99% of the preferred form. Modified phosphate linkages are particularly efficient in inhibiting exonucleolytic cleavage when introduced near the 5′- or 3′-terminal positions, and preferably the 5′-terminal positions, of an iRNA agent.
• 5′ conjugates can also inhibit 5′-3′ exonucleolytic cleavage. While not being bound by theory, a 5′ conjugate, such as naproxen or ibuprofen, may inhibit exonucleolytic cleavage by sterically blocking the exonuclease from binding to the 5′-end of oligonucleotide. Even small alkyl chains, aryl groups, or heterocyclic conjugates or modified sugars (D-ribose, deoxyribose, glucose etc.) can block 3′-5′-exonucleases.
• An iRNA agent can have increased resistance to nucleases when a duplexed iRNA agent includes a single-stranded nucleotide overhang on at least one end. In preferred embodiments, the nucleotide overhang includes 1 to 4, preferably 2 to 3, unpaired nucleotides. In a preferred embodiment, the unpaired nucleotide of the single-stranded overhang that is directly adjacent to the terminal nucleotide pair contains a purine base, and the terminal nucleotide pair is a G-C pair, or at least two of the last four complementary nucleotide pairs are G-C pairs. In further embodiments, the nucleotide overhang may have 1 or 2 unpaired nucleotides, and in an exemplary embodiment the nucleotide overhang is 5′-gc-3′. In preferred embodiments, the nucleotide overhang is on the 3′-end of the antisense strand. In one embodiment, the iRNA agent includes the motif 5′-cgc-3′ on the 3′-end of the antisense strand, such that a 2-nt overhang 5′-gc-3′ is formed.
• Thus, an iRNA agent can include modifications so as to inhibit degradation, e.g., by nucleases, e.g., endonucleases or exonucleases, found in the body of a subject. These monomers are referred to herein as NRMs, or Nuclease Resistance promoting Monomers, the corresponding modifications as NRM modifications. In many cases these modifications will modulate other properties of the iRNA agent as well, e.g., the ability to interact with a protein, e.g., a transport protein, e.g., serum albumin, or a member of the RISC, or the ability of the first and second sequences to form a duplex with one another or to form a duplex with another sequence, e.g., a target molecule.
• One or more different NRM modifications can be introduced into an iRNA agent or into a sequence of an iRNA agent. An NRM modification can be used more than once in a sequence or in an iRNA agent.
• NRM modifications include some which can be placed only at the terminus and others which can go at any position. Some NRM modifications can inhibit hybridization so it is preferable to use them only in terminal regions, and preferable to not use them at the cleavage site or in the cleavage region of a sequence which targets a subject sequence or gene, particularly on the antisense strand. They can be used anywhere in a sense strand, provided that sufficient hybridization between the two strands of the ds iRNA agent is maintained. In some embodiments it is desirable to put the NRM at the cleavage site or in the cleavage region of a sense strand, as it can minimize off-target silencing.
• In most cases, NRM modifications will be distributed differently depending on whether they are comprised on a sense or antisense strand. If on an antisense strand, modifications which interfere with or inhibit endonuclease cleavage should not be inserted in the region which is subject to RISC mediated cleavage, e.g., the cleavage site or the cleavage region (As described in Elbashir et al., 2001, Genes and Dev. 15: 188, hereby incorporated by reference). Cleavage of the target occurs about in the middle of a 20 or 21 nt antisense strand, or about 10 or 11 nucleotides upstream of the first nucleotide on the target mRNA which is complementary to the antisense strand. As used herein cleavage site refers to the nucleotides on either side of the cleavage site, on the target or on the iRNA agent strand which hybridizes to it. Cleavage region means the nucleotides within 1, 2, or 3 nucleotides of the cleavagee site, in either direction.
• Such modifications can be introduced into the terminal regions, e.g., at the terminal position or with 2, 3, 4, or 5 positions of the terminus, of a sense or antisense strand.
• Tethered Ligands
• The properties of an iRNA agent, including its pharmacological properties, can be influenced and tailored, for example, by the introduction of ligands, e.g. tethered ligands. In addition, pharmacological properties of an iRNA agent can be improved by incorporating a ligand in a formulation of the iRNA agent when the iRNA agent either has or does have a tethered ligand.
• A wide variety of entities, e.g., ligands, can be tethered to an iRNA agent or used as formulation conjugate or additive, e.g., to the carrier of a ligand-conjugated monomer subunit. Examples are described below in the context of a ligand-conjugated monomer subunit but that is only preferred, entities can be coupled at other points to an iRNA agent.
• Preferred moieties are ligands, which are coupled, preferably covalently, either directly or indirectly via an intervening tether, to the carrier. In preferred embodiments, the ligand is attached to the carrier via an intervening tether. The ligand or tethered ligand may be present on the ligand-conjugated monomer when the ligand-conjugated monomer is incorporated into the growing strand. In some embodiments, the ligand may be incorporated into a “precursor” ligand-conjugated monomer subunit after a “precursor” ligand-conjugated monomer subunit has been incorporated into the growing strand. For example, a monomer having, e.g., an amino-terminated tether, e.g., TAP-(CH₂)_nNH₂ may be incorporated into a growing sense or antisense strand. In a subsequent operation, i.e., after incorporation of the precursor monomer subunit into the strand, a ligand having an electrophilic group, e.g., a pentafluorophenyl ester or aldehyde group, can subsequently be attached to the precursor ligand-conjugated monomer by coupling the electrophilic group of the ligand with the terminal nucleophilic group of the precursor ligand-conjugated monomer subunit tether.
• In preferred embodiments, a ligand alters the distribution, targeting or lifetime of an iRNA agent into which it is incorporated. In preferred embodiments a ligand provides an enhanced affinity for a selected target, e.g., molecule, cell or cell type, compartment, e.g., a cellular or organ compartment, tissue, organ or region of the body, as, e.g., compared to a species absent such a ligand.
• Preferred ligands can improve transport, hybridization, and specificity properties and may also improve nuclease resistance of the resultant natural or modified oligoribonucleotide, or a polymeric molecule comprising any combination of monomers described herein and/or natural or modified ribonucleotides.
• Ligands in general can include therapeutic modifiers, e.g., for enhancing uptake; diagnostic compounds or reporter groups e.g., for monitoring distribution; cross-linking agents; nuclease-resistance conferring moieties; and natural or unusual nucleobases. General examples include lipophilic molecules, lipids, lectins, steroids (e.g., uvaol, hecigenin, diosgenin), terpenes (e.g., triterpenes, e.g., sarsasapogenin, Friedelin, epifriedelanol derivatized lithocholic acid), vitamins, carbohydrates (e.g., a dextran, pullulan, chitin, chitosan, inulin, cyclodextrin or hyaluronic acid), proteins, protein binding agents, integrin targeting molecules, polycationics, peptides, polyamines, and peptide mimics.
• The ligand may be a naturally occurring or recombinant or synthetic molecule, such as a synthetic polymer, e.g., a synthetic polyamino acid. Examples of polyamino acids include polylysine (PLL), poly L-aspartic acid, poly L-glutamic acid, styrene-maleic acid anhydride copolymer, poly(L-lactide-co-glycolied) copolymer, divinyl ether-maleic anhydride copolymer, N-(2-hydroxypropyl)methacrylamide copolymer (HMPA), polyethylene glycol (PEG), polyvinyl alcohol (PVA), polyurethane, poly(2-ethylacrylic acid), N-isopropylacrylamide polymers, or polyphosphazine. Example of polyamines include: polyethylenimine, polylysine (PLL), spermine, spermidine, polyamine, pseudopeptide-polyamine, peptidomimetic polyamine, dendrimer polyamine, arginine, amidine, protamine, cationic moieties, e.g., cationic lipid, cationic porphyrin, quaternary salt of a polyamine, or an alpha helical peptide.
• Ligands can also include targeting groups, e.g., a cell or tissue targeting agent, e.g., a thyrotropin, melanotropin, surfactant protein A, Mucin carbohydrate, a glycosylated polyaminoacid, transferrin, bisphosphonate, polyglutamate, polyaspartate, or an RGD peptide or RGD peptide mimetic.
• Ligands can be proteins, e.g., glycoproteins, lipoproteins, e.g. low density lipoprotein (LDL), or albumins, e.g. human serum albumin (HSA), or peptides, e.g., molecules having a specific affinity for a co-ligand, or antibodies e.g., an antibody, that binds to a specified cell type such as a cancer cell, endothelial cell, or bone cell. Ligands may also include hormones and hormone receptors. They can also include non-peptidic species, such as cofactors, multivalent lactose, multivalent galactose, N-acetyl-galactosamine, N-acetyl-glucosamine, multivalent mannose, or multivalent fucose. The ligand can be, for example, a lipopolysaccharide, an activator of p38 MAP kinase, or an activator of NF-κB.
• The ligand can be a substance, e.g, a drug, which can increase the uptake of the iRNA agent into the cell, for example, by disrupting the cell's cytoskeleton, e.g., by disrupting the cell's microtubules, microfilaments, and/or intermediate filaments. The drug can be, for example, taxon, vincristine, vinblastine, cytochalasin, nocodazole, japlakinolide, latrunculin A, phalloidin, swinholide A, indanocine, or myoservin.
• In one aspect, the ligand is a lipid or lipid-based molecule. Such a lipid or lipid-based molecule preferably binds a serum protein, e.g., human serum albumin (HSA). An HSA binding ligand allows for distribution of the conjugate to a target tissue, e.g., liver tissue, including parenchymal cells of the liver. Other molecules that can bind HSA can also be used as ligands. For example, neproxin or aspirin can be used. A lipid or lipid-based ligand can (a) increase resistance to degradation of the conjugate, (b) increase targeting or transport into a target cell or cell membrane, and/or (c) can be used to adjust binding to a serum protein, e.g., HSA.
• A lipid based ligand can be used to modulate, e.g., control the binding of the conjugate to a target tissue. For example, a lipid or lipid-based ligand that binds to HSA more strongly will be less likely to be targeted to the kidney and therefore less likely to be cleared from the body. A lipid or lipid-based ligand that binds to HSA less strongly can be used to target the conjugate to the kidney.
• In a preferred embodiment, the lipid based ligand binds HSA. Preferably, it binds HSA with a sufficient affinity such that the conjugate will be preferably distributed to a non-kidney tissue. However, it is preferred that the affinity not be so strong that the HSA-ligand binding cannot be reversed.
• In another aspect, the ligand is a moiety, e.g., a vitamin or nutrient, which is taken up by a target cell, e.g., a proliferating cell. These are particularly useful for treating disorders characterized by unwanted cell proliferation, e.g., of the malignant or non-malignant type, e.g., cancer cells. Exemplary vitamins include vitamin A, E, and K. Other exemplary vitamins include the B vitamins, e.g., folic acid, B12, riboflavin, biotin, pyridoxal or other vitamins or nutrients taken up by cancer cells.
• In another aspect, the ligand is a cell-permeation agent, preferably a helical cell-permeation agent. Preferably, the agent is amphipathic. An exemplary agent is a peptide such as tat or antennapedia. If the agent is a peptide, it can be modified, including a peptidylmimetic, invertomers, non-peptide or pseudo-peptide linkages, and use of D-amino acids. The helical agent is preferably an alpha-helical agent, which preferably has a lipophilic and a lipophobic phase.
• 5′-Phosphate Modifications
• In preferred embodiments, iRNA agents are 5′ phosphorylated or include a phosphoryl analog at the 5′ prime terminus. 5′-phosphate modifications of the antisense strand include those which are compatible with RISC mediated gene silencing. Suitable modifications include: 5′-monophosphate ((HO)2(O)P—O-5′); 5′-diphosphate ((HO)2(O)P—O—P(HO)(O)—O-5′); 5′-triphosphate ((HO)2(O)P—O—(HO)(O)P—O—P(HO)(O)—O-5′); 5′-guanosine cap (7-methylated or non-methylated) (7m-G-O-5′-(HO)(O)P—O—(HO)(O)P—O—P(HO)(O)—O-5′); 5′-adenosine cap (Appp), and any modified or unmodified nucleotide cap structure (N—O-5′-(HO)(O)P—O—(HO)(O)P—O—P(HO)(O)—O-5′); 5′-monothiophosphate (phosphorothioate; (HO)2(S)P—O-5′); 5′-monodithiophosphate (phosphorodithioate; (HO)(HS)(S)P—O-5′), 5′-phosphorothiolate ((HO)2(O)P—S-5′); any additional combination of oxygen/sulfur replaced monophosphate, diphosphate and triphosphates (e.g. 5′-alpha-thiotriphosphate, 5′-gamma-thiotriphosphate, etc.), 5′-phosphoramidates ((HO)2(O)P—NH-5′, (HO)(NH2)(O)P—O-5′), 5′-alkylphosphonates (R=alkyl=methyl, ethyl, isopropyl, propyl, etc., e.g. RP(OH)(O)—O-5′-, (OH)2(O)P-5′-CH2-), 5′-alkyletherphosphonates (R=alkylether=methoxymethyl (MeOCH2-), ethoxymethyl, etc., e.g. RP(OH)(O)—O-5′-).
• The sense strand can be modified in order to inactivate the sense strand and prevent formation of an active RISC, thereby potentially reducing off-target effects. This can be accomplished by a modification which prevents 5′-phosphorylation of the sense strand, e.g., by modification with a 5′-O-methyl ribonucleotide (see Nykänen et al., (2001) ATP requirements and small interfering RNA structure in the RNA interference pathway. Cell 107, 309-321.) Other modifications which prevent phosphorylation can also be used, e.g., simply substituting the 5′-OH by H rather than O-Me. Alternatively, a large bulky group may be added to the 5′-phosphate turning it into a phosphodiester linkage.
• Non-Natural Nucleobases
• Nitropyrrolyl and nitroindolyl are non-natural nucleobases that are members of a class of compounds known as universal bases. Universal bases are those compounds that can replace any of the four naturally occurring bases without substantially affecting the melting behavior or activity of the oligonucleotide duplex. In contrast to the stabilizing, hydrogen-bonding interactions associated with naturally occurring nucleobases, it is postulated that oligonucleotide duplexes containing 3-nitropyrrolyl nucleobases are stabilized solely by stacking interactions. The absence of significant hydrogen-bonding interactions with nitropyrrolyl nucleobases obviates the specificity for a specific complementary base. In addition, various reports confirm that 4-, 5- and 6-nitroindolyl display very little specificity for the four natural bases. Interestingly, an oligonucleotide duplex containing 5-nitroindolyl was more stable than the corresponding oligonucleotides containing 4-nitroindolyl and 6-nitroindolyl. Procedures for the preparation of 1-(2′-O-methyl-β-D-ribofuranosyl)-5-nitroindole are described in Gaubert, G.; Wengel, J. Tetrahedron Letters 2004, 45, 5629. Other universal bases amenable to the present invention include hypoxanthinyl, isoinosinyl, 2-aza-inosinyl, 7-deaza-inosinyl, nitroimidazolyl, nitropyrazolyl, nitrobenzimidazolyl, nitroindazolyl, aminoindolyl, pyrrolopyrimidinyl, and structural derivatives thereof. For a more detailed discussion, including synthetic procedures, of nitropyrrolyl, nitroindolyl, and other universal bases mentioned above see Vallone et al., Nucleic Acids Research, 27(17):3589-3596 (1999); Loakes et al., J. Mol. Bio., 270:426-436 (1997); Loakes et al., Nucleic Acids Research, 22(20):4039-4043 (1994); Oliver et al., Organic Letters, Vol. 3(13):1977-1980 (2001); Amosova et al., Nucleic Acids Research, 25(10):1930-1934 (1997); Loakes et al., Nucleic Acids Research, 29(12):2437-2447 (2001); Bergstrom et al., J. Am. Chem. Soc., 117:1201-1209 (1995); Franchetti et al., Biorg. Med. Chem. Lett. 11:67-69 (2001); and Nair et al., Nucelosides, Nucleotides & Nucleic Acids, 20(4-7):735-738 (2001).
• Difluorotolyl is a non-natural nucleobase that functions as a universal base. Difluorotolyl is an isostere of the natural nucleobase thymine. But unlike thymine, difluorotolyl shows no appreciable selectivity for any of the natural bases. Other aromatic compounds that function as universal bases and are amenable to the present invention are 4-fluoro-6-methylbenzimidazole and 4-methylbenzimidazole. In addition, the relatively hydrophobic isocarbostyrilyl derivatives 3-methyl isocarbostyrilyl, 5-methyl isocarbostyrilyl, and 3-methyl-7-propynyl isocarbostyrilyl are universal bases which cause only slight destabilization of oligonucleotide duplexes compared to the oligonucleotide sequence containing only natural bases. Other non-natural nucleobases contemplated in the present invention include 7-azaindolyl, 6-methyl-7-azaindolyl, imidizopyridinyl, 9-methyl-imidizopyridinyl, pyrrolopyrizinyl, isocarbostyrilyl, 7-propynyl isocarbostyrilyl, propynyl-7-azaindolyl, 2,4,5-trimethylphenyl, 4-methylindolyl, 4,6-dimethylindolyl, phenyl, napthalenyl, anthracenyl, phenanthracenyl, pyrenyl, stilbenyl, tetracenyl, pentacenyl, and structural derivates thereof. For a more detailed discussion, including synthetic procedures, of difluorotolyl, 4-fluoro-6-methylbenzimidazole, 4-methylbenzimidazole, and other non-natural bases mentioned above, see: Schweitzer et al., J. Org. Chem., 59:7238-7242 (1994); Berger et al., Nucleic Acids Research, 28(15):2911-2914 (2000); Moran et al., J. Am. Chem. Soc., 119:2056-2057 (1997); Morales et al., J. Am. Chem. Soc., 121:2323-2324 (1999); Guckian et al., J. Am. Chem. Soc., 118:8182-8183 (1996); Morales et al., J. Am. Chem. Soc., 122(6):1001-1007 (2000); McMinn et al., J. Am. Chem. Soc., 121:11585-11586 (1999); Guckian et al., J. Org. Chem., 63:9652-9656 (1998); Moran et al., Proc. Natl. Acad. Sci., 94:10506-10511 (1997); Das et al., J. Chem. Soc., Perkin Trans., 1:197-206 (2002); Shibata et al., J. Chem. Soc., Perkin Trans., 1: 1605-1611 (2001); Wu et al., J. Am. Chem. Soc., 122(32):7621-7632 (2000); O'Neill et al., J. Org. Chem., 67:5869-5875 (2002); Chaudhuri et al., J. Am. Chem. Soc., 117:10434-10442 (1995); and U.S. Pat. No. 6,218,108.
• Further details to the synthesis and use of universal bases is given in co-owned and co-pending PCT/US2005/025967, filed Jul. 21, 2005, hereby incorporated herein by reference in its entirety.
• Universal bases can be particularly helpful in situations where one attempts to target a gene in an organism that shows a variability between different strains of that organism. This is often true even for regions of a viral genome that are regarded as highly conserved. The incorporation of a universal base may allow the design of iRNA agents that target a large number of different strains of a virus even though they differ in one, or a few, e.g. in up to three, nucleotide positions.
• Universal bases are best included in a region of an iRNA agent that is least sensitive to nucleotide mismatches with regard to specifity and activity of the iRNA agent. It has been shown that position 2-9 of the antisense strand of an iRNA agent are most sensitive to mismatches between the antisense strand an the target mRNA, and this region has been termed the “seed-region” of an iRNA agent. Hence, when incorporating one or several universal base or bases into an iRNA agent, it or they are preferably incorporated outside this seed region.
• Table 1F and Table 1G show iRNA agents comprising universal bases in mutually complementary positions in the sense and antisense strand. However, while this is one preferred embodiment of the iRNA agents of the present invention, the effect of the universal base in an iRNA agent is more pronounced when the universal base is present in the antisense strand. It is therefore envisioned that the base in the sense strand in a position where it will pair up with a universal base in the antisense strand may be either a universal base, or any other suitable base, such as a, u, c or g. Preferably, one will test which base in such position of the sense strand will give the highest activity and/or selectivity for the iRNA agent. Alternatively, the base may be chosen that is present in this particular position in a majority of the target gene variants intended to be inhibited in their expression by the iRNA agent in question.
• Transport of iRNA Agents into Cells
• Not wishing to be bound by any theory, the chemical similarity between cholesterol-conjugated iRNA agents and certain constituents of lipoproteins (e.g. cholesterol, cholesteryl esters, phospholipids) may lead to the association of iRNA agents with lipoproteins (e.g. LDL, HDL) in blood and/or the interaction of the iRNA agent with cellular components having an affinity for cholesterol, e.g. components of the cholesterol transport pathway. Lipoproteins as well as their constituents are taken up and processed by cells by various active and passive transport mechanisms, for example, without limitation, endocytosis of LDL-receptor bound LDL, endocytosis of oxidized or otherwise modified LDLs through interaction with Scavenger receptor A, Scavenger receptor B1-mediated uptake of HDL cholesterol in the liver, pinocytosis, or transport of cholesterol across membranes by ABC (ATP-binding cassette) transporter proteins, e.g. ABC-A1, ABC-G1 or ABC-G4. Hence, cholesterol-conjugated iRNA agents could enjoy facilitated uptake by cells possessing such transport mechanisms, e.g. cells of the liver. As such, the present invention provides evidence and general methods for targeting iRNA agents to cells expressing certain cell surface components, e.g. receptors, by conjugating a natural ligand for such component (e.g. cholesterol) to the iRNA agent, or by conjugating a chemical moiety (e.g. cholesterol) to the iRNA agent which associates with or binds to a natural ligand for the component (e.g. LDL, HDL).
Other Embodiments
• An RNA, e.g., an iRNA agent, can be produced in a cell in vivo, e.g., from exogenous DNA templates that are delivered into the cell. For example, the DNA templates can be inserted into vectors and used as gene therapy vectors. Gene therapy vectors can be delivered to a subject by, for example, intravenous injection, local administration (U.S. Pat. No. 5,328,470), or by stereotactic injection (see, e.g., Chen et al. Proc. Natl. Acad. Sci. USA 91:3054-3057, 1994). The pharmaceutical preparation of the gene therapy vector can include the gene therapy vector in an acceptable diluent, or can comprise a slow release matrix in which the gene delivery vehicle is imbedded. The DNA templates, for example, can include two transcription units, one that produces a transcript that includes the top strand of an iRNA agent and one that produces a transcript that includes the bottom strand of an iRNA agent. When the templates are transcribed, the iRNA agent is produced, and processed into siRNA agent fragments that mediate gene silencing.
• Formulation
• The present invention also includes pharmaceutical compositions and formulations which include the dsRNA compounds of the invention. The pharmaceutical compositions of the present invention may be administered in a number of ways depending upon whether local or systemic treatment is desired and upon the area to be treated. Administration may be topical, pulmonary, e.g., by inhalation or insufflation of powders or aerosols, including by nebulizer; intratracheal, intranasal, epidermal and transdermal, oral or parenteral. Parenteral administration includes intravenous, intraarterial, subcutaneous, intraperitoneal or intramuscular injection or infusion; or intracranial, e.g., intrathecal or intraventricular, administration.
• Pharmaceutical compositions and formulations for topical administration may include transdermal patches, ointments, lotions, creams, gels, drops, suppositories, sprays, liquids and powders. Conventional pharmaceutical carriers, aqueous, powder or oily bases, thickeners and the like may be necessary or desirable. Coated condoms, gloves and the like may also be useful. Preferred topical formulations include those in which the dsRNAs of the invention are in admixture with a topical delivery agent such as lipids, liposomes, fatty acids, fatty acid esters, steroids, chelating agents and surfactants. Preferred lipids and liposomes include neutral (e.g. dioleoylphosphatidyl ethanolamine=DOPE, dimyristoylphosphatidyl choline=DMPC, distearolyphosphatidyl choline) negative (e.g. dimyristoylphosphatidyl glycerol=DMPG) and cationic (e.g. dioleoyltetramethylaminopropyl=DOTAP and dioleoylphosphatidyl ethanolamine=DOTMA). DsRNAs of the invention may be encapsulated within liposomes or may form complexes thereto, in particular to cationic liposomes. Alternatively, dsRNAs may be complexed to lipids, in particular to cationic lipids. Preferred fatty acids and esters include but are not limited arachidonic acid, oleic acid, eicosanoic acid, lauric acid, caprylic acid, capric acid, myristic acid, palmitic acid, stearic acid, linoleic acid, linolenic acid, dicaprate, tricaprate, monoolein, dilaurin, glyceryl 1-monocaprate, 1-dodecylazacycloheptan-2-one, an acylcarnitine, an acylcholine, or a C_1-10 alkyl ester (e.g. isopropylmyristate IPM), monoglyceride, diglyceride or pharmaceutically acceptable salt thereof. Topical formulations are described in detail in U.S. patent application Ser. No. 09/315,298 filed on May 20, 1999 which is incorporated herein by reference in its entirety.
• Compositions and formulations for oral administration include powders or granules, microparticulates, nanoparticulates, suspensions or solutions in water or non-aqueous media, capsules, gel capsules, sachets, tablets or minitablets. Thickeners, flavoring agents, diluents, emulsifiers, dispersing aids or binders may be desirable. Preferred oral formulations are those in which dsRNAs of the invention are administered in conjunction with one or more penetration enhancers, surfactants, and chelators. Preferred surfactants include fatty acids and/or esters or salts thereof, bile acids and/or salts thereof. Preferred bile acids/salts include chenodeoxycholic acid (CDCA) and ursodeoxychenodeoxycholic acid (UDCA), cholic acid, dehydrocholic acid, deoxycholic acid, glucholic acid, glycholic acid, glycodeoxycholic acid, taurocholic acid, taurodeoxycholic acid, sodium tauro-24,25-dihydro-fusidate and sodium glycodihydrofusidate. Preferred fatty acids include arachidonic acid, undecanoic acid, oleic acid, lauric acid, caprylic acid, capric acid, myristic acid, palmitic acid, stearic acid, linoleic acid, linolenic acid, dicaprate, tricaprate, monoolein, dilaurin, glyceryl 1-monocaprate, 1-dodecylazacycloheptan-2-one, an acylcarnitine, an acylcholine, or a monoglyceride, a diglyceride or a pharmaceutically acceptable salt thereof (e.g. sodium). Also preferred are combinations of penetration enhancers, for example, fatty acids/salts in combination with bile acids/salts. A particularly preferred combination is the sodium salt of lauric acid, capric acid and UDCA. Further penetration enhancers include polyoxyethylene-9-lauryl ether, polyoxyethylene-20-cetyl ether. DsRNAs of the invention may be delivered orally, in granular form including sprayed dried particles, or complexed to form micro or nanoparticles. DsRNA complexing agents include poly-amino acids; polyimines; polyacrylates; polyalkylacrylates, polyoxethanes, polyalkylcyanoacrylates; cationized gelatins, albumins, starches, acrylates, polyethyleneglycols (PEG) and starches; polyalkylcyanoacrylates; DEAE-derivatized polyimines, pollulans, celluloses and starches. Particularly preferred complexing agents include chitosan, N-trimethylchitosan, poly-L-lysine, polyhistidine, polyornithine, polyspermines, protamine, polyvinylpyridine, polythiodiethylaminomethylethylene P(TDAE), polyaminostyrene (e.g. p-amino), poly(methylcyanoacrylate), poly(ethylcyanoacrylate), poly(butylcyanoacrylate), poly(isobutylcyanoacrylate), poly(isohexylcynaoacrylate), DEAE-methacrylate, DEAE-hexylacrylate, DEAE-acrylamide, DEAE-albumin and DEAE-dextran, polymethylacrylate, polyhexylacrylate, poly(D,L-lactic acid), poly(DL-lactic-co-glycolic acid (PLGA), alginate, and polyethyleneglycol (PEG). Oral formulations for dsRNAs and their preparation are described in detail in U.S. application. Ser. No. 08/886,829 (filed Jul. 1, 1997), Ser. No. 09/108,673 (filed Jul. 1, 1998), Ser. No. 09/256,515 (filed Feb. 23, 1999), Ser. No. 09/082,624 (filed May 21, 1998) and Ser. No. 09/315,298 (filed May 20, 1999), each of which is incorporated herein by reference in their entirety.
• Compositions and formulations for parenteral, intrathecal or intraventricular administration may include sterile aqueous solutions which may also contain buffers, diluents and other suitable additives such as, but not limited to, penetration enhancers, carrier compounds and other pharmaceutically acceptable carriers or excipients.
• Pharmaceutical compositions of the present invention include, but are not limited to, solutions, emulsions, and liposome-containing formulations. These compositions may be generated from a variety of components that include, but are not limited to, preformed liquids, self-emulsifying solids and self-emulsifying semisolids.
• The pharmaceutical formulations of the present invention, which may conveniently be presented in unit dosage form, may be prepared according to conventional techniques well known in the pharmaceutical industry. Such techniques include the step of bringing into association the active ingredients with the pharmaceutical carrier(s) or excipient(s). In general, the formulations are prepared by uniformly and intimately bringing into association the active ingredients with liquid carriers or finely divided solid carriers or both, and then, if necessary, shaping the product.
• The compositions of the present invention may be formulated into any of many possible dosage forms such as, but not limited to, tablets, capsules, gel capsules, liquid syrups, soft gels, suppositories, and enemas. The compositions of the present invention may also be formulated as suspensions in aqueous, non-aqueous or mixed media. Aqueous suspensions may further contain substances which increase the viscosity of the suspension including, for example, sodium carboxymethylcellulose, sorbitol and/or dextran. The suspension may also contain stabilizers.
• In one embodiment of the present invention the pharmaceutical compositions may be formulated and used as foams. Pharmaceutical foams include formulations such as, but not limited to, emulsions, microemulsions, creams, jellies and liposomes. While basically similar in nature these formulations vary in the components and the consistency of the final product. The preparation of such compositions and formulations is generally known to those skilled in the pharmaceutical and formulation arts and may be applied to the formulation of the compositions of the present invention.
• Emulsions
• The compositions of the present invention may be prepared and formulated as emulsions. Emulsions are typically heterogenous systems of one liquid dispersed in another in the form of droplets usually exceeding 0.1 μm in diameter (Idson, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 199; Rosoff, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., Volume 1, p. 245; Block in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 2, p. 335; Higuchi et al., in Remington's Pharmaceutical Sciences, Mack Publishing Co., Easton, Pa., 1985, p. 301). Emulsions are often biphasic systems comprising two immiscible liquid phases intimately mixed and dispersed with each other. In general, emulsions may be of either the water-in-oil (w/o) or the oil-in-water (o/w) variety. When an aqueous phase is finely divided into and dispersed as minute droplets into a bulk oily phase, the resulting composition is called a water-in-oil (w/o) emulsion. Alternatively, when an oily phase is finely divided into and dispersed as minute droplets into a bulk aqueous phase, the resulting composition is called an oil-in-water (o/w) emulsion. Emulsions may contain additional components in addition to the dispersed phases, and the active drug which may be present as a solution in either the aqueous phase, oily phase or itself as a separate phase. Pharmaceutical excipients such as emulsifiers, stabilizers, dyes, and anti-oxidants may also be present in emulsions as needed. Pharmaceutical emulsions may also be multiple emulsions that are comprised of more than two phases such as, for example, in the case of oil-in-water-in-oil (o/w/o) and water-in-oil-in-water (w/o/w) emulsions. Such complex formulations often provide certain advantages that simple binary emulsions do not. Multiple emulsions in which individual oil droplets of an o/w emulsion enclose small water droplets constitute a w/o/w emulsion. Likewise a system of oil droplets enclosed in globules of water stabilized in an oily continuous phase provides an o/w/o emulsion.
• Emulsions are characterized by little or no thermodynamic stability. Often, the dispersed or discontinuous phase of the emulsion is well dispersed into the external or continuous phase and maintained in this form through the means of emulsifiers or the viscosity of the formulation. Either of the phases of the emulsion may be a semisolid or a solid, as is the case of emulsion-style ointment bases and creams. Other means of stabilizing emulsions entail the use of emulsifiers that may be incorporated into either phase of the emulsion. Emulsifiers may broadly be classified into four categories: synthetic surfactants, naturally occurring emulsifiers, absorption bases, and finely dispersed solids (Idson, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 199).
• Synthetic surfactants, also known as surface active agents, have found wide applicability in the formulation of emulsions and have been reviewed in the literature (Rieger, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 285; Idson, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), Marcel Dekker, Inc., New York, N.Y., 1988, volume 1, p. 199). Surfactants are typically amphiphilic and comprise a hydrophilic and a hydrophobic portion. The ratio of the hydrophilic to the hydrophobic nature of the surfactant has been termed the hydrophile/lipophile balance (HLB) and is a valuable tool in categorizing and selecting surfactants in the preparation of formulations. Surfactants may be classified into different classes based on the nature of the hydrophilic group: nonionic, anionic, cationic and amphoteric (Rieger, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 285).
• Naturally occurring emulsifiers used in emulsion formulations include lanolin, beeswax, phosphatides, lecithin and acacia. Absorption bases possess hydrophilic properties such that they can soak up water to form w/o emulsions yet retain their semisolid consistencies, such as anhydrous lanolin and hydrophilic petrolatum. Finely divided solids have also been used as good emulsifiers especially in combination with surfactants and in viscous preparations. These include polar inorganic solids, such as heavy metal hydroxides, nonswelling clays such as bentonite, attapulgite, hectorite, kaolin, montmorillonite, colloidal aluminum silicate and colloidal magnesium aluminum silicate, pigments and nonpolar solids such as carbon or glyceryl tristearate.
• A large variety of non-emulsifying materials are also included in emulsion formulations and contribute to the properties of emulsions. These include fats, oils, waxes, fatty acids, fatty alcohols, fatty esters, humectants, hydrophilic colloids, preservatives and antioxidants (Block, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 335; Idson, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 199).
• Hydrophilic colloids or hydrocolloids include naturally occurring gums and synthetic polymers such as polysaccharides (for example, acacia, agar, alginic acid, carrageenan, guar gum, karaya gum, and tragacanth), cellulose derivatives (for example, carboxymethylcellulose and carboxypropylcellulose), and synthetic polymers (for example, carbomers, cellulose ethers, and carboxyvinyl polymers). These disperse or swell in water to form colloidal solutions that stabilize emulsions by forming strong interfacial films around the dispersed-phase droplets and by increasing the viscosity of the external phase.
• Since emulsions often contain a number of ingredients such as carbohydrates, proteins, sterols and phosphatides that may readily support the growth of microbes, these formulations often incorporate preservatives. Commonly used preservatives included in emulsion formulations include methyl paraben, propyl paraben, quaternary ammonium salts, benzalkonium chloride, esters of p-hydroxybenzoic acid, and boric acid. Antioxidants are also commonly added to emulsion formulations to prevent deterioration of the formulation. Antioxidants used may be free radical scavengers such as tocopherols, alkyl gallates, butylated hydroxyanisole, butylated hydroxytoluene, or reducing agents such as ascorbic acid and sodium metabisulfite, and antioxidant synergists such as citric acid, tartaric acid, and lecithin.
• The application of emulsion formulations via dermatological, oral and parenteral routes and methods for their manufacture have been reviewed in the literature (Idson, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 199). Emulsion formulations for oral delivery have been very widely used because of ease of formulation, as well as efficacy from an absorption and bioavailability standpoint (Rosoff, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 245; Idson, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 199). Mineral-oil base laxatives, oil-soluble vitamins and high fat nutritive preparations are among the materials that have commonly been administered orally as o/w emulsions.
• In one embodiment of the present invention, the compositions of dsRNAs and nucleic acids are formulated as microemulsions. A microemulsion may be defined as a system of water, oil and amphiphile which is a single optically isotropic and thermodynamically stable liquid solution (Rosoff, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 245). Typically microemulsions are systems that are prepared by first dispersing an oil in an aqueous surfactant solution and then adding a sufficient amount of a fourth component, generally an intermediate chain-length alcohol to form a transparent system. Therefore, microemulsions have also been described as thermodynamically stable, isotropically clear dispersions of two immiscible liquids that are stabilized by interfacial films of surface-active molecules (Leung and Shah, in: Controlled Release of Drugs: Polymers and Aggregate Systems, Rosoff, M., Ed., 1989, VCH Publishers, New York, pages 185-215). Microemulsions commonly are prepared via a combination of three to five components that include oil, water, surfactant, cosurfactant and electrolyte. Whether the microemulsion is of the water-in-oil (w/o) or an oil-in-water (o/w) type is dependent on the properties of the oil and surfactant used and on the structure and geometric packing of the polar heads and hydrocarbon tails of the surfactant molecules (Schott, in Remington's Pharmaceutical Sciences, Mack Publishing Co., Easton, Pa., 1985, p. 271).
• The phenomenological approach utilizing phase diagrams has been extensively studied and has yielded a comprehensive knowledge, to one skilled in the art, of how to formulate microemulsions (Rosoff, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 245; Block, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 335). Compared to conventional emulsions, microemulsions offer the advantage of solubilizing water-insoluble drugs in a formulation of thermodynamically stable droplets that are formed spontaneously.
• Surfactants used in the preparation of microemulsions include, but are not limited to, ionic surfactants, non-ionic surfactants, Brij 96, polyoxyethylene oleyl ethers, polyglycerol fatty acid esters, tetraglycerol monolaurate (ML310), tetraglycerol monooleate (MO310), hexaglycerol monooleate (PO310), hexaglycerol pentaoleate (PO500), decaglycerol monocaprate (MCA750), decaglycerol monooleate (MO750), decaglycerol sequioleate (SO750), decaglycerol decaoleate (DA0750), alone or in combination with cosurfactants. The cosurfactant, usually a short-chain alcohol such as ethanol, 1-propanol, and 1-butanol, serves to increase the interfacial fluidity by penetrating into the surfactant film and consequently creating a disordered film because of the void space generated among surfactant molecules. Microemulsions may, however, be prepared without the use of cosurfactants and alcohol-free self-emulsifying microemulsion systems are known in the art. The aqueous phase may typically be, but is not limited to, water, an aqueous solution of the drug, glycerol, PEG300, PEG400, polyglycerols, propylene glycols, and derivatives of ethylene glycol. The oil phase may include, but is not limited to, materials such as Captex 300, Captex 355, Capmul MCM, fatty acid esters, medium chain (C₈-C₁₂) mono, di, and tri-glycerides, polyoxyethylated glyceryl fatty acid esters, fatty alcohols, polyglycolized glycerides, saturated polyglycolized C₈-C₁₀ glycerides, vegetable oils and silicone oil.
• Microemulsions are particularly of interest from the standpoint of drug solubilization and the enhanced absorption of drugs. Lipid based microemulsions (both o/w and w/o) have been proposed to enhance the oral bioavailability of drugs, including peptides (Constantinides et al., Pharmaceutical Research, 1994, 11, 1385-1390; Ritschel, Meth. Find. Exp. Clin. Pharmacol., 1993, 13, 205). Microemulsions afford advantages of improved drug solubilization, protection of drug from enzymatic hydrolysis, possible enhancement of drug absorption due to surfactant-induced alterations in membrane fluidity and permeability, ease of preparation, ease of oral administration over solid dosage forms, improved clinical potency, and decreased toxicity (Constantinides et al., Pharmaceutical Research, 1994, 11, 1385; Ho et al., J. Pharm. Sci., 1996, 85, 138-143). Often microemulsions may form spontaneously when their components are brought together at ambient temperature. This may be particularly advantageous when formulating thermolabile drugs, peptides or dsRNAs. Microemulsions have also been effective in the transdermal delivery of active components in both cosmetic and pharmaceutical applications. It is expected that the microemulsion compositions and formulations of the present invention will facilitate the increased systemic absorption of dsRNAs and nucleic acids from the gastrointestinal tract, as well as improve the local cellular uptake of dsRNAs and nucleic acids within the gastrointestinal tract, vagina, buccal cavity and other areas of administration.
• Microemulsions of the present invention may also contain additional components and additives such as sorbitan monostearate (Grill 3), Labrasol, and penetration enhancers to improve the properties of the formulation and to enhance the absorption of the dsRNAs and nucleic acids of the present invention. Penetration enhancers used in the microemulsions of the present invention may be classified as belonging to one of five broad categories surfactants, fatty acids, bile salts, chelating agents, and non-chelating non-surfactants (Lee et al., Critical Reviews in Therapeutic Drug Carrier Systems, 1991, p. 92). Each of these classes has been discussed above.
• Liposomes
• There are many organized surfactant structures besides microemulsions that have been studied and used for the formulation of drugs. These include monolayers, micelles, bilayers and vesicles. Vesicles, such as liposomes, have attracted great interest because of their specificity and the duration of action they offer from the standpoint of drug delivery. As used in the present invention, the term “liposome” means a vesicle composed of amphiphilic lipids arranged in a spherical bilayer or bilayers.
• Liposomes are unilamellar or multilamellar vesicles which have a membrane formed from a lipophilic material and an aqueous interior. The aqueous portion contains the composition to be delivered. Cationic liposomes possess the advantage of being able to fuse to the cell wall. Non-cationic liposomes, although not able to fuse as efficiently with the cell wall, are taken up by macrophages in vivo.
• In order to cross intact mammalian skin, lipid vesicles must pass through a series of fine pores, each with a diameter less than 50 nm, under the influence of a suitable transdermal gradient. Therefore, it is desirable to use a liposome which is highly deformable and able to pass through such fine pores.
• Further advantages of liposomes include; liposomes obtained from natural phospholipids are biocompatible and biodegradable; liposomes can incorporate a wide range of water and lipid soluble drugs; liposomes can protect encapsulated drugs in their internal compartments from metabolism and degradation (Rosoff, in Pharmaceutical Dosage Forms, Lieberman, Rieger and Banker (Eds.), 1988, Marcel Dekker, Inc., New York, N.Y., volume 1, p. 245). Important considerations in the preparation of liposome formulations are the lipid surface charge, vesicle size and the aqueous volume of the liposomes.
• Liposomes are useful for the transfer and delivery of active ingredients to the site of action. Because the liposomal membrane is structurally similar to biological membranes, when liposomes are applied to a tissue, the liposomes start to merge with the cellular membranes and as the merging of the liposome and cell progresses, the liposomal contents are emptied into the cell where the active agent may act.
• Liposomal formulations have been the focus of extensive investigation as the mode of delivery for many drugs. There is growing evidence that for topical administration, liposomes present several advantages over other formulations. Such advantages include reduced side-effects related to high systemic absorption of the administered drug, increased accumulation of the administered drug at the desired target, and the ability to administer a wide variety of drugs, both hydrophilic and hydrophobic, into the skin.
• Several reports have detailed the ability of liposomes to deliver agents including high-molecular weight DNA into the skin. Compounds including analgesics, antibodies, hormones and high-molecular weight DNAs have been administered to the skin. The majority of applications resulted in the targeting of the upper epidermis
• Liposomes fall into two broad classes. Cationic liposomes are positively charged liposomes which interact with the negatively charged DNA molecules to form a stable complex. The positively charged DNA/liposome complex binds to the negatively charged cell surface and is internalized in an endosome. Due to the acidic pH within the endosome, the liposomes are ruptured, releasing their contents into the cell cytoplasm (Wang et al., Biochem. Biophys. Res. Commun., 1987, 147, 980-985).
• Liposomes which are pH-sensitive or negatively-charged, entrap DNA rather than complex with it. Since both the DNA and the lipid are similarly charged, repulsion rather than complex formation occurs. Nevertheless, some DNA is entrapped within the aqueous interior of these liposomes. pH-sensitive liposomes have been used to deliver DNA encoding the thymidine kinase gene to cell monolayers in culture. Expression of the exogenous gene was detected in the target cells (Zhou et al., Journal of Controlled Release, 1992, 19, 269-274).
• One major type of liposomal composition includes phospholipids other than naturally-derived phosphatidylcholine. Neutral liposome compositions, for example, can be formed from dimyristoyl phosphatidylcholine (DMPC) or dipalmitoyl phosphatidylcholine (DPPC). Anionic liposome compositions generally are formed from dimyristoyl phosphatidylglycerol, while anionic fusogenic liposomes are formed primarily from dioleoyl phosphatidylethanolamine (DOPE). Another type of liposomal composition is formed from phosphatidylcholine (PC) such as, for example, soybean PC, and egg PC. Another type is formed from mixtures of phospholipid and/or phosphatidylcholine and/or cholesterol.
• Several studies have assessed the topical delivery of liposomal drug formulations to the skin. Application of liposomes containing interferon to guinea pig skin resulted in a reduction of skin herpes sores while delivery of interferon via other means (e.g. as a solution or as an emulsion) were ineffective (Weiner et al., Journal of Drug Targeting, 1992, 2, 405-410). Further, an additional study tested the efficacy of interferon administered as part of a liposomal formulation to the administration of interferon using an aqueous system, and concluded that the liposomal formulation was superior to aqueous administration (du Plessis et al., Antiviral Research, 1992, 18, 259-265).
• Non-ionic liposomal systems have also been examined to determine their utility in the delivery of drugs to the skin, in particular systems comprising non-ionic surfactant and cholesterol. Non-ionic liposomal formulations comprising Novasome™ I (glyceryl dilaurate/cholesterol/polyoxyethylene-10-stearyl ether) and Novasome™ II (glyceryl distearate/cholesterol/polyoxyethylene-10-stearyl ether) were used to deliver cyclosporin-A into the dermis of mouse skin. Results indicated that such non-ionic liposomal systems were effective in facilitating the deposition of cyclosporin-A into different layers of the skin (Hu et al. S.T.P.Pharma. Sci., 1994, 4, 6, 466).
• Liposomes also include “sterically stabilized” liposomes, a term which, as used herein, refers to liposomes comprising one or more specialized lipids that, when incorporated into liposomes, result in enhanced circulation lifetimes relative to liposomes lacking such specialized lipids. Examples of sterically stabilized liposomes are those in which part of the vesicle-forming lipid portion of the liposome (A) comprises one or more glycolipids, such as monosialoganglioside G _m1, or (B) is derivatized with one or more hydrophilic polymers, such as a polyethylene glycol (PEG) moiety. While not wishing to be bound by any particular theory, it is thought in the art that, at least for sterically stabilized liposomes containing gangliosides, sphingomyelin, or PEG-derivatized lipids, the enhanced circulation half-life of these sterically stabilized liposomes derives from a reduced uptake into cells of the reticuloendothelial system (RES) (Allen et al., FEBS Letters, 1987, 223, 42; Wu et al., Cancer Research, 1993, 53, 3765).
• Various liposomes comprising one or more glycolipids are known in the art. Papahadjopoulos et al. (Ann. N.Y. Acad. Sci., 1987, 507, 64) reported the ability of monosialoganglioside G _m1, galactocerebroside sulfate and phosphatidylinositol to improve blood half-lives of liposomes. These findings were expounded upon by Gabizon et al. (Proc. Natl. Acad. Sci. U.S.A., 1988, 85, 6949). U.S. Pat. No. 4,837,028 and WO 88/04924, both to Allen et al., disclose liposomes comprising (1) sphingomyelin and (2) the ganglioside G _m1 or a galactocerebroside sulfate ester. U.S. Pat. No. 5,543,152 (Webb et al.) discloses liposomes comprising sphingomyelin. Liposomes comprising 1,2-sn-dimyristoylphosphat-idylcholine are disclosed in WO 97/13499 (Lim et al).
• Many liposomes comprising lipids derivatized with one or more hydrophilic polymers, and methods of preparation thereof, are known in the art. Sunamoto et al. (Bull. Chem. Soc. Jpn., 1980, 53, 2778) described liposomes comprising a nonionic detergent, 2C_1215G, that contains a PEG moiety. Illum et al. (FEBS Lett., 1984, 167, 79) noted that hydrophilic coating of polystyrene particles with polymeric glycols results in significantly enhanced blood half-lives. Synthetic phospholipids modified by the attachment of carboxylic groups of polyalkylene glycols (e.g., PEG) are described by Sears (U.S. Pat. Nos. 4,426,330 and 4,534,899). Klibanov et al. (FEBS Lett., 1990, 268, 235) described experiments demonstrating that liposomes comprising phosphatidylethanolamine (PE) derivatized with PEG or PEG stearate have significant increases in blood circulation half-lives. Blume et al. (Biochimica et Biophysica Acta, 1990, 1029, 91) extended such observations to other PEG-derivatized phospholipids, e.g., DSPE-PEG, formed from the combination of distearoylphosphatidylethanolamine (DSPE) and PEG. Liposomes having covalently bound PEG moieties on their external surface are described in European Patent No. EP 0 445 131 B1 and WO 90/04384 to Fisher. Liposome compositions containing 1-20 mole percent of PE derivatized with PEG, and methods of use thereof, are described by Woodle et al. (U.S. Pat. Nos. 5,013,556 and 5,356,633) and Martin et al. (U.S. Pat. No. 5,213,804 and European Patent No. EP 0 496 813 B1). Liposomes comprising a number of other lipid-polymer conjugates are disclosed in WO 91/05545 and U.S. Pat. No. 5,225,212 (both to Martin et al.) and in WO 94/20073 (Zalipsky et al.) Liposomes comprising PEG-modified ceramide lipids are described in WO 96/10391 (Choi et al). U.S. Pat. No. 5,540,935 (Miyazaki et al.) and U.S. Pat. No. 5,556,948 (Tagawa et al.) describe PEG-containing liposomes that can be further derivatized with functional moieties on their surfaces.
• A limited number of liposomes comprising nucleic acids are known in the art. WO 96/40062 to Thierry et al. discloses methods for encapsulating high molecular weight nucleic acids in liposomes. U.S. Pat. No. 5,264,221 to Tagawa et al. discloses protein-bonded liposomes and asserts that the contents of such liposomes may include dsRNA. U.S. Pat. No. 5,665,710 to Rahman et al. describes certain methods of encapsulating oligodeoxynucleotides in liposomes. WO 97/04787 to Love et al. discloses liposomes comprising dsRNAs targeted to the raf gene.
• Transfersomes are yet another type of liposomes, and are highly deformable lipid aggregates which are attractive candidates for drug delivery vehicles. Transfersomes may be described as lipid droplets which are so highly deformable that they are easily able to penetrate through pores which are smaller than the droplet. Transfersomes are adaptable to the environment in which they are used, e.g. they are self-optimizing (adaptive to the shape of pores in the skin), self-repairing, frequently reach their targets without fragmenting, and often self-loading. To make transfersomes it is possible to add surface edge-activators, usually surfactants, to a standard liposomal composition. Transfersomes have been used to deliver serum albumin to the skin. The transfersome-mediated delivery of serum albumin has been shown to be as effective as subcutaneous injection of a solution containing serum albumin.
• Surfactants find wide application in formulations such as emulsions (including microemulsions) and liposomes. The most common way of classifying and ranking the properties of the many different types of surfactants, both natural and synthetic, is by the use of the hydrophile/lipophile balance (HLB). The nature of the hydrophilic group (also known as the “head”) provides the most useful means for categorizing the different surfactants used in formulations (Rieger, in Pharmaceutical Dosage Forms, Marcel Dekker, Inc., New York, N.Y., 1988, p. 285).
• If the surfactant molecule is not ionized, it is classified as a nonionic surfactant. Nonionic surfactants find wide application in pharmaceutical and cosmetic products and are usable over a wide range of pH values. In general their HLB values range from 2 to about 18 depending on their structure. Nonionic surfactants include nonionic esters such as ethylene glycol esters, propylene glycol esters, glyceryl esters, polyglyceryl esters, sorbitan esters, sucrose esters, and ethoxylated esters. Nonionic alkanolamides and ethers such as fatty alcohol ethoxylates, propoxylated alcohols, and ethoxylated/propoxylated block polymers are also included in this class. The polyoxyethylene surfactants are the most popular members of the nonionic surfactant class.
• If the surfactant molecule carries a negative charge when it is dissolved or dispersed in water, the surfactant is classified as anionic. Anionic surfactants include carboxylates such as soaps, acyl lactylates, acyl amides of amino acids, esters of sulfuric acid such as alkyl sulfates and ethoxylated alkyl sulfates, sulfonates such as alkyl benzene sulfonates, acyl isethionates, acyl taurates and sulfosuccinates, and phosphates. The most important members of the anionic surfactant class are the alkyl sulfates and the soaps.
• If the surfactant molecule carries a positive charge when it is dissolved or dispersed in water, the surfactant is classified as cationic. Cationic surfactants include quaternary ammonium salts and ethoxylated amines. The quaternary ammonium salts are the most used members of this class.
• If the surfactant molecule has the ability to carry either a positive or negative charge, the surfactant is classified as amphoteric. Amphoteric surfactants include acrylic acid derivatives, substituted alkylamides, N-alkylbetaines and phosphatides.
• The use of surfactants in drug products, formulations and in emulsions has been reviewed (Rieger, in Pharmaceutical Dosage Forms, Marcel Dekker, Inc., New York, N.Y., 1988, p. 285).
• Penetration Enhancers
• In one embodiment, the present invention employs various penetration enhancers to effect the efficient delivery of nucleic acids, particularly dsRNAs, to the skin of animals. Most drugs are present in solution in both ionized and nonionized forms. However, usually only lipid soluble or lipophilic drugs readily cross cell membranes. It has been discovered that even non-lipophilic drugs may cross cell membranes if the membrane to be crossed is treated with a penetration enhancer. In addition to aiding the diffusion of non-lipophilic drugs across cell membranes, penetration enhancers also enhance the permeability of lipophilic drugs.
• Penetration enhancers may be classified as belonging to one of five broad categories, i.e., surfactants, fatty acids, bile salts, chelating agents, and non-chelating non-surfactants (Lee et al., Critical Reviews in Therapeutic Drug Carrier Systems, 1991, p. 92). Each of the above mentioned classes of penetration enhancers are described below in greater detail.
• Surfactants: In connection with the present invention, surfactants (or “surface-active agents”) are chemical entities which, when dissolved in an aqueous solution, reduce the surface tension of the solution or the interfacial tension between the aqueous solution and another liquid, with the result that absorption of dsRNAs through the mucosa is enhanced. In addition to bile salts and fatty acids, these penetration enhancers include, for example, sodium lauryl sulfate, polyoxyethylene-9-lauryl ether and polyoxyethylene-20-cetyl ether) (Lee et al., Critical Reviews in Therapeutic Drug Carrier Systems, 1991, p. 92); and perfluorochemical emulsions, such as FC-43 (Takahashi et al., J. Pharm. Pharmacol., 1988, 40, 252).
• Fatty acids: Various fatty acids and their derivatives which act as penetration enhancers include, for example, oleic acid, lauric acid, capric acid (n-decanoic acid), myristic acid, palmitic acid, stearic acid, linoleic acid, linolenic acid, dicaprate, tricaprate, monoolein (1-monooleoyl-rac-glycerol), dilaurin, caprylic acid, arachidonic acid, glycerol 1-monocaprate, 1-dodecylazacycloheptan-2-one, acylcarnitines, acylcholines, C₁-C₁₀ alkyl esters thereof (e.g., methyl, isopropyl and t-butyl), and mono- and di-glycerides thereof (i.e., oleate, laurate, caprate, myristate, palmitate, stearate, linoleate, etc.) (Lee et al., Critical Reviews in Therapeutic Drug Carrier Systems, 1991, p. 92; Muranishi, Critical Reviews in Therapeutic Drug Carrier Systems, 1990, 7, 1-33; El Hariri et al., J. Pharm. Pharmacol., 1992, 44, 651-654).
• Bile salts: The physiological role of bile includes the facilitation of dispersion and absorption of lipids and fat-soluble vitamins (Brunton, Chapter 38 in: Goodman & Gilman's The Pharmacological Basis of Therapeutics, 9th Ed., Hardman et al. Eds., McGraw-Hill, New York, 1996, pp. 934-935). Various natural bile salts, and their synthetic derivatives, act as penetration enhancers. Thus the term “bile salts” includes any of the naturally occurring components of bile as well as any of their synthetic derivatives. The bile salts of the invention include, for example, cholic acid (or its pharmaceutically acceptable sodium salt, sodium cholate), dehydrocholic acid (sodium dehydrocholate), deoxycholic acid (sodium deoxycholate), glucholic acid (sodium glucholate), glycholic acid (sodium glycocholate), glycodeoxycholic acid (sodium glycodeoxycholate), taurocholic acid (sodium taurocholate), taurodeoxycholic acid (sodium taurodeoxycholate), chenodeoxycholic acid (sodium chenodeoxycholate), ursodeoxycholic acid (UDCA), sodium tauro-24,25-dihydro-fusidate (STDHF), sodium glycodihydrofusidate and polyoxyethylene-9-lauryl ether (POE) (Lee et al., Critical Reviews in Therapeutic Drug Carrier Systems, 1991, page 92; Swinyard, Chapter 39 In: Remington's Pharmaceutical Sciences, 18th Ed., Gennaro, ed., Mack Publishing Co., Easton, Pa., 1990, pages 782-783; Muranishi, Critical Reviews in Therapeutic Drug Carrier Systems, 1990, 7, 1-33; Yamamoto et al., J. Pharm. Exp. Ther., 1992, 263, 25; Yamashita et al., J. Pharm. Sci., 1990, 79, 579-583).
• Chelating Agents: Chelating agents, as used in connection with the present invention, can be defined as compounds that remove metallic ions from solution by forming complexes therewith, with the result that absorption of dsRNAs through the mucosa is enhanced. With regards to their use as penetration enhancers in the present invention, chelating agents have the added advantage of also serving as DNase inhibitors, as most characterized DNA nucleases require a divalent metal ion for catalysis and are thus inhibited by chelating agents (Jarrett, J. Chromatogr., 1993, 618, 315-339). Chelating agents of the invention include but are not limited to disodium ethylenediaminetetraacetate (EDTA), citric acid, salicylates (e.g., sodium salicylate, 5-methoxysalicylate and homovanilate), N-acyl derivatives of collagen, laureth-9 and N-amino acyl derivatives of beta-diketones (enamines)(Lee et al., Critical Reviews in Therapeutic Drug Carrier Systems, 1991, page 92; Muranishi, Critical Reviews in Therapeutic Drug Carrier Systems, 1990, 7, 1-33; Buur et al., J. Control Rel., 1990, 14, 43-51).
• Non-chelating non-surfactants: As used herein, non-chelating non-surfactant penetration enhancing compounds can be defined as compounds that demonstrate insignificant activity as chelating agents or as surfactants but that nonetheless enhance absorption of dsRNAs through the alimentary mucosa (Muranishi, Critical Reviews in Therapeutic Drug Carrier Systems, 1990, 7, 1-33). This class of penetration enhancers include, for example, unsaturated cyclic ureas, 1-alkyl- and 1-alkenylazacyclo-alkanone derivatives (Lee et al., Critical Reviews in Therapeutic Drug Carrier Systems, 1991, page 92); and non-steroidal anti-inflammatory agents such as diclofenac sodium, indomethacin and phenylbutazone (Yamashita et al., J. Pharm. Pharmacol., 1987, 39, 621-626).
• Agents that enhance uptake of dsRNAs at the cellular level may also be added to the pharmaceutical and other compositions of the present invention. For example, cationic lipids, such as lipofectin (Junichi et al, U.S. Pat. No. 5,705,188), cationic glycerol derivatives, and polycationic molecules, such as polylysine (Lollo et al., PCT Application WO 97/30731), are also known to enhance the cellular uptake of dsRNAs.
• Other agents may be utilized to enhance the penetration of the administered nucleic acids, including glycols such as ethylene glycol and propylene glycol, pyrrols such as 2-pyrrol, azones, and terpenes such as limonene and menthone.
• Carriers
• Certain compositions of the present invention also incorporate carrier compounds in the formulation. As used herein, “carrier compound” or “carrier” can refer to a nucleic acid, or analog thereof, which is inert (i.e., does not possess biological activity per se) but is recognized as a nucleic acid by in vivo processes that reduce the bioavailability of a nucleic acid having biological activity by, for example, degrading the biologically active nucleic acid or promoting its removal from circulation. The coadministration of a nucleic acid and a carrier compound, typically with an excess of the latter substance, can result in a substantial reduction of the amount of nucleic acid recovered in the liver, kidney or other extracirculatory reservoirs, presumably due to competition between the carrier compound and the nucleic acid for a common receptor. For example, the recovery of a partially phosphorothioate dsRNA in hepatic tissue can be reduced when it is coadministered with polyinosinic acid, dextran sulfate, polycytidic acid or 4-acetamido-4′isothiocyano-stilbene-2,2′-disulfonic acid (Miyao et al., Antisense Res. Dev., 1995, 5, 115-121; Takakura et al., Antisense & Nucl. Acid Drug Dev., 1996, 6, 177-183.
• Excipients
• In contrast to a carrier compound, a “pharmaceutical carrier” or “excipient” is a pharmaceutically acceptable solvent, suspending agent or any other pharmacologically inert vehicle for delivering one or more nucleic acids to an animal. The excipient may be liquid or solid and is selected, with the planned manner of administration in mind, so as to provide for the desired bulk, consistency, etc., when combined with a nucleic acid and the other components of a given pharmaceutical composition. Typical pharmaceutical carriers include, but are not limited to, binding agents (e.g., pregelatinized maize starch, polyvinylpyrrolidone or hydroxypropyl methylcellulose, etc.); fillers (e.g., lactose and other sugars, microcrystalline cellulose, pectin, gelatin, calcium sulfate, ethyl cellulose, polyacrylates or calcium hydrogen phosphate, etc.); lubricants (e.g., magnesium stearate, talc, silica, colloidal silicon dioxide, stearic acid, metallic stearates, hydrogenated vegetable oils, corn starch, polyethylene glycols, sodium benzoate, sodium acetate, etc.); disintegrants (e.g., starch, sodium starch glycolate, etc.); and wetting agents (e.g., sodium lauryl sulphate, etc).
• Pharmaceutically acceptable organic or inorganic excipient suitable for non-parenteral administration which do not deleteriously react with nucleic acids can also be used to formulate the compositions of the present invention. Suitable pharmaceutically acceptable carriers include, but are not limited to, water, salt solutions, alcohols, polyethylene glycols, gelatin, lactose, amylose, magnesium stearate, talc, silicic acid, viscous paraffin, hydroxymethylcellulose, polyvinylpyrrolidone and the like.
• Formulations for topical administration of nucleic acids may include sterile and non-sterile aqueous solutions, non-aqueous solutions in common solvents such as alcohols, or solutions of the nucleic acids in liquid or solid oil bases. The solutions may also contain buffers, diluents and other suitable additives. Pharmaceutically acceptable organic or inorganic excipients suitable for non-parenteral administration which do not deleteriously react with nucleic acids can be used.
• Suitable pharmaceutically acceptable excipients include, but are not limited to, water, salt solutions, alcohol, polyethylene glycols, gelatin, lactose, amylose, magnesium stearate, talc, silicic acid, viscous paraffin, hydroxymethylcellulose, polyvinylpyrrolidone and the like.
• Pharmaceutical Compositions for the Delivery to the Respiratory Tract
• Another aspect of the invention provides for the delivery of IRNA agents to the respiratory tract, particularly for the treatment of cystic fibrosis. The respiratory tract includes the upper airways, including the oropharynx and larynx, followed by the lower airways, which include the trachea followed by bifurcations into the bronchi and bronchioli. The upper and lower airways are called the conductive airways. The terminal bronchioli then divide into respiratory bronchioli which then lead to the ultimate respiratory zone, the alveoli, or deep lung. The deep lung, or alveoli, are the primary target of inhaled therapeutic aerosols for systemic delivery of iRNA agents.
• Pulmonary delivery compositions can be delivered by inhalation by the patient of a dispersion so that the composition, preferably the iRNA agent, within the dispersion can reach the lung where it can, for example, be readily absorbed through the alveolar region directly into blood circulation. Pulmonary delivery can be effective both for systemic delivery and for localized delivery to treat diseases of the lungs.
• Pulmonary delivery can be achieved by different approaches, including the use of nebulized, aerosolized, micellular and dry powder-based formulations; administration by inhalation may be oral and/or nasal. Delivery can be achieved with liquid nebulizers, aerosol-based inhalers, and dry powder dispersion devices. Metered-dose devices are preferred. One of the benefits of using an atomizer or inhaler is that the potential for contamination is minimized because the devices are self contained. Dry powder dispersion devices, for example, deliver drugs that may be readily formulated as dry powders. An iRNA composition may be stably stored as lyophilized or spray-dried powders by itself or in combination with suitable powder carriers. The delivery of a composition for inhalation can be mediated by a dosing timing element which can include a timer, a dose counter, time measuring device, or a time indicator which when incorporated into the device enables dose tracking, compliance monitoring, and/or dose triggering to a patient during administration of the aerosol medicament.
• Examples of pharmaceutical devices for aerosol delivery include metered dose inhalers (MDIs), dry powder inhalers (DPIs), and air-jet nebulizers. Exemplary delivery systems by inhalation which can be readily adapted for delivery of the subject iRNA agents are described in, for example, U.S. Pat. Nos. 5,756,353; 5,858,784; and PCT applications WO98/31346; WO98/10796; WO00/27359; WO01/54664; WO02/060412. Other aerosol formulations that may be used for delivering the iRNA agents are described in U.S. Pat. Nos. 6,294,153; 6,344,194; 6,071,497, and PCT applications WO02/066078; WO02/053190; WO01/60420; WO00/66206. Further, methods for delivering iRNA agents can be adapted from those used in delivering other oligonucleotides (e.g., an antisense oligonucleotide) by inhalation, such as described in Templin et al., Antisense Nucleic Acid Drug Dev, 2000, 10:359-68; Sandrasagra et al., Expert Opin Biol Ther, 2001, 1:979-83; Sandrasagra et al., Antisense Nucleic Acid Drug Dev, 2002, 12:177-81.
• The delivery of the inventive agents may also involve the administration of so called “pro-drugs”, i.e. formulations or chemical modifications of a therapeutic substance that require some form of processing or transport by systems innate to the subject organism to release the therapeutic substance, preferably at the site where its action is desired; this latter embodiment may be used in conjunction with delivery of the respiratory tract, but also together with other embodiments of the present invention. For example, the human lungs can remove or rapidly degrade hydrolytically cleavable deposited aerosols over periods ranging from minutes to hours. In the upper airways, ciliated epithelia contribute to the “mucociliary excalator” by which particles are swept from the airways toward the mouth. Pavia, D., “Lung Mucociliary Clearance,” in Aerosols and the Lung: Clinical and Experimental Aspects, Clarke, S. W. and Pavia, D., Eds., Butterworths, London, 1984. In the deep lungs, alveolar macrophages are capable of phagocytosing particles soon after their deposition. Warheit et al. Microscopy Res. Tech., 26: 412-422 (1993); and Brain, J. D., “Physiology and Pathophysiology of Pulmonary Macrophages,” in The Reticuloendothelial System, S. M. Reichard and J. Filkins, Eds., Plenum, New. York., pp. 315-327, 1985.
• In preferred embodiments, particularly where systemic dosing with the iRNA agent is desired, the aerosoled iRNA agents are formulated as microparticles. Microparticles having a diameter of between 0.5 and ten microns can penetrate the lungs, passing through most of the natural barriers. A diameter of less than ten microns is required to bypass the throat; a diameter of 0.5 microns or greater is required to avoid being exhaled.
• Other Components
• The compositions of the present invention may additionally contain other adjunct components conventionally found in pharmaceutical compositions, at their art-established usage levels. Thus, for example, the compositions may contain additional, compatible, pharmaceutically-active materials such as, for example, antipruritics, astringents, local anesthetics or anti-inflammatory agents, or may contain additional materials useful in physically formulating various dosage forms of the compositions of the present invention, such as dyes, flavoring agents, preservatives, antioxidants, opacifiers, thickening agents and stabilizers. However, such materials, when added, should not unduly interfere with the biological activities of the components of the compositions of the present invention. The formulations can be sterilized and, if desired, mixed with auxiliary agents, e.g., lubricants, preservatives, stabilizers, wetting agents, emulsifiers, salts for influencing osmotic pressure, buffers, colorings, flavorings and/or aromatic substances and the like which do not deleteriously interact with the nucleic acid(s) of the formulation.
• Aqueous suspensions may contain substances which increase the viscosity of the suspension including, for example, sodium carboxymethylcellulose, sorbitol and/or dextran. The suspension may also contain stabilizers.
• Certain embodiments of the invention provide pharmaceutical compositions containing (a) one or more dsRNA agents and (b) one or more other chemotherapeutic agents which function by a non-RNA interference mechanism. Examples of such chemotherapeutic agents include but are not limited to daunorubicin, daunomycin, dactinomycin, doxorubicin, epirubicin, idarubicin, esorubicin, bleomycin, mafosfamide, ifosfamide, cytosine arabinoside, bis-chloroethylnitrosurea, busulfan, mitomycin C, actinomycin D, mithramycin, prednisone, hydroxyprogesterone, testosterone, tamoxifen, dacarbazine, procarbazine, hexamethylmelamine, pentamethylmelamine, mitoxantrone, amsacrine, chlorambucil, methylcyclohexylnitrosurea, nitrogen mustards, melphalan, cyclophosphamide, 6-mercaptopurine, 6-thioguanine, cytarabine, 5-azacytidine, hydroxyurea, deoxycoformycin, 4-hydroxyperoxycyclophosphoramide, 5-fluorouracil (5-FU), 5-fluorodeoxyuridine (5-FUdR), methotrexate (MTX), colchicine, taxol, vincristine, vinblastine, etoposide (VP-16), trimetrexate, irinotecan, topotecan, gemcitabine, teniposide, cisplatin and diethylstilbestrol (DES). See, generally, The Merck Manual of Diagnosis and Therapy, 15th Ed. 1987, pp. 1206-1228, Berkow et al., eds., Rahway, N.J. When used with the compounds of the invention, such chemotherapeutic agents may be used individually (e.g., 5-FU and oligonucleotide), sequentially (e.g., 5-FU and oligonucleotide for a period of time followed by MTX and oligonucleotide), or in combination with one or more other such chemotherapeutic agents (e.g., 5-FU, MTX and oligonucleotide, or 5-FU, radiotherapy and oligonucleotide). Anti-inflammatory drugs, including but not limited to nonsteroidal anti-inflammatory drugs and corticosteroids, and antiviral drugs, including but not limited to ribivirin, vidarabine, acyclovir and ganciclovir, may also be combined in compositions of the invention. See, generally, The Merck Manual of Diagnosis and Therapy, 15th Ed., Berkow et al., eds., 1987, Rahway, N.J., pages 2499-2506 and 46-49, respectively). Other non-dsRNA chemotherapeutic agents are also within the scope of this invention. Two or more combined compounds may be used together or sequentially.
• Toxicity and therapeutic efficacy of such compounds can be determined by standard pharmaceutical procedures in cell cultures or experimental animals, e.g., for determining the LD50 (the dose lethal to 50% of the population) and the ED50 (the dose therapeutically effective in 50% of the population). The dose ratio between toxic and therapeutic effects is the therapeutic index and it can be expressed as the ratio LD50/ED50. Compounds which exhibit high therapeutic indices are preferred.
• The data obtained from cell culture assays and animal studies can be used in formulation a range of dosage for use in humans. The dosage of compositions of the invention lies generally within a range of circulating concentrations that include the ED50 with little or no toxicity. The dosage may vary within this range depending upon the dosage form employed and the route of administration utilized. For any compound used in the method of the invention, the therapeutically effective dose can be estimated initially from cell culture assays. A dose may be formulated in animal models to achieve a circulating plasma concentration range of the compound or, when appropriate, of the polypeptide product of a target sequence (e.g., achieving a decreased concentration of the polypeptide) that includes the IC50 (i.e., the concentration of the test compound which achieves a half-maximal inhibition of symptoms) as determined in cell culture. Such information can be used to more accurately determine useful doses in humans. Levels in plasma may be measured, for example, by high performance liquid chromatography.
• In addition to their administration individually or as a plurality, as discussed above, the dsRNAs of the invention can be administered in combination with other known agents effective in treatment of influenza infection. In any event, the administering physician can adjust the amount and timing of dsRNA administration on the basis of results observed using standard measures of efficacy known in the art or described herein.
• Treatment Methods and Routes of Delivery
• A composition that includes an iRNA agent, e.g., an iRNA agent that targets influenza virus, can be delivered to a subject by a variety of routes to achieve either local delivery to the site of action of systemic delivery to the subject. Exemplary routes include direct local administration to the site of treatment, such as the lungs and nasal passage as well as intravenous, nasal, oral, and ocular delivery. The preferred means of administering the iRNA agents of the present invention is through direct administration to the lungs and nasal passage as a liquid, aerosol or nubulized solution.
• In general, the delivery of the iRNA agents of the present invention is done to achieve delivery into the subject to the site of infection. The preferred means of achieving this is through either a local administration to the lungs or nasal passage, e.g. into the respiratory tissues via inhalation or intranasal administration, or via systemic administration, e.g. parental administration.
• Formulations for inhalation or parenteral administration are well known in the art. Such formulation may include sterile aqueous solutions which may also contain buffers, diluents and other suitable additives. For intravenous use, the total concentration of solutes should be controlled to render the preparation isotonic.
• The active compounds disclosed herein are preferably administered to the lung(s) or nasal passage of a subject by any suitable means. Active compounds may be administered by administering an aerosol suspension of respirable particles comprised of the active compound or active compounds, which the subject inhales. The active compound can be aerosolized in a variety of forms, such as, but not limited to, dry powder inhalants, metered dose inhalants, or liquid/liquid suspensions. The respirable particles may be liquid or solid. The particles may optionally contain other therapeutic ingredients such as amiloride, benzamil or phenamil, with the selected compound included in an amount effective to inhibit the reabsorption of water from airway mucous secretions, as described in U.S. Pat. No. 4,501,729.
• The particulate pharmaceutical composition may optionally be combined with a carrier to aid in dispersion or transport. A suitable carrier such as a sugar (i.e., lactose, sucrose, trehalose, mannitol) may be blended with the active compound or compounds in any suitable ratio (e.g., a 1 to 1 ratio by weight).
• Particles comprised of the active compound for practicing the present invention should include particles of respirable size, that is, particles of a size sufficiently small to pass through the mouth or nose and larynx upon inhalation and into the bronchi and alveoli of the lungs. In general, particles ranging from about 1 to 10 microns in size (more particularly, less than about 5 microns in size) are respirable. Particles of non-respirable size which are included in the aerosol tend to deposit in the throat and be swallowed, and the quantity of non-respirable particles in the aerosol is preferably minimized. For nasal administration, a particle size in the range of 10-500 uM is preferred to ensure retention in the nasal cavity.
• Liquid pharmaceutical compositions of active compound for producing an aerosol may be prepared by combining the active compound with a suitable vehicle, such as sterile pyrogen free water. The hypertonic saline solutions used to carry out the present invention are preferably sterile, pyrogen-free solutions, comprising from one to fifteen percent (by weight) of the physiologically acceptable salt, and more preferably from three to seven percent by weight of the physiologically acceptable salt.
• Aerosols of liquid particles comprising the active compound may be produced by any suitable means, such as with a pressure-driven jet nebulizer or an ultrasonic nebulizer. See, e.g., U.S. Pat. No. 4,501,729. Nebulizers are commercially available devices which transform solutions or suspensions of the active ingredient into a therapeutic aerosol mist either by means of acceleration of compressed gas, typically air or oxygen, through a narrow venturi orifice or by means of ultrasonic agitation.
• Suitable formulations for use in nebulizers consist of the active ingredient in a liquid carrier, the active ingredient comprising up to 40% w/w of the formulation, but preferably less than 20% w/w. The carrier is typically water (and most preferably sterile, pyrogen-free water) or a dilute aqueous alcoholic solution, preferably made isotonic, but may be hypertonic with body fluids by the addition of, for example, sodium chloride. Optional additives include preservatives if the formulation is not made sterile, for example, methyl hydroxybenzoate, antioxidants, flavoring agents, volatile oils, buffering agents and surfactants.
• Aerosols of solid particles comprising the active compound may likewise be produced with any solid particulate therapeutic aerosol generator. Aerosol generators for administering solid particulate therapeutics to a subject produce particles which are respirable and generate a volume of aerosol containing a predetermined metered dose of a therapeutic at a rate suitable for human administration. One illustrative type of solid particulate aerosol generator is an insufflator. Suitable formulations for administration by insufflation include finely comminuted powders which may be delivered by means of an insufflator or taken into the nasal cavity in the manner of a snuff. In the insufflator, the powder (e.g., a metered dose thereof effective to carry out the treatments described herein) is contained in capsules or cartridges, typically made of gelatin or plastic, which are either pierced or opened in situ and the powder delivered by air drawn through the device upon inhalation or by means of a manually-operated pump. The powder employed in the insufflator consists either solely of the active ingredient or of a powder blend comprising the active ingredient, a suitable powder diluent, such as lactose, and an optional surfactant. The active ingredient typically comprises from 0.1 to 100 w/w of the formulation.
• A second type of illustrative aerosol generator comprises a metered dose inhaler. Metered dose inhalers are pressurized aerosol dispensers, typically containing a suspension or solution formulation of the active ingredient in a liquefied propellant. During use these devices discharge the formulation through a valve adapted to deliver a metered volume, typically from 10 to 200 ul, to produce a fine particle spray containing the active ingredient. Suitable propellants include certain chlorofluorocarbon compounds, for example, dichlorodifluoromethane, trichlorofluoromethane, dichlorotetrafluoroethane and mixtures thereof. The formulation may additionally contain one or more co-solvents, for example, ethanol, surfactants, such as oleic acid or sorbitan trioleate, antioxidant and suitable flavoring agents.
• An iRNA agent can be incorporated into pharmaceutical compositions suitable for administration. For example, compositions can include one or more species of an iRNA agent and a pharmaceutically acceptable carrier. As used herein the language “pharmaceutically acceptable carrier” is intended to include any and all solvents, dispersion media, coatings, antibacterial and antifungal agents, isotonic and absorption delaying agents, and the like, compatible with pharmaceutical administration. The use of such media and agents for pharmaceutically active substances is well known in the art. Except insofar as any conventional media or agent is incompatible with the active compound, use thereof in the compositions is contemplated. Supplementary active compounds can also be incorporated into the compositions.
• Administration can be provided by the subject or by another person, e.g., a caregiver. A caregiver can be any entity involved with providing care to the human: for example, a hospital, hospice, doctor's office, outpatient clinic; a healthcare worker such as a doctor, nurse, or other practitioner; or a spouse or guardian, such as a parent. The medication can be provided in measured doses or in a dispenser which delivers a metered dose.
• The term “therapeutically effective amount” is the amount present in the composition that is needed to provide the desired level of drug in the subject to be treated to give the anticipated physiological response.
• The term “physiologically effective amount” is that amount delivered to a subject to give the desired palliative or curative effect.
• The term “pharmaceutically acceptable carrier” means that the carrier can be taken into the lungs with no significant adverse toxicological effects on the lungs.
• The term “co-administration” refers to administering to a subject two or more agents, and in particular two or more iRNA agents. The agents can be contained in a single pharmaceutical composition and be administered at the same time, or the agents can be contained in separate formulation and administered serially to a subject. So long as the two agents can be detected in the subject at the same time, the two agents are said to be co-administered.
• The types of pharmaceutical excipients that are useful as carrier include stabilizers such as human serum albumin (HSA), bulking agents such as carbohydrates, amino acids and polypeptides; pH adjusters or buffers; salts such as sodium chloride; and the like. These carriers may be in a crystalline or amorphous form or may be a mixture of the two.
• Bulking agents that are particularly valuable include compatible carbohydrates, polypeptides, amino acids or combinations thereof. Suitable carbohydrates include monosaccharides such as galactose, D-mannose, sorbose, and the like; disaccharides, such as lactose, trehalose, and the like; cyclodextrins, such as 2-hydroxypropyl-.beta.-cyclodextrin; and polysaccharides, such as raffinose, maltodextrins, dextrans, and the like; alditols, such as mannitol, xylitol, and the like. A preferred group of carbohydrates includes lactose, threhalose, raffinose maltodextrins, and mannitol. Suitable polypeptides include aspartame. Amino acids include alanine and glycine, with glycine being preferred.
• Suitable pH adjusters or buffers include organic salts prepared from organic acids and bases, such as sodium citrate, sodium ascorbate, and the like; sodium citrate is preferred.
• Dosage
• An iRNA agent can be administered at a unit dose less than about 75 mg per kg of bodyweight, or less than about 70, 60, 50, 40, 30, 20, 10, 5, 2, 1, 0.5, 0.1, 0.05, 0.01, 0.005, 0.001, or 0.0005 mg per kg of bodyweight, and less than 200 nmol of iRNA agent (e.g., about 4.4×1016 copies) per kg of bodyweight, or less than 1500, 750, 300, 150, 75, 15, 7.5, 1.5, 0.75, 0.15, 0.075, 0.015, 0.0075, 0.0015, 0.00075, 0.00015 nmol of iRNA agent per kg of bodyweight. The unit dose, for example, can be administered by injection (e.g., intravenous or intramuscular, intrathecally, or directly into an organ), an inhaled dose, or a topical application.
• Delivery of an iRNA agent directly to an organ (e.g., to the lung) can be at a dosage on the order of about 0.00001 mg to about 3 mg per organ, or preferably about 0.0001-0.001 mg per organ, about 0.03-3.0 mg per organ, about 0.1-3.0 mg per eye or about 0.3-3.0 mg per organ.
• The dosage can be an amount effective to treat or prevent a disease or disorder. It can be given prophylactically or as the primary or a part of a treatment protocol.
• In one embodiment, the unit dose is administered less frequently than once a day, e.g., less than every 2, 4, 8 or 30 days. In another embodiment, the unit dose is not administered with a frequency (e.g., not a regular frequency). For example, the unit dose may be administered a single time. Because iRNA agent mediated silencing can persist for several days after administering the iRNA agent composition, in many instances, it is possible to administer the composition with a frequency of less than once per day, or, for some instances, only once for the entire therapeutic regimen.
• In one embodiment, a subject is administered an initial dose, and one or more maintenance doses of an iRNA agent, e.g., a double-stranded iRNA agent, or siRNA agent, (e.g., a precursor, e.g., a larger iRNA agent which can be processed into an siRNA agent, or a DNA which encodes an iRNA agent, e.g., a double-stranded iRNA agent, or siRNA agent, or precursor thereof). The maintenance dose or doses are generally lower than the initial dose, e.g., one-half less of the initial dose. A maintenance regimen can include treating the subject with a dose or doses ranging from 0.01 to 75 mg/kg of body weight per day, e.g., 70, 60, 50, 40, 30, 20, 10, 5, 2, 1, 0.5, 0.1, 0.05, 0.01, 0.005, 0.001, or 0.0005 mg per kg of body weight per day. The maintenance doses are preferably administered no more than once every 5, 10, or 30 days. Further, the treatment regimen may last for a period of time which will vary depending upon the nature of the particular disease, its severity and the overall condition of the patient. In preferred embodiments the dosage may be delivered no more than once per day, e.g., no more than once per 24, 36, 48, or more hours, e.g., no more than once every 5 or 8 days. Following treatment, the patient can be monitored for changes in his condition and for alleviation of the symptoms of the disease state. The dosage of the compound may either be increased in the event the patient does not respond significantly to current dosage levels, or the dose may be decreased if an alleviation of the symptoms of the disease state is observed, if the disease state has been ablated, or if undesired side-effects are observed.
• The effective dose can be administered in a single dose or in two or more doses, as desired or considered appropriate under the specific circumstances. If desired to facilitate repeated or frequent infusions, implantation of a delivery device, e.g., a pump, semi-permanent stent (e.g., intravenous, intraperitoneal, intracisternal or intracapsular), or reservoir may be advisable.
• Following successful treatment, it may be desirable to have the patient undergo maintenance therapy to prevent the recurrence of the disease state, wherein the compound of the invention is administered in maintenance doses, ranging from 0.001 g to 100 g per kg of body weight (see U.S. Pat. No. 6,107,094).
• The concentration of the iRNA agent composition is an amount sufficient to be effective in treating or preventing a disorder or to regulate a physiological condition in humans. The concentration or amount of iRNA agent administered will depend on the parameters determined for the agent and the method of administration, e.g. nasal, buccal, or pulmonary. For example, nasal formulations tend to require much lower concentrations of some ingredients in order to avoid irritation or burning of the nasal passages. It is sometimes desirable to dilute an oral formulation up to 10-100 times in order to provide a suitable nasal formulation.
• Certain factors may influence the dosage required to effectively treat a subject, including but not limited to the severity of the disease or disorder, previous treatments, the general health and/or age of the subject, and other diseases present. It will also be appreciated that the effective dosage of an iRNA agent such as an siRNA used for treatment may increase or decrease over the course of a particular treatment. Changes in dosage may result and become apparent from the results of diagnostic assays. For example, the subject can be monitored after administering an iRNA agent composition. Based on information from the monitoring, an additional amount of the iRNA agent composition can be administered.
• Dosing is dependent on severity and responsiveness of the disease condition to be treated, with the course of treatment lasting from several days to several months, or until a cure is effected or a diminution of disease state is achieved. Optimal dosing schedules can be calculated from measurements of drug accumulation in the body of the patient. Persons of ordinary skill can easily determine optimum dosages, dosing methodologies and repetition rates. Optimum dosages may vary depending on the relative potency of individual compounds, and can generally be estimated based on EC50s found to be effective in in vitro and in vivo animal models as described above.
• The invention is further illustrated by the following examples, which should not be construed as further limiting.
EXAMPLES
• Nucleic acid sequences are represented below using standard nomenclature, and specifically the abbreviations of Table 3.

  TABLE 3
  Abbreviations of nucleotide monomers used in nucleic acid sequence
  representation. It will be understood that these monomers, when
  present in an oligonucleotide, are mutually linked by
  5′-3′-phosphodiester bonds.

  Abbreviationa	Nucleotide(s)
  A, a	2′-deoxy-adenosine-5′-phosphate, adenosine-5′-phosphate
  C, c	2′-deoxy-cytidine-5′-phosphate, cytidine-5′-phosphate
  G, g	2′-deoxy-guanosine-5′-phosphate, guanosine-5′-phosphate
  T, t	2′-deoxy-thymidine-5′-phosphate, thymidine-5′-phosphate
  U, u	2′-deoxy-uridine-5′-phosphate, uridine-5′-phosphate
  N, n	any 2′-deoxy-nucleotide/nucleotide
  	(G, A, C, or T, g, a, c or u)
  am	2′-O-methyladenosine-5′-phosphate
  cm	2′-O-methylcytidine-5′-phosphate
  gm	2′-O-methylguanosine-5′-phosphate
  tm	2′-O-methyl-thymidine-5′-phosphate
  um	2′-O-methyluridine-5′-phosphate
  A, C, G, T, U,	underlined: nucleoside-5′-phosphorothioate
  a, c, g, t, u
  x	universal base
  acapital letters represent 2′-deoxyribonucleotides (DNA), lower case letters represent ribonucleotides (RNA)

• Source of Reagents
• Where the source of a reagent is not specifically given herein, such reagent may be obtained from any supplier of reagents for molecular biology at a quality/purity standard for application in molecular biology.
Example 1 Selection of Sequences
• siRNA design was carried out to identify siRNAs targeting Influenza A mRNAs of MP, NP, PA, PB1 and PB2 protein. In a first round, the siRNA in silico selection resulted in 44 sequences targeting MP, 3 sequences targeting NP and 1 sequence targeting PB1. No siRNAs specific for influenza A genes PA or PB2 passed the first selection process demanding 80% target coverage and 80% target efficiency (see below).
• To setup an environment for sequence analysis, the fastA package (Pearson, W. R., & Lipman, D. J., PNAS 1988, 85:2444) was downloaded from ftp://ftp.virginia.edu/pub/ and installed on a workstation under the Suse Linux® 9.3 operating system with standard installation settings. For the purpose of running perl scripts, it was ensured that the perl interpreter, version 5.8.6 (copyright 1987-2004, Larry Wall), coming with the Suse Linux 9.3 standard installation was functional. BioEdit Sequence Alignment Editor (Hall, T. A., Nucl. Acids. Symp. Ser. 1999, 41:95) was downloaded from the Brown Lab Web Server at the web site of North Carolina State University and installed on a computer under Microsoft Windows2000® operating system.
• Workflow for the in silico selection was as follows: influenza A sequences of interest were downloaded, aligned and a statistics was generated to obtain distribution of bases at every position relative to a calculated consensus. A perl script was used to identify candidate target regions satisfying defined cut-off criteria. siRNA sequences to candidate target regions were analyzed for specificity by fasta algorithm to human RefSeq database. Another perl script was used to score siRNAs according to predicted specificity. Finally, those siRNAs were manually selected that satisfied specificity criteria.
• Influenza A sequences of interest available on Jun. 24, 2005 were downloaded from NCBI Influenza Virus Database available on the web site of the National Center for Biotechnology Information. The number of sequences per gene is shown for MP, NP, PB1, PB2, and PA in Table 4, the corresponding accession numbers are given in Table 4.

  TABLE 4
  Number of gene sequences for influenza genes MP, NP PB1, PB2, and PA from
  various viral subtypes that were employed in in silico selection of siRNA sequences

  Gene	H1N1	H2N2	H3N2	H5N1	H7N3	H7N7	H9N2	Total

  MP

  	10	2	13	166	28	16	128	363
  NP	12	3	10	169	12	6	138	350
  PB1	3	2	10	163	10	7	127	322
  PB2	2	1	10	164	12	9	133	331
  PA	2	2	10	171	11	8	124	328

• The ClustalW multiple alignment function (Thompson, J. D., et al., Nucleic Acids Res. 1994; 22:4673) of BioEdit Sequence Alignment Editor was used to generate a global alignment of all sequences using default parameters for each target, respectively. A Positional nucleotide numerical summary output was generated providing information on base distribution at every position relative to the calculated consensus sequence for each target.
• Cut-off criteria for the identification of candidate targeting regions of 19 nucleotides in length were defined as:
• Criterium 1, target coverage: at least 80% of all sequences available for the respective influenza A gene needed to be represented in a candidate region
• Criterium 2, targeting efficiency: at least 80% of all sequences in which the candidate region was represented needed to be identical within the candidate region.
• Criterium 1 was defined in order to avoid regions for which little sequence information was available, criterium 2 ensures targeting of a high number of subtypes.
• A perl script was used for screening the Positional nucleotide numerical summary file to identify candidate target regions with a length of 19 bases matching the cut-off criteria and to generate a file to be used as fastA input in the following analysis step. For script input the total number of sequences were entered for each target and a value of 80 for percentage conservation. All candidate sense siRNA sequences corresponding to the most frequent sequences in the candidate target regions were extracted and saved in a fastA-formatted file. In order to consider potential dTdT-overhang interactions of siRNAs with the target sequence, all sequences were extended at the 5′ end with ‘AA’ resulting in 21mer input sequences. A further file was generated for each candidate target region with information on region properties: target coverage (sequences present) targeting efficiency, total number of mismatches, number of conserved sequences, and number of sequences present.
• For further selection, candidate siRNAs were ranked according to their predicted potential for interacting with host (here, without limitation, human) genes (off-target potential). siRNAs with low off-target potential are assumed to be more specific in vivo.
• For predicting siRNA-specific off-target potential, the following assumptions were made:
• 1) positions 2 to 9 (counting 5′ to 3′) of a strand (seed region) contributes more to the off-target potential than the remaining sequence (non-seed region) (Haley, B., and Zamore, P. D., Nat Struct Mol. Biol. 2004, 11:599).
• 2) an off-target score can be calculated for each hit, based on identity to siRNA sequence and position of mismatches
• 3) by introducing appropriate nucleotide modifications into the sense strand (e.g. all nucleotides comprising a pyrimidine base are 2′-O-methyl modified nucleotides), the sense strand can be made inactive towards RNA interference; hence, only the off-target potential of the antisense strand need be considered
• To identify potential off-target genes, the 21 mer sequences corresponding to the candidate target regions plus a 3′-terminal AA tail (to account for the TT overhangs) were subjected to a homology search against publically available human mRNA sequences. To this purpose, fastA (version 3.4) searches were performed with all 21mer input sequences against a human RefSeq database (downloaded available version from ftp://ftp.ncbi.nih.gov/refseq/ on 2005-07-25). fastA search was executed with parameters-values-pairs—b 30-g 30 in order to take into account the homology over the full length of the 21 mer. The search resulted in a list of potential off-targets for candidate siRNAs.
• To sort the resulting list of potential off-targets, fastA output files were analyzed to identify the host gene with the highest off-target score. The following off-target properties for each 21 mer input sequence were extracted for each potential off-target to calculate the off-target score:
• 1. Number of identical nucleotides to 21mer sequence (Identity)
• 2. Number of mismatches in seed region
• The off-target score was calculated for considering assumption 1 and 2 as follows:
  Identity−0.2*number of seed mismatches
• All siRNAs were sorted according to their highest off-target score (ascending). An off-target score of 16.8 was used as a cut-off for siRNA selection. 42 siRNAs specific for influenza A matrix protein (MP), 3 siRNAs specific for influenza A nucleocapsid protein (NP), and 1 siRNA specific for influenza A Polymerase Basic protein 1 (PB1) had off target scores at or below this threshold.
• Given the comparatively low number of candidate siRNAs resulting from the above selection procedure, the Positional nucleotide numerical summary was re-examined with cut-off for criterium 1 (target coverage) set to 70% and criterium 2 (target specificity) remaining at 80%, followed by a repeat off-target score ranking as described above. 2 additional siRNAs specific for influenza A MP mRNA with a targeting efficiency of 79.9% were additionally selected, for a total of 48 candidate siRNAs. The sequences of these 48 candidate siRNAs are shown in Table 1A.
• Because the selection process described above resulted only in a limited number of candidate agents, the selection criteria were somewhat relaxed to yield further candidate agents. Specifically, criterium 1, above, was relaxed to 50% target coverage, criterium 2, target efficiency, was kept at 80%, and the above selection process was repeated. This procedure yielded the additional agents AL-DP-8001 to AL-DP-8040, listed in Table 1C.
• In this process, it was realized that the off-target scoring step led to the greatest attrition rate in potential agents. In order to obtain yet more candidate agents, the selection process was therefore repeated once more, using criterium 1 at 80% target coverage, criterium 2 at 80% target efficiency, and the off-target scoring was omitted. This procedure yielded the additional agents listed in Table 1D. Yet further candidate agents, listed in Table 1E, were obtained by repeating the selection once again, using criterium 1 at 50% target coverage, criterium 2 at 80% target efficiency, and omitting off-target scoring.
• Additional candidate iRNA agents were identified by allowing for the incorporation of universal bases. A Perl script was used to first identify candidate sequences having target coverage and target efficiency of 100% when the incorporation of up to 3 universal bases in the non-seed region (corresponding to positions 2-9 of the antisense strand) of the iRNA agent per strand. Table 1F shows the agents identified in this manner. In a second round, additional iRNA agents were identified that possess target coverage and target efficiency of 80% when allowing for the incorporation of one universal base. These iRNA agents are shown in Table 1G.
Example 2 siRNA Synthesis
• Synthesis of Nucleotides Comprising Natural Bases
• Single-stranded RNAs were produced by solid phase synthesis on a scale of 1 μmole using an Expedite 8909 synthesizer (Applied Biosystems, Applera Deutschland GmbH, Darmstadt, Germany) and controlled pore glass (CPG, 500 Å, Glen Research, Sterling Va.) as solid support. RNA and RNA containing 2′-O-methyl nucleotides were generated by solid phase synthesis employing the corresponding phosphoramidites and 2′-O-methyl phosphoramidites, respectively (Proligo Biochemie GmbH, Hamburg, Germany). These building blocks were incorporated at selected sites within the sequence of the oligoribonucleotide chain using standard nucleoside phosphoramidite chemistry such as described in Current protocols in nucleic acid chemistry, Beaucage, S. L. et al. (Edrs.), John Wiley & Sons, Inc., New York, N.Y., USA. Phosphorothioate linkages were introduced by replacement of the iodine oxidizer solution with a solution of the Beaucage reagent (Chruachem Ltd, Glasgow, UK) in acetonitrile (1%). Further ancillary reagents were obtained from Mallinckrodt Baker (Griesheim, Germany).
• Deprotection and purification by anion exchange HPLC of the crude oligoribonucleotides were carried out according to established procedures. Yields and concentrations were determined by UV absorption of a solution of the respective RNA at a wavelength of 260 nm using a spectral photometer (DU 640B, Beckman Coulter GmbH, Unterschleiβheim, Germany). Double stranded RNA was generated by mixing an equimolar solution of complementary strands in annealing buffer (20 mM sodium phosphate, pH 6.8; 100 mM sodium chloride), heated in a water bath at 85-90° C. for 3 minutes and cooled to room temperature over a period of 3-4 hours. The purified RNA solution was stored at −20° C. until use.
• As a result of the synthesis strategy described above, all oligonucleotides synthesized as described above do not comprise a phosphate group on their 5′-most nucleotide.
• Synthesis of Nucleotides Comprising Universal Bases
Synthesis of Phosphoramidite and controlled pore glass support of 5′-O-(4,4′-dimethoxitrityl)-2′-O-(tert-butyldimethylsilyl)-1′-(5-nitroindole)-D-riboside
• 
Step A: 1-O-Methyl-D-riboside (102)
• To a solution of D-ribose (25 g) in dry methanol (300 mL) was added conc. sulfuric acid (1.88 mL) and stirred at room temperature for 3 days. The reaction mixture was then neutralized with 1 N sodium hydroxide solution and concentrated into a crude residue. The crude residue was dissolved in methanol (200 mL) and the solids were filtered off. The filtrate was concentrated into a crude residue, which was applied to a column of silica gel eluted with dichloromethane-methanol (5:1) to give a pure compound (23.0 g, 82%) as a syrup.
Step B: 1-O-Methyl-2,3,5-tri-O-(2,4-dichlorobenzyl)-D-riboside (103)
• To a solution of 1-O-methyl-D-riboside (13.43 g, 81.83 mmol), 18-crown-6 (1.34 g) in dry THF (100 mL) was added powdered potassium hydroxide (69 g, 1.23 mol) and stirred at room temperature for 40 to 60 min. 2,4-Dichlorobenzyl chloride (51 mL, 368.2 mmol) was added dropwise and the reaction mixture was stirred at the same temperature overnight. The solids were filtered off and the filtrate was concentrated into a crude residue which was applied to a column of silica gel eluted with hexanes-ethyl acetate (4:1) to give a pure compound (48 g, 92%) as a white solid.
• ¹H-NMR (CDCl₃, 400 MHz): δ 7.46-7.34 (m, 5H, ArH), 7.24-7.16 (m, 4H, ArH), 4.99 (s, 1H, H-1), 4.71 (dd, 2H, J_gem=12.8 Hz, OCH₂Ar), 4.63-4.61 (m, 4H, 2 OCH₂Ar), 4.38-4.36 (m, 1H), 4.19-4.16 (dd, 1H), 3.98 (d, 1H, J=4.4 Hz), 3.75 (dd, 1H, J=3.6, J=10.2 Hz, H-5a), 3.66 (dd, 1H, J=3.6, J=10.4 Hz, H-5b), 3.37 (s, 3H, OCH₃).
Step B: 1-Bromo-2,3,5-tri-O-(2,4-dichlorobenzyl)-D-ribose (104)
• To a cold solution of 1-O-methyl-2,3,5-tri-O-(2,4-dichlorobenzyl)-D-riboside (3.22 g, 5.02 mmol) in dry dichloromethane (50 mL) cooled with ice-bath was added HOAc-HBr (5.3 mL, 30%) and stirred at 0-25° C. for 3 h. The reaction mixture was concentrated into a crude residue which was co-evaporated with toluene (3×30 mL) into a crude residue which was dried under a good vacuum and used for next reaction without purification and identification as a syrup.
Step D: 1-(5-Nitroindole)-2,3,5-tri-O-(2,4-dichlorobenzyl)-D-riboside (105)
• To a solution of 5-nitroindole (2.44 g, 15.06 mmol) in dry CH₃CN (30 mL) was added sodium hydride (602 mg, 15.06 mmol, 60%) and stirred at room temperature for 3-4 h under an argon atmosphere. The above obtained sugar donor (104) in dry CH₃CN (10 mL) was added and stirred at the same temperature under an argon atmosphere overnight. The solids were filtered off and the filtrate was concentrated into a crude residue which was applied to a column of silica gel eluted with hexanes-ethyl acetate (3:1) to give a pure compound 105 (2.16 g, 60%) as a α and β mixture (1:1).
Steps E, F: 5′-O-(4,4′-dimethoxitrityl)-1′-(5-nitroindole)-D-riboside (106) and (107)
• To a cold solution of 1-(5-nitroindole)-2,3,5-tri-O-(2,4-dichlorobenzyl)-D-riboside 105 (1.16 g, 1.51 mmol) in dry dichloromethane (100 mL) at −78° C. was added BCl₃ in dichloromethane (23 mL, 1.0M) and stirred at the same temperature for 2 h under an argon atmosphere and at −40° C. for 2 h. The reaction mixture was quenched with methanol-dichloromethane (1:1, 50 mL) and neutralized with ammonia-methanol solution. The solids were filtered off and the filtrate was concentrated into a crude residue which was applied to a column of silica gel eluted with dichloromethane-methanol (10:1) to give a pure compound (300 mg, 68%) as a α and β mixture (1:1). To a solution of the above obtained compound (840 mg, 2.86 mmol) in dry pyridine (3-4 ml) and DMAP (90 mg) was added DMTrCl (1.06 g) and stirred at room temperature under an argon atmosphere overnight. The reaction mixture was concentrated into a crude residue which was applied to a column of silica gel eluted with hexanes-ethyl acetate (1:1) to give a pure compound 106 (550 mg) and compound 107 (190 mg), a mixture of compound 106 and 107 (360 mg).
• Compound 106: ¹H-NMR (CDCl₃, 2D g-COSY and 2D NOESY, 400 MHz): δ 8.49 (d, 1H, J=1.6 Hz), 8.35 (d, 1H), 8.03 (dd, 1H, J=2.0, J=9.0 Hz), 7.70-7.69 (m, 2H), 7.47-7.14 (m, 8H, ArH), 6.86-6.81 (m, 5H, ArH), 6.71 (d, 1H, J=3.6 Hz), 6.41 (d, J=5.2 Hz, H′-1), 4.73 (t, 1H, J=4.8 Hz, H′-2), 4.46-4.42 (m, 3H, H′-3, H′-4, H′-5), 3.79 (s, 6H, 2OCH₃), 3.51 (dd, 1H, J=3.2, J=10.4 Hz, H′-5a), 3.26 (dd, 1H, J=3.2, J=10.6 Hz, H′-5b).
• Compound 107: ¹H-NMR (CDCl₃, 2D g-COSY and 2D NOESY, 400 MHz): δ 8.55 (d, 1H, J=2.0 Hz), 7.98 (dd, 1H, J=2.4, J=9.2 Hz), 7.60 (d, 1H, J=9.2 Hz), 7.53 (d, 1H, J=3.2 Hz), 7.44-7.42 (m, 2H), 7.34-7.24 (m, 7H, ArH), 6.84-6.81 (m, 4H, ArH), 6.68 (d, 1H, J=3.2 Hz), 6.00 (d, 1H, J=5.2 Hz, H′-1), 4.53 (t, 1H, J=7.6 Hz), 4.46-4.44 (m, 1H), 4.23-4.20 (m, 1H), 3.80-3.76 (m, 7H, 2OCH₃, H′-5), 3.55 (dd, 1H, H′-5a), 3.43 (dd, 1H, H′-5b).
Step G: 5′-O-(4,4′-dimethoxitrityl)-2′-O-(tert-butyldimethylsilyl)-1′-(5-nitroindole)-D-riboside (108) and 5′-O-(4,4′-dimethoxitrityl)-3′-O-(tert-butyldimethylsilyl)-1′-(5-nitroindole)-D-riboside (109)
• To a solution of 5′-O-(4,4′-dimethoxitrityl)-1′-(5-nitroindole)-D-riboside (106) (550 mg, 0.92 mmol), AgNO₃ (188 mg, 1.104 mmol), and pyridine (0.74 mL, 9.2 mmol) in dry THF (9.2 mL) was added TBDMSCl (188 mg, 1.196 mmol) and stirred at room temperature under an argon atmosphere overnight. The solids were filtered off and the filtrate was concentrated into a crude residue which was applied to a column of silica gel eluted with hexanes-ethyl acetate (4:1) to give a pure compound 108 (230 mg, 35%), compound 109 (150 mg, 23%), and a mixture of compound 108 and 109 (110 mg, 17%) in total yield of 75%.
• Compound 108: ¹H-NMR (CDCl₃, 2D g-COSY, 2D NOESY, 400 MHz): δ 8.56 (d, 1H, J=2.4 Hz), 7.88 (dd, 1H, J=2.4, J=8.8 Hz), 7.62 (d, 1H, J=9.2 Hz), 7.54 (d, 1H, J=3.6 Hz), 7.46-7.44 (m, 2H), 7.36-7.25 (m, 6H, ArH), 6.85-6.83 (d, 5H, ArH), 6.69 (d, 1H, J=3.6 Hz), 5.94 (d, 1H, J=7.2 Hz, H′-1), 4.69 (dd, 1H, H′-2), 4.31-4.29 (m, 2H, H′-3, H′-4), 3.80 (s, 6H, 2OCH₃), 3.58 (dd, 1H, J=2.0, J=10.6 Hz, H′-5a), 3.40 (dd, 1H, J=2.0, J=10.4 Hz, H′-5b), 2.85 (d, 1H, J=0.8 Hz, 3′-OH), 0.78 (s, 9H, t-Bu), −0.016 (s, 3H, SiCH₃), −0.43 (s, 3H, SiCH₃).
• Compound 109: ¹H-NMR (CDCl₃, 2D g-COSY, 2D NOESY, 400 MHz): δ 8.61 (d, 1H, J=2.4 Hz), 8.05 (dd, 1H, J=2.0, J=8.8 Hz), 7.69-7.65 (m, 2H), 7.47-7.45 (m, 2H, ArH), 7.36-7.27 (m, 5H, ArH), 6.86-6.83 (m, 3H, ArH), 6.71 (d, 1H, J=3.2 Hz), 5.99 (d, 1H, J=4.8 Hz, H′-1), 4.51 (t, 1H, J=4.8 Hz, J=5.6 Hz, H′-3), 4.40-4.36 (m, 1H, H′-2), 4.17-4.15 (m, 2H, H′-4, H′-5), 3.82 (s, 3H, OCH₃), 3.81 (s, 3H, OCH₃), 3.63 (dd, 1H, J=2.4, J=11.0 Hz, H′-5a), 3.31 (dd, 1H, J=2.8, J=11.0 Hz, H′-5b), 2.95 (d, 1H, J=6.0 Hz, 2′-OH), 0.91 (s, 9H, t-Bu), 0.05 (s, 3H, SiCH₃), 0.00 (s, 3H, SiCH₃).
Step H: 5′-O-(4,4′-dimethoxitrityl)-2′-O-(tert-butyldimethylsilyl)-1′-(5-nitroindole)-D-riboside-3′-O-cyanoethyl-N,N-diisopropylphosphoramidate (110)
• 2-Cyanoethyl-N,N-diisopropylchlorophosphoramidite (153 mg, 0.646 mmol) was added to a solution of 5′-O-(4,4′-dimethoxitrityl)-3′-O-(tert-butyldimethylsilyl)-1-(5-nitroindole)-D-β-riboside 108 (230 mg, 0.323 mmol), diisopropylethylamine (306 uL, 1.78 mmol) and DMAP (10 mg) in dry dichloromethane (3 mL) and stirred at room temperature for 4-6 h under an argon atmosphere. The reaction mixture was concentrated to a crude residue which was applied to a column of silica gel which was saturated with 2% triethylamine in hexanes and eluted with hexanes-ethyl acetate (2:1) to give a pure title compound 110 (250 mg, 85%) as an amorphous solid.
• ³¹P-NMR (CDCl3, 400 MHz): δ 149.54 (s), 146.57 (s). Anal. Cald of C₅₀H₆₅N₄O₉PSi: 924.43. Found: 947.43 [M+Na]⁺.
Step I: Solid supports of 2′-hydroxyl or 3′-hydroxyl of 5′-O-(4,4′-dimethoxitrityl)-1-(5-nitroindole)-D-riboside (111)
• Succinic anhydride was added to a solution of a mixture of 2′-OTBDMS (108) or 3′-O-TBDMS of 5′-O-(4,4′-Dimethoxitrityl)-1-(5-nitroindole)-D-β-riboside (109), and DMAP in dry dichloromethane. The reaction mixture is stirred at room temperature under an argon atmosphere for 6 h. Another portion of succinct anhydrous and DMAP are added and stirred for total of 16 h. The mixture is concentrated to a crude residue which is dissolved in ethyl acetate (50 ml), washed with citric acid (400 mg/20 ml), brine, and dried (Na₂SO₄). The organic layer is concentrated to a crude nucleoside succinate which was directly used for next reaction without further purification.
• Nucleoside succinate, DMAP, DTNP, and Ph₃P are agitated at room temperature for 20 min [Nucleoside and nucleotides, 1996, 15(4), 879-888.]. Then 1caa-CPG is added and agitated at the same temperature for 45 min. The solids are filtered off and washed with CH₃CN, dichloromethane, and ether. The solid supports are dried, capped under standard procedure, and washed to give solid support.
• The nitroindole-comprising Controlled Glass Support and phosphoramidate thus obtained are employed in standard oligonucleotide synthesis as described above for oligonucleotides comprising natural bases.
Example 3 siRNA Testing In Vitro
• The ability of the iRNA agents to inhibit replication of influenza virus was tested in human cell lines in vitro, or is tested in mice in vivo. The iRNA agent is transfected into the cells, e.g., by transfection or electroporation, allowed to act on the cells for a certain time, e.g., 24 hours, and levels of infectivity were determined by a plaque forming or ELISA assay. Complementing these direct assays, we tested the inhibition of target gene expression by RNAi Agents for several influenza genes recombinantly expressed in mammalian host cells.
• Viruses and Cell Lines
• Influenza virus A/PR/8/34 (PR8), subtype H1N1, was obtained from Charles River Laboratories (ATCC #VR-1469). A/WSN/33 (WSN), subtype H1N1, may be obtained from Thomas Chambers, University of Kentucky, Lexington, Ky. USA (see Castrucci, M. R., et al., J. Virol. 1992, 66:4647), or Dr. Peter Palese, Mount Sinai School of Medicine New York City, N.Y., USA (see WO 04/028471). Virus stocks were propagated in the allantoic cavity of embryonated hen eggs at 34° C. for 48-72 h (PR8) or 37° C. for 24 h (WSN) (Tompkins, S. M., et al. Proc. Natl. Acad. Sci. 2004, 101:8682).
• MDCK cells were obtained from the American Type Culture Collection (ATCC, Rockville Md., USA; ATCC #CCL-34) and were grown in MEM containing 8% heat-inactivated fetal bovine serum (FBS), 2 mM L-glutamine, 1 mM Sodium Pyruvate, 1.5 g/L sodium bicarbonate and non-essential amino acids at 37° C. under a 5% CO₂/95% air atmosphere.
• Vero E6 African green monkey kidney epithelial cells were obtained from ATCC (Rockville Md., USA, ATCC #CRL-1586) and were grown in DMEM supplemented with 4.5 g/1 D-Glucose, 2 mM L-Glutamine, 110 mg/l sodium pyruvate, 10% fetal bovine serum (Hyclone, Cat #30070.03) and 0.1% Penicillin/Streptomycin at 37° C. under a 5% CO₂/95% air atmosphere.
• Cos-7 African green monkey kidney cells were obtained from the German Collection of Microorganisms and Cell Cultures (DSMZ, Braunschweig, Germany, DSMZ #ACC 60) and were grown in Dulbecco's MEM, 10% fetal calf serum, 2 mM L-glutamine, 1.2 μg/ml sodium bicarbonate, 100 u penicillin/100 μg/ml streptomycin (Biochrom AG, Berlin, Germany).
Example 3.1 Plaque Forming Assay
• Cell Culture, siRNA Transfection, and Virus Infection.
• MDCK cells were plated in 24-well plates at 7.5×10⁴ cells per well in 0.5 ml growth medium a day before transfection. MDCK cells were 80% confluent the day of siRNA transfection. Before transfection cells are fed with 0.25 ml growth medium.
• Prior to adding to cells, 1.5 ml (50 μl per well) Optimem I (Invitrogen) and 90 μl (3 μl per well) Lipofectamin 2000 (Invitrogen), the amount sufficient for transfection of one 24 well plate, were combined in a 2 ml Sarstedt tube and incubated for 10-15 minutes at room temperature. The appropriate amount of siRNA dissolved in annealing buffer is then added to the Optimem/lipofectamine 2000 mixture to give the desired final concentration, mixed, and incubated an additional 15-25 minutes at room temperature. Next, 50 μl of the siRNA/reagent complex is added dropwise to each well as dictated by the experimental design. Plates are then gently rocked to ensure complete mixing and incubated at 37° C. at 5% CO2/95% air for 14 hours.
• Subsequently, the transfection medium was gently aspirated, cells washed once with 0.25-0.5 ml of PBS, and 100 μl of varying concentrations of PR8 in MEM medium was added to each well. After incubation at 37° C. for 1-2 hour, 0.5 ml of overlay media (MEM, 20 mM HEPES, 0.075% NaHCO3, 2 mM glutamine, 0.6% agarose, 0.5 μg/ml TPCK-trypsin) were added, and plates incubated for 48 hrs at 37° C. in an incubator at 5% CO2/95% air. Plates were then fixed and immunostained for viral plaques as described below.
• Immunostaining and Viral Quantitation
• 48 hours post-infection, cells were fixed in neutral buffered 10% formalin for 45 minutes, and wells rinsed with PBS. Wells were then blocked with permeabilization buffer (1×PBS, 2% FBS, 0.5% saponin, 0.1% sodium azide) for 15 minutes at room temperature, and 125 μl of a solution containing 0.5 μg/ml mouse anti-influenza A biotinylated antibody MAB8258B (Chemicon) was added. Following incubation for 1 hr at room temperature, wells were rinsed twice with PBS to remove unbound antibody, and 125 μl of a solution of 1 μg/ml of horse radish peroxidase (HRP) conjugated streptavidin (Vector Laboratories) in PBS per well was added, plates incubated for 45 min, and washed three times with PBS. 200 μl of TMB substrate (Vector Laboratories #SK-4400) per well were added. Following incubation for 5-10 minutes at room temperature in the dark, the calorimetric reaction was stopped with distilled water, the water discarded and the plates air-dried. Stained influenza plaques were counted by inverted light microscopy at 4× magnification. Plaque forming activity was compared to cells transfected with Lipofectamin only (mock-treated), and expressed in terms of [(plaque forming activity in treated cells)/(plaque forming activity in mock-treated cells)]×100=% remaining infectivity
Example 3.2 ELISA Assay
• MDCK or Vero cells were plated in 96-well plates at 10⁴ cells per well in 0.1 ml growth medium a day before transfection. The cells were 80% confluent the day of siRNA transfection. Before transfection, cells were fed with 44 μl growth medium.
• 1.08 ml (9 μl per well) Optimem I (Invitrogen) and 42 μl (0.35 μl per well) Lipofectamin 2000 (Invitrogen), the amount sufficient for transfection of one 96 well plate, were combined in a 2 ml Sarstedt tube and incubated for 10-15 minutes at room temperature. The appropriate amount of siRNA dissolved in annealing buffer was then added to the Optimem/lipofectamine 2000 mixture to give the desired final concentration, mixed, and incubated an additional 15-25 minutes at room temperature. Next, 10 μl of the siRNA/reagent complex was added to each well as dictated by the experimental design. Plates were gently rocked to ensure complete mixing and then incubated at 37° C. in an incubator at 5% CO₂/95% air for 14 hours.
• Subsequently, cells were washed once with PBS, infected with PR8 influenza virus in 50 μl of MEM per well, and incubated for 1-2 hours. Thereafter, plates were washed once with PBS, and 200 μl of MEM with 0.25/0.5 μg/ml (MDCK/VERO, respectively) of trypsin were added. Two days post infection, plates were fixed in 10% Buffered Formalin for 15 min. Cells were rinsed with PBS, blocked with blocking buffer for 15 min. at RT, and 50 μl of a solution containing 0.5 μg/ml of biotinylated anti-influenza A monoclonal antibody MAB8258B (Chemicon) per well were added. Plates were incubated at RT for 1 hour, washed twice with PBS, and 50 μl per well of a solution containing 1 μg/ml of AP-conjugated streptavidin (Vector Laboratories) in blocking buffer was added. After incubation for 45 min and washing 3× with PBS, 100 μl per well of pNPP substrate solution was added. Plates were developed at RT in the dark and read at 405 nm.
Example 3.3 Inhibition of Recombinantly Expressed Influenza Target Genes by siRNA
• Consensus sequences of MP (SEQ ID NO: 1453), NP (SEQ ID NO: 1454), PA (SEQ ID NO: 1455), PB1 (SEQ ID NO: 1456) and PB2 (SEQ ID NO: 1457) (see Table 5) were synthesized by GENEART (Regensburg, Germany) and cloned into GENEART standard vectors. MP and PA were subcloned into psiCheck-2 (Promega, Mannheim, Germany) via AsiSI and NotI (both NEBn, Frankfurt, Germany) sites, NP, (PB1) and PB2 via XhoI and NotI, resulting in a construct with the flu gene between the stop-codon and the polyA-signal of Renilla luciferase. Correct cloning was confirmed by end sequencing performed by GATC Biotech (Konstanz, Germany).
• Transfections:
• Cos-7 cells were seeded at 1.5×10⁴ cells/well on white 96-well plates with clear bottom (Greiner Bio-One GmbH, Frickenhausen, Germany) in 75 μl of growth medium. Directly after seeding the cells, 50 ng of plasmid/well were transfected with Lipofectamine2000 (Invitrogen) as described below for the siRNAs, with the plasmid diluted in Opti-MEM to a final volume of 12.5 μl/well, prepared as a mastermix for the whole plate.
• siRNA transfections were performed in quadruplicates 4 h after plasmid transfection. For each well 0.5 μl Lipofectamine2000 (Invitrogen GmbH, Karlsruhe, Germany) were mixed with 12 μl Opti-MEM (Invitrogen) and incubated for 15 min at room temperature. For an siRNA concentration of 50 nM in the 100 μl transfection volume, 1 μl of a 5 μM siRNA were mixed with 11.5 μl Opti-MEM per well, combined with the Lipofectamine2000-Opti-MEM mixture and again incubated for 15 minutes at room temperature. During incubation, the growth medium was removed from cells and replaced by 75 μl/well of fresh medium. siRNA-Lipofectamine2000-complexes were applied completely (25 μl each per well) to the cells and cells were incubated for 24 h at 37° C. and 5% CO₂ in a humidified incubator (Heraeus GmbH, Hanau, Germany).
• Cells were harvested by removing growth medium and application of 150 μl of a 1:1 mixture consisting of medium and Dual-Glo Luciferase substrate, from the Dual-Glo Luciferase Assay System (Promega, Mannheim, Germany). The luciferase assay was performed according to the manufacturer's protocol for Dual-Glo Luciferase assay and luminescence was measured in a Victor-Light 1420 Luminescence Counter (Perkin Elmer, Rodgau-Jügesheim, Germany). Values obtained with Renilla luciferase were normalized to the respective values obtained with Firefly luciferase. Values acquired with siRNAs directed against an influenza gene were normalized to the value obtained with an unspecific siRNA (directed against neomycin resistance gene) set to 100%.
• Effective siRNAs from the screen were further characterized by dose response curves. Transfections of dose response curves were performed at the following siRNA concentrations according to the above protocol: 100 nM, 25 nM, 6.3 nM, 1.6 nM, 400 pM, 100 pM, 24 pM, 6 pM, 1.5 pM, 380 fM. IC₅₀ values determined by parametrized curve fitting using the program XLfit.

  TABLE 5
  Virtual consensus sequences for influenza genes MP (SEQ ID NO: 1453),
  NP (SEQ ID NO: 1454), PA (SEQ ID NO: 1455), PB1 (SEQ ID NO: 1456) and
  PB2 (SEQ ID NO: 1457) for cloning into Cos-7 cells

  MP: virtual consensus derived from gi|13383290|gb|AB049165|
  Influenza A virus (A/parakeet/Chiba/1/97(H9N2)) M1, M2 genes for
  membrane ion channel, matrix protein, complete ads.

  SEQ ID NO: 1453

  ATGAGTCTTC TAACCGAGGT CGAAACGTAC GTTCTCTCTA TCATCCCGTC AGGCCCCCTC  60
  AAAGCCGAGA TCGCGCAGAG ACTTGAAGAT GTCTTTGCAG AGAAGAACAC AGATCTCGAG 120
  GCTCTCATGG AATGGCTAAA GACAAGACCA ATCCTGTCAC CTCTGACTAA GGGGATTTTA 180
  GGGTTTGTGT TCACGCTCAC CGTGCCCAGT GAGCGAGGAC TGCAGCGTAG ACGCTTTGTC 240
  CAGAATGCCC TAAATGGGAA TGGAGACCCA AACAACATGG ACAGGGCAGT TAAACTATAC 300
  AAGAAGCTGA AGAGGGAAAT AACATTCCAT GGGGCTAAGG AAGTTGCACT CAGTTACTCT 360
  GCTGGTGCAC TTGCCAGTTG CATGGGTCTC ATATACAACC GGATGGGAAC AGTGACCACA 420
  GAAGTGGCTC TTGGCCTAGT GTGTGCCACT TGTGAGCAGA TTGCAGATTC ACAACATCGG 480
  TCCCACAGGC AGATGGCGAC TACCACCAAC CCACTAATCA GACATGAGAA CAGAATGGTG 540
  CTGGCCAGCA CTACAGCTAA GGCTATGGAG CAGATGGCTG GATCAAGTGA GCAGGCAGCG 600
  GAAGCCATGG AAGTCGCAAG TCAGGCTAGG CAGATGGTGC AGGCAATGAG GACAATTGGG 660
  ACTCATCCTA GCTCCAGTGC AGGTCTAAAA GATAATCTTC TTGAAAATTT GCAGGCCTAC 720
  CAGAAACGAA TGGGGGTGCA GATGCAGCGA TTCAAGTGAT CCTCTCGTTG TTGCAGCAAG 780
  TATCATTGGG ATCTTGCACT TGATATTGTG GATTCTTGAT CGTCTTTTCT TCAAATGCAT 840
  TTATCGTCGC CTTAAATACG GTTTGAAAAG AGGGCCTTCT ACGGAAGGAG TACCTGAGTC 900
  TATGAGGGAA GAGTATCGAC AGGAACAGCA GAGTGCTGTG GATGTTGACG ATGGTCATTT 960
  TGTCAACATA GAGCTGGAGT AA                                          982
  NP: virtual consensus derived from H5N1 gi|14326108|AF370122|
  Influenza A virus (A/Goose/Guangdong/3/97(H5N1)) nucleoprotein gene,
  complete cds.

  SEQ ID NO: 1454

  CTCACTGAGT GACATCAAAA TCATGGCGTC TCAAGGCACC AAACGATCTT ATGAACAGAT   60
  GGAAACTGGT GGAGAACGCC AGAATGCTAC TGAGATCAGA GCATCTGTTG GAAGAATGGT  120
  TGGTGGAGTT GGGAGGTTTT ATATACAGAT GTGCACTGAA CTCAAACTCA GCGACTATGA  180
  AGGAAGGCTG ATTCAGAACA GCATAACAAT AGAGAGAATG GTTGTCTCTG CATTTGATGA  240
  AAGGAGGAAC AAATACCTGG AAGAACATCC CAGTGCGGGG AAGGACCCAA AGAAAACTGG  300
  AGGTCCAATC TACCGAAGAA GAGACGGGAA ATGGGTGAGA GAGCTGATTC TGTATGACAA  360
  AGAGGAGATC AGGAGAATTT GGCGTCAAGC GAACAATGGA GAAGATGCAA CTGCTGGTCT  420
  CACTCACCTG ATGATCTGGC ATTCCAATCT AAATGATGCC ACATACCAGA GAACAAGAGC  480
  TCTCGTGCGT ACTGGGATGG ACCCTAGAAT GTGCTCTCTG ATGCAAGGAT CAACTCTCCC  540
  GAGGAGATCT GGAGCTGCTG GTGCGGCAGT AAAGGGAGTC GGAACTATGG TGATGGAACT  600
  AATTCGGATG ATAAAGCGAG GGATTAACGA TCGGAATTTC TGGAGAGGTG AAAATGGGCG  660
  AAGAACAAGG ATTGCATATG AGAGAATGTG CAACATTCTC AAAGGGAAAT TCCAAACAGC  720
  AGCACAAAGA GCAATGATGG ATCAGGTACG GGAAAGCAGA AATCCTGGGA ATGCTGAGAT  780
  CGAAGATCTC ATATTTCTGG CACGGTCTGC ACTCATCCTG AGAGGATCAG TGGCCCACAA  840
  GTCCTGCTTG CCTGCTTGTG TGTACGGGCT TGCCGTGGCC AGTGGATATG ACTTTGAGAG  900
  AGAAGGGTAC TCTCTGGTCG GGATTGATCC TTTCCGTCTG CTGCAAAACA GCCAGGTCTT  960
  TAGTCTAATT AGACCAAATG AGAATCCAGC ACATAAAAGT CAATTGGTGT GGATGGCATG 1020
  CCATTCTGCA GCATTTGAAG ATCTGAGAGT CTCAAGCTTC ATCAGAGGGA CAAGAGTGGC 1080
  CCCAAGGGGA CAACTATCTA CTAGAGGAGT ACAAATTGCT TCAAATGAGA ACATGGAAAC 1140
  AATGGACTCC AGCACTCTTG AACTGAGAAG CAGATATTGG GCTATAAGGA CCAGGAGTGG 1200
  AGGAAACACC AACCAGCAGA GAGCATCTGC AGGACAAATC AGTGTGCAGC CTACTTTCTC 1260
  GGTACAGAGA AATCTTCCCT TCGAAAGAGC GACCATTATG GCGGCATTCA CAGGGAATAC 1320
  AGAGGGCAGA ACATCTGACA TGAGGACTGA AATCATAAGG ATGATGGAAA GCTCCAGACC 1380
  AGAAGATGTG TCTTTCCAGG GGCGGGGAGT CTTCGAGCTC TCGGACGAAA AGGCAACGAA 1440
  CCCGATCGTG CCTTCCTTTG ACATGAGTAA TGAAGGATCT TATTTCTTCG GAGACAATGC 1500
  AGAGGAGTAT GACAATTGAA G                                           1521
  PA: virtual consensus derived from H5N1gi|47156500|AY585473|
  Influenza A virus (A/duck/Guangxi/35/2001(H5N1)) polymerase (PA)
  mRNA, complete ads.

  SEQ ID NO: 1455

  ATGGAAGACT TTGTGCGACA ATGCTTCAAT CCAATGATTG TCGAGCTTGC GGAAAAGGCA   60
  ATGAAAGAAT ATGGGGAAGA TCCGAAAATC GAAACGAACA AATTTGCAGC AATATGCACA  120
  CACTTAGAAG TCTGTTTCAT GTATTCAGAT TTTCACTTTA TTGATGAACG GGGCGAATCA  180
  ATAATTGTAG AATCTGGCGA TCCGAATGCA TTATTGAAAC ACCGATTTGA AATAATTGAA  240
  GGAAGAGACC GAACAATGGC CTGGACAGTG GTGAATAGTA TCTGCAACAC CACAGGAGTT  300
  GAGAAACCTA AATTTCTCCC AGATTTGTAT GACTACAAAG AGAACCGATT CATTGAAATT  360
  GGAGTGACAC GGAGGGAAGT TCATATATAC TATCTAGAGA AAGCCAACAA GATAAAATCC  420
  GAGAAGACAC ACATTCACAT ATTCTCATTC ACTGGGGAGG AAATGGCCAC CAAAGCGGAC  480
  TACACCCTTG ATGAAGAGAG CAGGGCAAGA ATCAAAACCA GGCTGTTCAC CATAAGGCAG  540
  GAAATGGCCA GTAGGGGTCT ATGGGATTCC TTTCGTCAGT CCGAGAGAGG CGAAGAGACA  600
  ATTGAAGAAA GATTTGAAAT CACAGGAACC ATGCGCAGGC TTGCCGACCA AAGTCTCCCA  660
  CCGAACTTCT CCAGCCTTGA AAACTTTAGA GCCTATGTGG ATGGATTCGA ACCGAACGGC  720
  TGCATTGAGG GCAAGCTTTC TCAAATGTCA AAAGAAGTGA ACGCCAGAAT TGAGCCATTT  780
  CTGAAGACAA CACCACGCCC TCTCAGATTA CCTGATGGGC CTCCCTGCTC TCAGCGGTCG  840
  AAGTTCTTGC TGATGGATGC CCTTAAATTA AGCATCGAAG ACCCGAGTCA TGAGGGGGAG  900
  GGGATACCGC TATATGATGC AATCAAATGC ATGAAAACAT TTTTCGGCTG GAAAGAGCCC  960
  AACATCGTAA AACCACATGA AAAAGGCATA AACCCCAATT ACCTCCTGGC TTGGAAGCAA 1020
  GTGCTGGCAG AACTCCAAGA TATTGAAAAT GAGGAGAAAA TCCCAAAAAC AAAGAACATG 1080
  AAGAAAACAA GCCAATTGAA GTGGGCACTC GGTGAGAACA TGGCACCAGA GAAAGTAGAC 1140
  TTTGAGGATT GCAAAGATGT TAGCGATCTA AGACAGTATG ACAGTGATGA ACCAGAGCCT 1200
  AGATCACTAG CAAGCTGGAT CCAGAGTGAA TTCAACAAGG CATGTGAATT GACAGATTCG 1260
  AGTTGGATTG AACTTGATGA AATAGGGGAA GACGTTGCTC CAATTGAGCA CATTGCAAGT 1320
  ATGAGAAGGA ACTATTTCAC AGCGGAAGTA TCCCATTGCA GGGCCACTGA ATACATAATG 1380
  AAGGGGGTGT ACATAAACAC AGCTCTGTTG AATGCATCCT GTGCAGCCAT GGATGACTTT 1440
  CAACTGATTC CAATGATAAG CAAATGCAGA ACCAAAGAAG GAAGACGGAA AACTAACCTG 1500
  TATGGATTCA TTATAAAAGG AAGATCCCAT TTGAGGAATG ATACCGATGT GGTAAACTTT 1560
  GTGAGTATGG AATTCTCTCT TACTGACCCG AGGCTGGAGC CACACAAGTG GGAAAAGTAC 1620
  TGTGTTCTCG AGATAGGAGA CATGCTCCTA CGGACTGCAA TAGGCCAAGT TTCAAGGCCC 1680
  ATGTTCCTGT ATGTGAGAAC CAATGGAACC TCCAAGATCA AAATGAAATG GGGAATGGAG 1740
  ATGAGGCGAT GCCTTCTTCA ATCCCTTCAA CAGATTGAGA GCATGATTGA GGCCGAGTCT 1800
  TCTGTCAAAG AGAAAGACAT GACCAAAGAA TTCTTTGAAA ACAAATCAGA AACATGGCCA 1860
  ATTGGAGAGT CACCCAAAGG AGTGGAGGAA GGCTCCATCG GGAAGGTGTG CAGAACCTTA 1920
  CTGGCGAAAT CTGTGTTCAA CAGTCTATAT GCATCTCCAC AACTCGAGGG GTTTTCAGCT 1980
  GAATCAAGAA AATTGCTTCT CATTGTTCAG GCACTTAGGG ACAACCTGGA ACCTGGGACC 2040
  TTCGATCTTG GAGGGCTATA TGAAGCAATT GAGGAGTGCC TGATTAATGA TCCCTGGGTT 2100
  TTTGCTTAATG CGTCTTGGTT CAACTCCTTC CTCACACATG CACTGAAATA GTT       2153
  PB1: virtual consensus derived from H5N1gi|58531084|AB166860|
  Influenza A virus (A/chicken/Yamaguchi/7/2004(H5N1)) PB1 gene for
  polymerase basic protein 1, complete ads.

  SEQ ID NO: 1456

  ATGGATGTCA ATCCGACTTT ACTTTTCTTG AAAGTACCAG TGCAAAATGC TATAAGTACC   60
  ACATTCCCTT ATACTGGAGA CCCTCCATAC AGCCATGGAA CAGGGACAGG ATACACCATG  120
  GACACAGTCA ACAGAACACA CCAATATTCA GAAAAGGGGA AGTGGACAAC AAACACAGAG  180
  ACTGGAGCAC CCCAACTCAA CCCGATTGAT GGACCACTAC CTGAGGATAA TGAGCCCTGT  240
  GGGTATGCAC AAACAGATTG TGTATTGGAA GCAATGGCTT TCCTTGAAGA ATCCCACCCA  300
  GGGATCTTTG AAAACTCGTG TCTTGAAACG ATGGAAATTG TTCAACAAAC AAGAGTGGAT  360
  AAACTGACCC AAGGTCGCCA GACCTATGAC TGGACATTGA ATAGAAACCA ACCGGCTGCA  420
  ACTGCTTTGG CCAACACTAT AGAAATCTTC AGATCGAACG GTCTAACAGC CAATGAATCG  480
  GGACGGCTAA TAGATTTCCT CAAGGATGTG ATGGAATCAA TGGATAAGGA AGAAATGGAG  540
  ATAACAACAC ATTTCCAGAG AAAGAGAAGA GTGAGGGACA ACATGACCAA GAAAATGGTC  600
  ACACAAAGAA CAATAGGGAA GAAAAAACAA AGGCTGAACA AAAAGAGCTA CCTGATAAGA  660
  GCACTGACAC TGAACACAAT GACAAAAGAT GCAGAAAGAG GCAAATTGAA GAGGCGAGCA  720
  ATTGCAACAC CCGGAATGCA AATCAGAGGA TTCGTGTACT TTGTTGAAAC ACTAGCGAGG  780
  AGTATCTGTG AGAAACTTGA GCAATCTGGA CTCCCAGTCG GAGGGAATGA GAAGAAGGCT  840
  AAATTGGCAA ACGTCGTGAG GAAGATGATG ACTAACTCAC AAGATACTGA ACTCTCCTTT  900
  ACAATTACTG GAGACAATAC CAAATGGAAT GAGAATCAGA ATCCTAGGAT GTTTCTGGCA  960
  ATGATAACGT ACATCACAAG GAACCAGCCA GAATGGTTTC GGAATGTCTT AAGCATTGCC 1020
  CCTATAATGT TCTCAAACAA AATGGCGAGA TTAGGAAAAG GATACATGTT CGAAAGTAAG 1080
  AGCATGAAGT TACGAACACA AATACCAGCA GAAATGCTTG CAAACATTGA TCTCAAATAC 1140
  TTCAATGAAT TAACGAAAAA GAAAATTGAG AAAATAAGAC CTCTATTAAT AGATGGTACA 1200
  GCCTCATTGA GCCCTGGAAT GATGATGGGC ATGTTCAACA TGCTGAGTAC AGTCCTAGGA 1260
  GTCTCAATCC TGAATCTTGG ACAGAAAAGG TACACCAAAA CCACATATTG GTGGGACGGA 1320
  CTCCAATCCT CTGATGATTT CGCTCTCATC GTAAATGCAC CGAATCATGA GGGAATACAA 1380
  GCAGGAGTGG ATAGGTTTTA TAGGACTTGT AAACTAGTTG GAATCAATAT GAGCAAGAAG 1440
  AAGTCTTACA TAAATCGGAC AGGGACATTT GAATTCACGA GCTTTTTCTA CCGCTATGGA 1500
  TTTGTAGCCA ATTTCAGTAT GGAGCTGCCC AGTTTTGGAG TGTCTGGAAT TAATGAATCG 1560
  GCCGACATGA GCATTGGTGT TACAGTGATA AAGAACAATA TGATAAACAA CGACCTTGGG 1620
  CCAGCAACAG CTCAGATGGC TCTTCAGCTA TTCATCAAGG ACTACAGATA CACATACCGA 1680
  TGCCACAGAG GGGATACGCA AATCCAAACG AGGAGATCAT TCGAGCTGAA GAAGCTGTGG 1740
  GAGCAAACCC GTTCAAAGGC AGGACTGTTG GTTTCAGATG GAGGACCAAA TCTATACAAT 1800
  ATCCGAAATC TCCATATTCC TGAGGTCTGC TTAAAATGGG AATTGATGGA TGAAGATTAC 1860
  CAGGGCAGAC TGTGTAATCC TCTGAATCCG TTCGTCAGCC ATAAGGAAAT TGAATCTGTC 1920
  AACAATGCTG TAGTAATGCC AGCTCATGGC CCGGCCAAAA GCGTGGAATA TGATGCCGTT 1980
  GCAACTACAC ATTCATGGAT TCCTAAAAGG AATCGTTCCA TTCTCAATAC GAGTCAAAGG 2040
  GGAATTCTTG AGGATGAACA GATGTACCAG AAGTGCTGCA ATCTATTCGA GAAATTCTTC 2100
  CCCAGCAGTT CATATCGGAG GCCAGTTGGA ATTTCCAGCA TGGTGGAGGC CATGGTGTCT 2160
  AGGGCCCGAA TTGACGCACG AATTGATTTC GAGTCTGGAA GGATTAAGAA AGAAGAGTTT 2220
  GCTGAGATCA TGAAGATCTG TTCCACCATT GAAGAGCTCA GACGGCAAAA ATAG       2274
  PB2: virtual consensus derived from H5N1gi|19697859|AY059525|
  Influenza A virus (A/Duck/Hong Kong/2986.1/2000(H5N1)) segment 1
  polymerase (PB2) gene, partial cds.

  SEQ ID NO: 1457

  ATGGAGAGAA TAAAAGAATT AAGAGATCTA ATGTCGCAGT CTCGCACTCG CGAGATACTA   60
  ACAAAAACCA CTGTGGACCA TATGGCCATA ATCAAGAAAT ACACATCAGG AAGACAAGAG  120
  AAGAACCCTG CTCTCAGAAT GAAATGGATG ATGGCAATGA AATATCCAAT CACAGCAGAC  180
  AAGAGAATAA TAGAGATGAT TCCTGAAAGG AATGAACAAG GGCAGACGCT TTGGAGCAAG  240
  ACAAATGATG CTGGATCGGA CAGGGTGATG GTGTCTCCCC TAGCTGTAAC TTGGTGGAAT  300
  AGGAATGGGC CGACGACAAG TGCAGTCTAT TATCCAAAGG TTTACAAAAC ATACTTTGAG  360
  AAGGTTGAAA GGTTAAAACA TGGAACCTTC GGTCCCGTTC ATTTCCGAAA CCAAATTAAA  420
  ATACGCCGCC GAGTTGATAT AAATCCTGGC CATGCAGATC TCAATGCTAA AGAAGCACAA  480
  GATGTCATCA TGGAGGTCGT TTTCCCAAAT GAAGTGGGAG CTAGAATATT GACATCAGAG  540
  TCGCAATTGA CAATAACGAA AGAAAAGAAA GAAGAGCTCC AGGATTGTAA GATTGCTCCT  600
  TTAATGGTTG CATACATGTT GGAAAGGGAA CTGGTCCGCA AAACCAGATT CCTACCGGTA  660
  GCAGGCGGAA CAAGCAGTGT GTACATTGAG GTATTGCATT TGACTCAAGG GACCTGCTGG  720
  GAACAGATGT ACACTCCAGG CGGAGAAGTG AGAAATGACG ATGTTATCCA GAGTATGATC  780
  ATCGCTGCCA GAAACATTGT TAGGAGAGCA ACGGTATCAG CGGATCCACT GGCATCACTG  840
  CTGGAGATGT GTCACAGCAC ACAAATTGGT GGGATAAGGA TGGTGGACAT CCTTAGGCAA  900
  AATCCAACTG AGGAACAAGC TGTGGATATA TGCAAAGCAG CAATGGGTTT GAGGATCAGT  960
  TCATCCTTTA GCTTTGGAGG CTTCACTTTC AAAAGAACAA GTGGAACATC CGTCAAGAAG 1020
  GAAGAGGAAG TGCTTACAGG CAACCTCCAA ACATTGAAAA TAAGAGTACA TGAGGGGTAT 1080
  GAGGAATTCA CAATGGTTGG GCGGAGGGCA ACAGCTATCC TGAGGAAAGC AACTAGAAGG 1140
  CTGATTCAGT TGATAGTAAG TGGAAGAGAC GAACAATCAA TCGCTGAGGC AATCATTGTA 1200
  GCAATGGTGT TCTCACAGGA GGATTGCATG ATAAAGGCAG TCCGAGGCGA TCTGAATTTC 1260
  GTAAACAGAG CAAACCAAAG ATTAAACCCC ATGCATCAAC TCCTGAGACA TTTTCAAAAG 1320
  GATGCAAAAG TGCTATTTCA GAATTGGGGA ATTGAACCCA TTGATAATGT CATGGGGATG 1380
  ATCGGAATAT TACCTGACAT GACTCCCAGC ACAGAAATGT CACTGAGAGG AGTAAGAGTT 1440
  AGTAAAATGG GAGTGGATGA ATATTCCAGC ACTGAGAGAG TAGTTGTAAG TATTGACCGT 1500
  TTCTTAAGGG TTCGAGATCA GCGGGGGAAC GTACTCTTAT CTCCCGAAGA GGTCAGCGAA 1560
  ACACAGGGAA CAGAGAAATT GGCAATAACA TATTCATCAT CAATGATGTG GGAAATCAAC 1620
  GGTCCTGAGT CAGTGCTTGT TAACACCTAT CAATGGATCA TCAGAAACTG GGAGACTGTG 1680
  AAGATTCAAT GGTCTCAAGA CCCCACGATG CTGTACAATA AGATGGAGTT TGAACCGTTC 1740
  CAATCCTTGG TACCTAAAGC TGCCAGAGGT CAATACAGTG GATTTGTGAG AACACTATTC 1800
  CAACAAATGC GTGACGTACT GGGGACATTT GATACTGTCC AGATAATAAA GCTGCTACCA 1860
  TTTGCAGCAG CCCCACCGGA GCAGAGCAGA ATGCAGTTTT CTTCTCTAAC TGTGAATGTG 1920
  AGAGGCTCAG GAATGAGAAT ACTTGTAAGG GGCAATTCCC CTGTGTTCAA CTACAATAAG 1980
  GCAACCAAAA GGCTTACCGT TCTTGGAAAG GACGCAGGTG CATTAACAGA GGATCCAGAT 2040
  GAGGGAACAG CCGGAGTGGA ATCTGCAGTA CTGAGGGGAT TCCTAATTCT AGGCAAGGAG 2100
  GACAAAAGAT ATGGACCAGC ATTGAGCATC AATGAACTGA GCAATCTTGC GAAAGGGGAG 2160
  AAAGCTAATG TGCTGATAGG GCAAGGAGAC GTGGTGTTGG TAATGAAACG GAAACGGGAC 2220
  TCTAGCATAC TTACTGACAG CCAGACAGCG ACCAAAAGAA TTCGGATGGC CATCAATTAG 2280

• Table 1A, C, D and E list the duplex identifier, the sequences of sense and antisense strand, the agents' target genes, and the results from the above assays, where performed, for selected exemplary agents of the invention. Table 1B and H list the duplex identifier, the duplex identifier of the corresponding unmodified sequence, the sequences of sense and antisense strand, and the agents' target genes, for selected exemplary agents bearing modified nucleic acids groups, in order to stabilize these agents against degradation, in which all pyrimidine base comprising nucleotides comprised a 2′-O-methyl group in the sense strand, and all pyrimidine base comprising nucleotides in a sequence context of 5′-ca-3′ or 5′-ua-3′ comprised a 2′-O-methyl group in the antisense strand, except for those agents where the antisense strand does not comprise nucleotides in a sequence context of 5′-ca-3′ or 5′-ua-3′, in which all uridines in a sequence context of 5′-ug-3′ are 2′-O-methyl-modified nucleotides in the antisense strand (e.g. AL-DP-2295, AL-DP-2301, and AL-DP-2302). Table 2 lists concentrations at 50% maximal inhibition calculated from the dose response determinations in Cos-7 cells engineered to express influenza genes for some particularly preferred RNAi agents of the invention.

  TABLE 6
  Sequences used in analysis of Influenza A Matrix Protein (MP)

  AY180470	Influenza A virus strain A/Quail/Nanchang/12-340/2000 (H1N1)
  	matrix protein (M) gene, partial cds.
  AY633213	Influenza A virus (A/mallard/Alberta/211/98 (H1N1)) matrix
  	protein (M) gene, complete cds.
  AY664487	Influenza A virus (A/mallard/Alberta/119/98 (H1N1))
  	nonfunctional matrix protein mRNA, partial sequence.
  M55476	Influenza virus type A matrix protein (M1) gene, complete cds
  	and M2 protein (M2) gene, complete cds.
  M55479	Influenza virus type A matrix protein (M1) gene, complete cds
  	and M2 protein (M2) gene, complete cds.
  M55480	Influenza virus type A matrix protein (M1) gene, complete cds
  	and M2 protein (M2) gene, complete cds.
  M63528	Influenza A virus (A/turkey/Minnesota/166/81 (H1N1)) membrane
  	protein M1 and membrane protein M2 genes, complete cds.
  U49119	Influenza A virus matrix proteins M1 and M2 (M) gene, complete
  	cds.
  Z26859	Influenza virus type A M and M2 genes for matrix proteins
  Z26860	Influenza virus type A M and M2 genes for matrix proteins
  AY422021	Influenza A virus (A/duck/Hokkaido/95/01(H2N2)) matrix protein
  	1 (M) gene, partial cds.
  M12699	Avian Influenza A/Mallard/NY/6750/78 RNA segment 7 encoding M1
  	and M2 proteins, complete cds.
  AF213915	Influenza A virus (A/Chicken/Italy/5945/95(H3N2)) segment 7
  	matrix protein (M) gene, partial cds.
  AY180498	Influenza A virus strain A/Chicken/Nanchang/3-120/2001 (H3N2)
  	matrix protein (M) gene, partial cds.
  AY664458	Influenza A virus (A/ruddy turnstone/Delaware/142/99 (H3N2))
  	nonfunctional matrix protein mRNA, partial sequence.
  AY769614	Influenza A virus (A/turkey/Ohio/313053/04(H3N2)) matrix
  	protein gene, partial cds.
  AY779257	Influenza A virus (A/turkey/North Carolina/12344/03(H3N2))
  	matrix protein 2 (M) gene, partial cds; and matrix protein 1 (M) gene,
  	complete cds.
  AY779258	Influenza A virus (A/turkey/Minnesota/764-2/03(H3N2)) matrix
  	protein 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY862623	Influenza A virus (A/chicken/Korea/S6/03(H3N2)) matrix protein
  	(M) gene, complete cds.
  AY862624	Influenza A virus (A/duck/Korea/S7/03(H3N2)) matrix protein
  	(M) gene, complete cds.
  AY862625	Influenza A virus (A/duck/Korea/S8/03(H3N2)) matrix protein
  	(M) gene, complete cds.
  AY862626	Influenza A virus (A/duck/Korea/S9/03(H3N2)) matrix protein
  	(M) gene, complete cds.
  AY862627	Influenza A virus (A/duck/Korea/S10/03(H3N2)) matrix protein
  	(M) gene, complete cds.
  AY862628	Influenza A virus (A/dove/Korea/S11/03(H3N2)) matrix protein
  	(M) gene, complete cds.
  Z26858	Influenza virus type A M and M2 genes for matrix proteins
  AB166865	Influenza A virus (A/chicken/Yamaguchi/7/2004(H5N1)) M1 and M2
  	genes for matrix protein and membrane ion channel, complete cds.
  AB188819	Influenza A virus (A/chicken/Oita/8/2004(H5N1)) M2, M1 genes
  	for membrane ion channel 2, matrix protein 1, complete cds.
  AF509043	Influenza A virus (A/Chicken/Hong Kong/FY150/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509044	Influenza A virus (A/Pheasant/Hong Kong/FY155/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509045	Influenza A virus (A/Silky Chicken/Hong Kong/SF189/01 (H5N1))
  	M1 protein (M1) gene, complete cds.
  AF509046	Influenza A virus (A/Quail/Hong Kong/SF203/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509047	Influenza A virus (A/Pigeon/Hong Kong/SF215/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509048	Influenza A virus (A/Chicken/Hong Kong/SF219/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509049	Influenza A virus (A/Chicken/Hong Kong/715.5/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509050	Influenza A virus (A/Chicken/Hong Kong/751.1/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509051	Influenza A virus (A/Chicken/Hong Kong/822.1/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509052	Influenza A virus (A/Chicken/Hong Kong/829.2/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509053	Influenza A virus (A/Chicken/Hong Kong/830.2/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509054	Influenza A virus (A/Chicken/Hong Kong/858.3/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509055	Influenza A virus (A/Chicken/Hong Kong/866.3/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509056	Influenza A virus (A/Chicken/Hong Kong/867.1/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509057	Influenza A virus (A/Chicken/Hong Kong/879.1/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509058	Influenza A virus (A/Chicken/Hong Kong/873.3/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509059	Influenza A virus (A/Chicken/Hong Kong/876.1/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509060	Influenza A virus (A/Chicken/Hong Kong/891.1/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509061	Influenza A virus (A/Chicken/Hong Kong/893.2/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509062	Influenza A virus (A/Goose/Hong Kong/76.1/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509063	Influenza A virus (A/Goose/Hong Kong/ww100/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509064	Influenza A virus (A/Duck/Hong Kong/573.4/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509065	Influenza A virus (A/Duck/Hong Kong/646.3/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AY059506	Influenza A virus (A/Goose/Hong Kong/ww26/2000(H5N1)) segment
  	7 matrix protein (M) gene, partial cds.
  AY059507	Influenza A virus (A/Goose/Hong Kong/ww28/2000(H5N1)) segment
  	7 matrix protein (M) gene, partial cds.
  AY059508	Influenza A virus (A/Duck/Hong Kong/ww381/2000(H5N1)) segment
  	7 matrix protein (M) gene, partial cds.
  AY059509	Influenza A virus (A/Duck/Hong Kong/ww461/2000(H5N1)) segment
  	7 matrix protein (M) gene, partial cds.
  AY059510	Influenza A virus (A/Goose/Hong Kong/ww491/2000(H5N1)) segment
  	7 matrix protein (M) gene, partial cds.
  AY059511	Influenza A virus (A/Duck/Hong Kong/2986.1/2000(H5N1)) segment
  	7 matrix protein (M) gene, partial cds.
  AY059512	Influenza A virus (A/Goose/Hong Kong/3014.8/2000(H5N1))
  	segment 7 matrix protein (M) gene, partial cds.
  AY075029	Influenza A virus (A/Chicken/Hong Kong/317.5/2001(H5N1))
  	matrix protein 1 and matrix protein 2 (M) gene, complete cds.
  AY075035	Influenza A virus (A/Duck/Hong Kong/380.5/2001(H5N1)) matrix
  	protein
  1 and matrix protein 2 (M) gene, complete cds.
  AY221530	Influenza A virus (A/Chicken/HongKong/NT873.3/01-MB(H5N1))
  	matrix protein (M) gene, complete cds.
  AY221531	Influenza A virus (A/Chicken/HongKong/NT873.3/01(H5N1)) matrix
  	protein (M) gene, complete cds.
  AY221532	Influenza A virus (A/Chicken/HongKong/FY150/01-MB(H5N1))
  	matrix protein (M) gene, complete cds.
  AY221533	Influenza A virus (A/Chicken/HongKong/FY150/01(H5N1)) matrix
  	protein (M) gene, complete cds.
  AY221534	Influenza A virus (A/Pheasant/HongKong/FY155/01-MB(H5N1))
  	matrix protein (M) gene, complete cds.
  AY221535	Influenza A virus (A/Pheasant/HongKong/FY155/01(H5N1)) matrix
  	protein (M) gene, complete cds.
  AY221536	Influenza A virus (A/Chicken/HongKong/YU822.2/01-MB(H5N1))
  	matrix protein (M) gene, complete cds.
  AY221537	Influenza A virus (A/Chicken/HongKong/YU822.2/01(H5N1)) matrix
  	protein (M) gene, complete cds.
  AY221538	Influenza A virus (A/Chicken/HongKong/YU562/01(H5N1)) matrix
  	protein (M) gene, complete cds.
  AY518361	Influenza A virus (A/duck/China/E319-2/03(H5N1)) membrane ion
  	channel M2 and matrix protein M1 (M) gene, complete cds.
  AY575895	Influenza A virus (A/Gs/HK/739.2/02 (H5N1)) matrix protein (M)
  	gene, complete cds.
  AY575896	Influenza A virus (A/Eg/HK/757.3/02 (H5N1)) matrix protein (M)
  	gene, partial cds.
  AY575897	Influenza A virus (A/G.H/HK/793.1/02 (H5N1)) matrix protein
  	(M) gene, partial cds.
  AY575898	Influenza A virus (A/Dk/HK/821/02 (H5N1)) matrix protein (M)
  	gene, partial cds.
  AY575899	Influenza A virus (A/Ck/HK/31.4/02 (H5N1)) matrix protein (M)
  	gene, complete cds.
  AY575900	Influenza A virus (A/Ck/HK/61.9/02 (H5N1)) matrix protein (M)
  	gene, complete cds.
  AY575901	Influenza A virus (A/Ck/HK/YU777/02 (H5N1)) matrix protein (M)
  	gene, complete cds.
  AY575902	Influenza A virus (A/Ck/HK/96.1/02 (H5N1)) matrix protein (M)
  	gene, complete cds.
  AY575903	Influenza A virus (A/Ck/HK/409.1/02 (H5N1)) matrix protein (M)
  	gene, complete cds.
  AY575904	Influenza A virus (A/Ph/HK/sv674.15/02 (H5N1)) matrix protein
  	(M) gene, complete cds.
  AY585378	Influenza A virus (A/duck/Fujian/01/2002(H5N1)) matrix protein
  	mRNA, complete cds.
  AY585379	Influenza A virus (A/duck/Fujian/13/2002(H5N1)) matrix protein
  	mRNA, complete cds.
  AY585380	Influenza A virus (A/duck/Fujian/17/2001(H5N1)) matrix protein
  	mRNA, complete cds.
  AY585381	Influenza A virus (A/duck/Fujian/19/2000(H5N1)) matrix protein
  	mRNA, complete cds.
  AY585382	Influenza A virus (A/duck/Guangdong/01/2001(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585383	Influenza A virus (A/duck/Guangdong/07/2000(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585384	Influenza A virus (A/duck/Guangdong/12/2000(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585385	Influenza A virus (A/duck/Guangdong/22/2002(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585386	Influenza A virus (A/duck/Guangdong/40/2000(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585387	Influenza A virus (A/duck/Guangxi/07/1999(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585388	Influenza A virus (A/duck/Guangxi/22/2001(H5N1)) matrix
  	protein mRNA, partial cds.
  AY585389	Influenza A virus (A/duck/Guangxi/35/2001(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585390	Influenza A virus (A/duck/Guangxi/53/2002(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585391	Influenza A virus (A/duck/Shanghai/08/2001(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585392	Influenza A virus (A/duck/Shanghai/13/2001(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585393	Influenza A virus (A/duck/Shanghai/35/2002(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585394	Influenza A virus (A/duck/Shanghai/37/2002(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585395	Influenza A virus (A/duck/Shanghai/38/2001(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585396	Influenza A virus (A/duck/Zhejiang/11/2000(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585397	Influenza A virus (A/duck/Zhejiang/52/2000(H5N1)) matrix
  	protein mRNA, complete cds.
  AY585398	Influenza A virus (A/duck/Guangxi/50/2001(H5N1)) matrix
  	protein mRNA, complete cds.
  AY590578	Influenza A virus (A/chicken/Nakorn-Patom/Thailand/CU-
  	K2/2004(H5N1)) matrix protein M2 and matrix protein M1 (M) gene, partial
  	and complete cds.
  AY609315	Influenza A virus (A/chicken/Guangdong/174/04(H5N1)) segment
  	7, complete sequence.
  AY651374	Influenza A virus (A/Ck/Indonesia/BL/2003(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651375	Influenza A virus (A/Dk/Indonesia/MS/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651376	Influenza A virus (A/Ck/Indonesia/PA/2003(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651377	Influenza A virus (A/Ck/Indonesia/2A/2003(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651378	Influenza A virus (A/Ck/Indonesia/4/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651379	Influenza A virus (A/Ck/Indonesia/5/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651380	Influenza A virus (A/Ck/Thailand/1/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651381	Influenza A virus (A/Ck/Thailand/73/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651382	Influenza A virus (A/Ck/Thailand/9.1/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651383	Influenza A virus (A/Qa/Thailand/57/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651384	Influenza A virus (A/bird/Thailand/3.1/2004(H5N1)) membrane
  	ion channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene,
  	complete cds.
  AY651385	Influenza A virus (A/Dk/Thailand/71.1/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651386	Influenza A virus (A/Gs/Thailand/79/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651391	Influenza A virus (A/Ck/Viet Nam/33/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651392	Influenza A virus (A/Ck/Viet Nam/35/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651393	Influenza A virus (A/Ck/Viet Nam/36/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651394	Influenza A virus (A/Ck/Viet Nam/37/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651395	Influenza A virus (A/Ck/Viet Nam/38/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651396	Influenza A virus (A/Ck/Viet Nam/39/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651397	Influenza A virus (A/Ck/Viet Nam/C57/2004 (H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651398	Influenza A virus (A/Dk/Viet Nam/11/2004(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651399	Influenza A virus (A/Gf/HK/38/2002 (H5N1)) membrane ion channel
  	2 and matrix protein 1 (M) gene, partial cds.
  AY651400	Influenza A virus (A/Ck/HK/31.2/2002(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651401	Influenza A virus (A/Ck/HK/37.4/2002(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651402	Influenza A virus (A/SCk/HK/YU100/2002(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651403	Influenza A virus (A/Ck/HK/YU22/2002(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651404	Influenza A virus (A/Ck/HK/3176.3/2002(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, partial cds.
  AY651405	Influenza A virus (A/Ck/HK/3169.1/2002(H5N1)) matrix protein 1
  	and membrane ion channel 2 (M) gene, partial cds.
  AY651406	Influenza A virus (A/Ck/HK/FY157/2003(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651407	Influenza A virus (A/Ck/HK/YU324/2003(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651408	Influenza A virus (A/Ck/HK/2133.1/2003(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, partial cds.
  AY651409	Influenza A virus (A/Ck/HK/NT93/2003(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651410	Influenza A virus (A/Ck/HK/SSP141/2003(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651411	Influenza A virus (A/Ck/HK/WF157/2003(H5N1)) membrane ion
  	channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651412	Influenza A virus (A/peregrine falcon/HK/D0028/2004(H5N1))
  	membrane ion channel 2 (M) gene, partial cds; and matrix protein 1 (M)
  	gene, complete cds.
  AY651413	Influenza A virus (A/black headed gull/HK/12.1/2003(H5N1))
  	membrane ion channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651414	Influenza A virus (A/grey heron/HK/861.1/2002(H5N1)) membrane
  	ion channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651415	Influenza A virus (A/feral pigeon/HK/862.7/2002(H5N1))
  	membrane ion channel 2 and matrix protein 1 (M) gene, complete cds.
  AY651416	Influenza A virus (A/tree sparrow/HK/864/2002(H5N1)) matrix
  	protein
  1 and membrane ion channel 2 (M) gene, partial cds.
  AY651417	Influenza A virus (A/teal/China/2978.1/2002(H5N1)) membrane
  	ion channel 2 and matrix protein 1 (M) gene, partial cds.
  AY651418	Influenza A virus (A/Dk/HN/5806/2003(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651419	Influenza A virus (A/Dk/ST/4003/2003(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651420	Influenza A virus (A/Ck/ST/4231/2003(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651421	Influenza A virus (A/Dk/YN/6255/2003(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651422	Influenza A virus (A/Dk/YN/6445/2003(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651423	Influenza A virus (A/Ck/YN/374/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651424	Influenza A virus (A/Dk/HN/101/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651425	Influenza A virus (A/Dk/HN/303/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete
  	cds.
  AY651426	Influenza A virus (A/Ph/ST/44/2004(H5N1)) membrane ion channel
  	2 (M) gene, partial cds; and matrix protein 1 (M) gene, complete cds.
  AY651427	Influenza A virus (A/Ck/YN/115/2004(H5N1)) membrane ion
  	channel 2 (M) gene, partial ads; and matrix protein 1 (M) gene, complete
  	cds.
  AY653194	Influenza A virus (A/chicken/Jilin/9/2004(H5N1)) segment 7,
  	complete sequence.
  AY676045	Influenza A virus strain (A/duck/Hong Kong/821/02(H5N1))
  	membrane protein (M) gene, complete cds.
  AY676046	Influenza A virus strain (A/egret/Hong Kong/757.2/03(H5N1))
  	membrane protein (M) gene, complete cds.
  AY676047	Influenza A virus strain (A/chicken/Korea/ES/03(H5N1))
  	membrane protein (M) gene, complete cds.
  AY676048	Influenza A virus strain (A/duck/Korea/ESD1/03(H5N1)) membrane
  	protein (M) gene, complete cds.
  AY684709	Influenza A virus (A/chicken/Hubei/327/2004(H5N1)) matrix
  	protein 2 (M2) and matrix protein 1 (M1) genes, complete cds.
  AY737292	Influenza A virus (A/chicken/Guangdong/191/04(H5N1)) segment
  	7, complete sequence.
  AY737298	Influenza A virus (A/chicken/Guangdong/178/04(H5N1)) segment
  	7, complete sequence.
  AY737306	Influenza A virus (A/duck/Guangdong/173/04(H5N1)) segment 7,
  	complete sequence.
  AY770077	Influenza A virus (A/chicken/Hubei/489/2004(H5N1)) matrix
  	protein 2 (M2) and matrix protein 1 (M1) genes, complete cds.
  AY770998	Influenza A virus (A/chicken/Ayutthaya/Thailand/CU-
  	23/04(H5N1)) matrix protein gene, complete cds.
  AY818145	Influenza A virus (A/chicken/Vietnam/C58/04(H5N1)) matrix
  	protein M1 gene, complete cds.
  AY818146	Influenza A virus (A/quail/Vietnam/36/04(H5N1)) matrix protein
  	M1 gene, complete cds.
  AY856865	Influenza A virus (A/duck/Shandong/093/2004(H5N1)) segment 7,
  	complete sequence.
  DQ055851	Influenza A virus (A/chicken/Yunnan/K001/2004(H5N1)) matrix
  	protein M1 gene, complete cds.
  AB189048	Influenza A virus (A/chicken/Kyoto/3/2004(H5N1)) M2, M1 genes
  	for membrane ion channel; M2, matrix protein 1, complete cds,.
  AB189056	Influenza A virus (A/crow/Kyoto/53/2004(H5N1)) M2, M1 genes
  	for membrane ion channel; M2, matrix protein 1, complete cds,.
  AB189064	Influenza A virus (A/crow/Osaka/102/2004(H5N1)) M2, M1 genes
  	for membrane ion channel; M2, matrix protein 1, complete cds,.
  AF046082	Influenza A virus (A/Chicken/Hong Kong/220/97 (H5N1)) matrix
  	protein 2 (M2) and matrix protein 1 (M1) genes, complete cds.
  AF098560	Influenza A virus (A/Chicken/Hong Kong/258/97 (H5N1)) M1
  	matrix protein (M) and M2 matrix protein (M) genes, partial cds.
  AF098561	Influenza A virus (A/Chicken/Hong Kong/y388/97 (H5N1)) M1
  	matrix protein (M) and M2 matrix protein (M) genes, partial cds.
  AF098562	Influenza A virus (A/Chicken/Hong Kong/728/97 (H5N1)) M1
  	matrix protein (M) and M2 matrix protein (M) genes, partial cds.
  AF098563	Influenza A virus (A/Chicken/Hong Kong/786/97 (H5N1)) M1
  	matrix protein (M) and M2 matrix protein (M) genes, partial cds.
  AF098564	Influenza A virus (A/Chicken/Hong Kong/915/97 (H5N1)) M1
  	matrix protein (M) and M2 matrix protein (M) genes, partial cds.
  AF098566	Influenza A virus (A/Duck/Hong Kong/p46/97 (H5N1)) M1 matrix
  	protein (M) and M2 matrix protein (M) genes, partial cds.
  AF098567	Influenza A virus (A/Duck/Hong Kong/y283/97 (H5N1)) M1 matrix
  	protein (M) and M2 matrix protein (M) genes, partial cds.
  AF098568	Influenza A virus (A/Goose/Hong Kong/w355/97 (H5N1)) M1 matrix
  	protein (M) and M2 matrix protein (M) genes, partial cds.
  AF144306	Influenza A virus (A/Goose/Guangdong/1/96(H5N1)) matrix
  	proteins M1 and M2 (M) gene, alternatively spliced products, complete cds.
  AF216711	Influenza A virus (A/Environment/Hong Kong/437-4/99 (H5N1))
  	matrix protein 1 and matrix protein 2 genes, complete cds.
  AF216719	Influenza A virus (A/Environment/Hong Kong/437-6/99 (H5N1))
  	matrix protein 1 and matrix protein genes, complete cds.
  AF216727	Influenza A virus (A/Environment/Hong Kong/437-8/99 (H5N1))
  	matrix protein 1 and matrix protein 2 genes, complete cds.
  AF216735	Influenza A virus (A/Environment/Hong Kong/437-10/99 (H5N1))
  	matrix protein 1 and matrix protein 2 genes, complete cds.
  AF359560	Influenza A virus (A/Goose/Guangdong/3/97(H5N1)) matrix
  	protein
  1 and matrix protein 2 (M) gene, complete cds.
  AF398429	Influenza A virus (A/Goose/Hong Kong/385.3/2000(H5N1)) matrix
  	protein 1 (M) gene, partial cds.
  AF398430	Influenza A virus (A/Goose/Hong Kong/385.5/2000(H5N1)) matrix
  	protein 1 (M) gene, partial cds.
  AF468843	Influenza A virus (A/Duak/Anyang/AVL-1/2001(H5N1)) matrix
  	protein
  1 and matrix protein 2 genes, complete cds.
  AF509040	Influenza A virus (A/Chicken/Hong Kong/FY77/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509041	Influenza A virus (A/Chicken/Hong Kong/YU562/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF509042	Influenza A virus (A/Chicken/Hong Kong/YU563/01 (H5N1)) M1
  	protein (M1) gene, complete cds.
  AF073180	Influenza A virus (A/Chicken/New Jersey/15086-3/94 (H7N3NSA))
  	matrix protein 1 (M1) and matrix protein 2 (M2) genes, complete cds.
  AF073197	Influenza A virus (A/Turkey/Oregon/71 (H7N3NSB)) matrix
  	protein 1 (M1) and matrix protein 2 (M2) genes, complete cds.
  AY664433	Influenza A Virus (A/ruddy turnstone/New Jersey/65/85(H7N3))
  	nonfunctional matrix protein mRNA, partial sequence.
  AY677732	Influenza A virus (A/chicken/British Columbia/CN7-3/04 (H7N3))
  	matrix protein 1 (M1) gene, complete cds.
  AF073198	Influenza A virus (A/Turkey/Colorado/13356/91 (H7N3NSA))
  	matrix protein 1 (M1) and matrix protein 2 (M2) genes, complete cds.
  AF073200	Influenza A virus (A/Quail/Arkansas/16309-7/94(H7N3NSA))
  	matrix protein 1 (M1) and matrix protein 2 (M2) genes, complete cds.
  AF073201	Influenza A virus (A/Turkey/Utah/24721-10/95 (H7N3NSA)) matrix
  	protein 1 (M1) and matrix protein 2 (M2) genes, complete cds.
  AJ627492	Influenza A virus (A/turkey/Italy/214845/2002(H7N3)) gene for
  	membrane protein 1 and gene for membrane protein 2, genomic RNA.
  AJ627497	Influenza A virus (A/turkey/Italy/220158/2002(H7N3)) gene for
  	membrane protein 1 and gene for membrane protein 2, genomic RNA.
  AY241600	Influenza A virus (A/Chicken/New York/12273-11/99(H7N3))
  	matrix protein 1 and matrix protein 2 genes, complete cds.
  AY241602	Influenza A virus (A/chicken/NY/14714-9/99(H7N3)) matrix
  	protein
  1 and matrix protein 2 genes, complete cds.
  AY241615	Influenza A virus (A/Duck/NJ/117228-7/01(H7N3)) matrix protein
  	1 and matrix protein 2 genes, complete cds.
  AY241616	Influenza A virus (A/Duck/PA/143585/01(H7N3)) matrix protein 1
  	and matrix protein 2 genes, complete cds.
  AY300975	Influenza A virus (A/Blue-winged Teal/TX/2/01 (H7N3) membrane
  	protein (M) gene, complete cds.
  AY303652	Influenza A virus (A/chicken/Chile/176822/02(H7N3)) matrix
  	protein
  1 and matrix protein 2 genes, complete cds.
  AY303653	Influenza A virus (A/chicken/Chile/4322/02(H7N3)) matrix
  	protein
  1 and matrix protein 2 genes, complete cds.
  AY303654	Influenza A virus (A/chicken/Chile/4957/02(H7N3)) matrix
  	protein
  1 gene, complete cds; and matrix protein 2 gene, partial cds.
  AY303655	Influenza A virus (A/chicken/Chile/4968/02(H7N3)) matrix
  	protein
  1 and matrix protein 2 genes, complete cds.
  AY303656	Influenza A virus (A/chicken/Chile/4977/02(H7N3)) matrix
  	protein
  1 and matrix protein 2 genes, complete cds.
  AY303657	Influenza A virus (A/turkey/Chile/4418/02(H7N3)) matrix
  	protein
  1 gene, complete cds; and matrix protein 2 gene, partial cds.
  AY586427	Influenza A Virus (A/turkey/Italy/214845/02 (H7N3)) matrix
  	protein gene, partial cds.
  AY586428	Influenza A virus (A/turkey/Italy/220158/2002 (H7N3)) matrix
  	protein gene, partial cds.
  AY586429	Influenza A Virus (A/mallard/Italy/43/01(H7N3)) matrix protein
  	gene, partial cds.
  AY586430	Influenza A virus (A/mallard/Italy/33/01(H7N3)) matrix protein
  	gene, partial cds.
  AY611525	Influenza A virus (A/chicken/British Columbia/04(H7N3)) matrix
  	protein 2 (M) and matrix protein 1 (M) genes, complete cds.
  AY646079	Influenza A virus (A/chicken/British
  	Columbia/GSC_human_B/04(H7N3)) matrix protein 2 and matrix protein 1 (M)
  	gene, complete cds.
  AY648288	Influenza A virus (A/GSC_chicken_B/British Columbia/04(H7N3))
  	matrix protein 2 (M) and matrix protein 1 (M) genes, complete cds.
  AY650271	Influenza A virus (A/GSC_chicken/British Columbia/04(H7N3))
  	matrix protein 2 (M) and matrix protein 1 (M) genes, complete cds.
  AJ619676	Influenza A virus (A/chicken/Germany/R28/03(H7N7)) M1 gene for
  	membrane protein 1, genomic RNA.
  AY340086	Influenza A virus (A/Netherlands/124/03(H7N7)) matrix protein
  	gene, partial cds.
  AY340087	Influenza A virus (A/Netherlands/126/03(H7N7)) matrix protein
  	gene, partial cds.
  AY340088	Influenza A virus (A/Netherlands/127/03(H7N7)) matrix protein
  	gene, partial cds.
  AY340089	Influenza A virus (A/Netherlands/219/03(H7N7)) matrix protein
  	gene, complete cds.
  AY340090	Influenza A virus (A/Netherlands/33/03(H7N7)) matrix protein
  	gene, complete cds.
  AY340091	Influenza A virus (A/chicken/Netherlands/1/03(H7N7)) matrix
  	protein gene, complete cds.
  AY664468	Influenza A virus (A/ruddy turnstone/Delaware/134/99 (H7N7))
  	nonfunational matrix protein mRNA, partial sequenae.
  L37795	Influenza virus A/chicken/Brescia/1902 (H7N7) matrix protein
  	(M1) gene and transmembrane protein (M2) gene, complete cds.
  L37796	Influenza virus A/FPV/Dobson (H7N7) matrix protein (M1) gene
  	and transmembrane protein (M2) gene, complete cds.
  L37797	Influenza virus A/FPV/Weybridge (H7N7) matrix protein (M1)
  	gene and transmembrane protein (M2) gene, complete cds.
  M23917	Influenza A/chicken/FPV/Weybridge (H7N7) M1 matrix protein
  	gene, complete cds.
  M23921	Influenza A/chicken/FPV/Weybridge (H7N7) M2 matrix protein
  	gene, complete cds.
  M38299	Influenza A/FPV/Weybridge (H7N7) matrix (M) protein (seg 7)
  	gene, complete cds.
  M63523	Influenza A virus (A/chicken/Victoria/1/85 (H7N7)) membrane
  	protein M1 and membrane protein M2 genes, complete cds.
  M63526	Influenza virus type A (strain A/FPV/Dobson/27 (H7N7))
  	membrane protein M1 and membrane protein M2 genes, complete cds.
  AB049165	Influenza A virus (A/parakeet/Chiba/1/97(H9N2)) M1, M2 genes
  	for membrane ion channel, matrix protein, complete cds.
  AB049166	Influenza A virus (A/parakeet/Narita/92A/98(H9N2)) M1, M2
  	genes for membrane ion channel, matrix protein, complete cds.
  AF222671	Influenza A virus (A/Silky Chicken/Hong Kong/SF44/99(H9N2))
  	segment 7 M1 (M1) gene, partial cds.
  AF508684	Influenza A virus (A/Ostrich/South Africa/9508103/95(H9N2))
  	segment 7 matrix protein M1 (M) gene, complete cds.
  AF508685	Influenza A virus (A/Chicken/Pakistan/4/99(H9N2)) segment 7
  	matrix protein M1 (M) gene, partial cds.
  AF508686	Influenza A virus (A/Chicken/Pakistan/5/99(H9N2)) segment 7
  	matrix protein M1 (M) gene, partial cds.
  AF508687	Influenza A virus (A/Chicken/Germany/R45/98 (H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508688	Influenza A virus (A/Duck/Germany/113/95(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508689	Influenza A virus (A/Chicken/Iran/11T/99(H9N2)) segment 7
  	matrix protein M1 (M) gene, partial cds.
  AF508690	Influenza A virus (A/Chicken/Saudi Arabia/532/99(H9N2))
  	segment 7 matrix protein M1 (M) gene, partial cds.
  AF508691	Influenza A virus (A/Pheasant/Ireland/PV18/97(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508692	Influenza A virus (A/Chicken/Korea/99029/99(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508693	Influenza A virus (A/Chicken/Beijing/8/98(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508694	Influenza A virus (A/Chicken/Guangdong/10/00(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508695	Influenza A virus (A/Chicken/Guangdong/11/97(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508696	Influenza A virus (A/Chicken/Heilongjiang/10/97(H9N2)) segment
  	7 matrix protein M1 (M) gene, complete cds.
  AF508697	Influenza A virus (A/Chicken/Henan/62/00(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508698	Influenza A virus (A/Chicken/Ningxia/5/99(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508699	Influenza A virus (A/Chicken/Sichuan/5/97(H9N2)) segment 7
  	matrix protein M1 (M) gene, partial cds.
  AF508700	Influenza A virus (A/Chicken/Shandong/6/96(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508701	Influenza A virus (A/Chicken/Shijiazhuang/2/99(H9N2)) segment
  	7 matrix protein M1 (M) gene, partial cds.
  AF508702	Influenza A virus (A/Chicken/Shenzhen/9/97(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF508703	Influenza A virus (A/Duck/Nanjing/1/97(H9N2)) segment 7 matrix
  	protein M1 (M) gene, complete cds.
  AF508704	Influenza A virus (A/Quail/Shanghai/8/96(H9N2)) segment 7
  	matrix protein M1 (M) gene, complete cds.
  AF523482	Influenza A virus (A/Duck/Shantou/1043/00(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523483	Influenza A virus (A/Duck/Shantou/2134/00(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523484	Influenza A virus (A/Wild Duck/Shantou/4808/01(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523485	Influenza A virus (A/Duck/Shantou/1042/00(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523486	Influenza A virus (A/Duck/Shantou/2143/00(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523487	Influenza A virus (A/Duck/Shantou/2144/00(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523488	Influenza A virus (A/Duck/Shantou/1881/00(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523489	Influenza A virus (A/Duck/Shantou/1796/00(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523490	Influenza A virus (A/Duck/Shantou/2102/00(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523491	Influenza A virus (A/Duck/Shantou/830/00(H9N2)) matrix protein
  	(M) gene, complete cds.
  AF523492	Influenza A virus (A/Duck/Shantou/2088/01(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523493	Influenza A virus (A/Duck/Shantou/1605/01(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523494	Influenza A virus (A/Duck/Hong Kong/610/79(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523495	Influenza A virus (A/Duck/Hong Kong/552/79(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523496	Influenza A virus (A/Duck/Hong Kong/289/78(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523497	Influenza A virus (A/Duck/Hong Kong/86/76(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF523498	Influenza A virus (A/Duck/Hong Kong/366/78(H9N2)) matrix
  	protein (M) gene, partial cds.
  AF536719	Influenza A virus (A/Chicken/Beijing/1/95(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AF536720	Influenza A virus (A/Chicken/Beijing/2/97(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AF536721	Influenza A virus (A/Chicken/Beijing/3/99(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AF536722	Influenza A virus (A/Chicken/Guangdong/97(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AF536723	Influenza A virus (A/Chicken/Hebei/1/96(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AF536724	Influenza A virus (A/Chicken/Hebei/2/98(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AF536725	Influenza A virus (A/Chicken/Hebei/3/98(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AF536726	Influenza A virus (A/Chicken/Henan/98(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AF536727	Influenza A virus (A/Chicken/Liaoning/99(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AF536728	Influenza A virus (A/Chicken/Shandong/98(H9N2)) nonfunctional
  	matrix protein gene, partial sequence.
  AJ291398	Influenza A virus (A/Chicken/Pakistan/2/99 (H9N2)) M1 gene for
  	Matrix Protein 1 (exon 1) and M2 gene for Matrix Protein 2 (exons 1 and 2),
  	genomic RNA
  AJ427865	Influenza A virus (A/quail/Hong Kong/FY298/00 (H9N2)) partial
  	m gene for matrix protein, genomic RNA
  AY180461	Influenza A virus strain A/Pigeon/Nanchang/2-0461/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180462	Influenza A virus strain A/Duck/Nanchang/11-290/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180463	Influenza A virus strain A/Duck/Nanchang/11-197/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180464	Influenza A virus strain A/Duck/Nanchang/11-392/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180477	Influenza A virus strain A/Chicken/Nanchang/4-361/2001 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180485	Influenza A virus strain A/Pigeon/Nanchang/11-145/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180486	Influenza A virus strain A/Duck/Nanchang/1-0070/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180489	Influenza A virus strain A/Duck/Nanchang/10-389/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180490	Influenza A virus strain A/Chicken/Nanchang/1-0016/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180492	Influenza A virus strain A/Pigeon/Nanchang/7-058/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180495	Influenza A virus strain A/Quail/Nanchang/2-0460/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180502	Influenza A virus strain A/Chicken/Nanchang/4-010/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180504	Influenza A virus strain A/Quail/Nanchang/4-040/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180506	Influenza A virus strain A/Chicken/Nanchang/4-301/2001 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180516	Influenza A virus strain A/Duck/Nanchang/7-092/2000 (H9N2)
  	matrix protein (M) gene, partial cds.
  AY180519	Influenza A virus strain A/Wild Duck/Nanchang/2-0480/2000
  	(H9N2) matrix protein (M) gene, partial cds.
  AY253755	Influenza A virus (A/Chicken/Shanghai/F/98(H9N2)) matrix
  	protein M1 and membrane ion channel M2 genes, complete cds.
  AY496852	Influenza A virus (A/chicken/Mudanjiang/0823/2000(H9N2))
  	matrix protein (M1) mRNA, complete cds.
  AY633165	Influenza A virus (A/mallard/Alberta/17/91(H9N2)) matrix
  	protein (M) gene, complete cds.
  AY633277	Influenza A virus (A/mallard/Alberta/321/88(H9N2)) matrix
  	protein (M) gene, complete cds.
  AY633293	Influenza A virus (A/mallard/Alberta/11/91(H9N2)) matrix
  	protein (M) gene, complete cds.
  AY664464	Influenza A virus (A/shorebird/Delaware/276/99 (H9N2))
  	nonfunctional matrix protein mRNA, partial sequence.
  AY664679	Influenza A virus (A/chicken/HongKong/CSW153/03(H9N2))
  	membrane protein M2 (M) gene, partial cds; and membrane protein M1 (M)
  	gene, complete cds.
  AY664680	Influenza A virus (A/chicken/HongKong/AP45/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664681	Influenza A virus (A/chicken/HongKong/BD90/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664682	Influenza A virus (A/chicken/HongKong/CSW291/03(H9N2))
  	membrane protein M2 (M) gene, partial cds; and membrane protein M1 (M)
  	gene, complete cds.
  AY664683	Influenza A virus (A/chicken/HongKong/CSW304/03(H9N2))
  	membrane protein M2 (M) and membrane protein M1 (M) genes, partial cds.
  AY664684	Influenza A virus (A/chicken/HongKong/FY23/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664685	Influenza A virus (A/guineafowl/HongKong/NT101/03(H9N2))
  	membrane protein M2 (M) gene, partial cds; and membrane protein M1 (M)
  	gene, complete cds.
  AY664686	Influenza A virus (A/chicken/HongKong/NT142/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664687	Influenza A virus (A/chicken/HongKong/SF1/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664688	Influenza A virus (A/chicken/HongKong/SSP101/03(H9N2))
  	membrane protein M2 (M) gene, partial cds; and membrane protein M1 (M)
  	gene, complete cds.
  AY664689	Influenza A virus (A/chicken/HongKong/TP38/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664690	Influenza A virus (A/chicken/HongKong/WF126/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664691	Influenza A virus (A/pigeon/HongKong/WF53/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664692	Influenza A virus (A/pheasant/HongKong/WF54/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664693	Influenza A virus (A/guineafowl/HongKong/NT184/03(H9N2))
  	membrane protein M2 (M) gene, partial cds; and membrane protein M1 (M)
  	gene, complete cds.
  AY664694	Influenza A virus (A/chicken/HongKong/WF120/03(H9N2)) membrane
  	protein M2 (M) and membrane protein M1 (M) genes, partial cds.
  AY664695	Influenza A virus (A/chicken/HongKong/NT366/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY664696	Influenza A virus (A/chicken/HongKong/SSP418/03(H9N2))
  	membrane protein M2 (M) gene, partial cds; and membrane protein M1 (M)
  	gene, complete cds.
  AY664697	Influenza A virus (A/chicken/HongKong/YU427/03(H9N2)) membrane
  	protein M2 (M) gene, partial cds; and membrane protein M1 (M) gene,
  	complete cds.
  AY800234	Influenza A virus (A/chicken/Korea/S1/2003(H9N2)) matrix
  	protein (M) gene, complete cds.
  AY862614	Influenza A virus (A/silky chicken/Korea/S3/03(H9N2)) matrix
  	protein (M) gene, complete cds.
  AY862615	Influenza A virus (A/chicken/Korea/S4/03(H9N2)) matrix protein
  	(M) gene, complete cds.
  AY862616	Influenza A virus (A/chicken/Korea/S5/03(H9N2)) matrix protein
  	(M) gene, complete cds.
  AY862617	Influenza A virus (A/chicken/Korea/S12/03(H9N2)) matrix
  	protein (M) gene, complete cds.
  AY862618	Influenza A virus (A/duck/Korea/S13/03(H9N2)) matrix protein
  	(M) gene, complete cds.
  AY862619	Influenza A virus (A/dove/Korea/S14/03(H9N2)) matrix protein
  	(M) gene, partial cds.
  AY862620	Influenza A virus (A/chicken/Korea/S15/03(H9N2)) matrix
  	protein (M) gene, complete cds.
  AY862621	Influenza A virus (A/chicken/Korea/S16/03(H9N2)) matrix
  	protein (M) gene, complete cds.
  AY862622	Influenza A virus (A/chicken/Korea/S18/03(H9N2)) matrix
  	protein (M) gene, complete cds.
  AF156458	Influenza A virus (A/Chicken/Hong Kong/G9/97(H9N2)) segment 7
  	matrix protein M1 (M1) and matrix protein M2 (M2) genes, complete cds.
  AF156459	Influenza A virus (A/Chicken/Hong Kong/G23/97(H9N2)) segment 7
  	matrix protein M1 (M1) and matrix protein M2 (M2) genes, complete cds.
  AF156460	Influenza A virus (A/Pigeon/Hong Kong/Y233/97(H9N2)) segment 7
  	matrix protein M1 (M1) and matrix protein M2 (M2) genes, complete cds.
  AF156461	Influenza A virus (A/Duck/Hong Kong/Y280/97(H9N2)) segment 7
  	matrix protein M1 (M1) and matrix protein M2 (M2) genes, complete cds.
  AF156462	Influenza A virus (A/Duck/Hong Kong/Y439/97(H9N2)) segment 7
  	matrix protein M1 (M1) and matrix protein M2 (M2) genes, complete cds.
  AF156463	Influenza A virus (A/Quail/Hong Kong/G1/97 (H9N2)) segment 7
  	matrix protein M1 (M1) gene, complete cds; and matrix protein M2 (M2) gene,
  	partial cds.
  AF156464	Influenza A virus (A/Chicken/Hong Kong/739/94(H9N2)) segment 7
  	matrix protein M1 (M1) gene, complete cds; and matrix protein M2 (M2) gene,
  	partial cds.
  AF156465	Influenza A virus (A/Quail/Hong Kong/AF157/92(H9N2)) segment 7
  	matrix protein M1 (M1) gene, complete cds; and matrix protein M2 (M2) gene,
  	partial cds.
  AF156466	Influenza A virus (A/Chicken/Beijing/1/94(H9N2)) segment 7
  	matrix protein M1 (M1) gene, complete cds; and matrix protein M2 (M2) gene,
  	partial cds.
  AF156467	Influenza A virus (A/Chicken/Korea/38349-p96323/96(H9N2))
  	segment 7 matrix protein M1 (M1) gene, complete cds; and matrix protein M2
  	(M2) gene, partial cds.
  AF156468	Influenza A virus (A/Chicken/Korea/25232-96006/96(H9N2))
  	segment 7 matrix protein M1 (M1) gene, complete cds; and matrix protein M2
  	(M2) gene, partial cds.
  AF156469	Influenza A virus (A/Shorebird/Delaware/9/96(H9N2)) segment 7
  	matrix protein M1 (M1) gene, complete cds; and matrix protein M2 (M2) gene,
  	partial cds.
  AF156470	Influenza A virus (A/Quail/Arkansas/29209-1/93(H9N2)) segment
  	7 matrix protein M1 (M1) gene, complete cds; and matrix protein M2 (M2)
  	gene, partial cds.
  AF156471	Influenza A virus (A/Turkey/California/189/66(H9N2)) segment 7
  	matrix protein M1 (M1) gene, complete cds; and matrix protein M2 (M2) gene,
  	partial cds.
  AF203788	Influenza A virus (A/Chicken/Korea/MS96/96(H9N2)) matrix
  	protein
  1 mRNA, complete cds; and matrix protein 2 mRNA, partial cds.
  AF222662	Influenza A virus (A/Quail/Hong Kong/A17/99(H9N2)) segment 7
  	M1 (M1) gene, partial cds.
  AF222663	Influenza A virus (A/Pigeon/Hong Kong/FY6/99(H9N2)) segment 7
  	M1 (M1) gene, partial cds.
  AF222664	Influenza A virus (A/Chicken/Hong Kong/NT16/99(H9N2)) segment
  	7 M1 (M1) gene, partial cds.
  AF222665	Influenza A virus (A/Quail/Hong Kong/SSP10/99(H9N2)) segment 7
  	M1 (M1) gene, partial cds.
  AF222666	Influenza A virus (A/Pheasant/Hong Kong/SSP11/99(H9N2))
  	segment 7 M1 (M1) gene, partial cds.
  AF222667	Influenza A virus (A/Chicken/Hong Kong/FY20/99(H9N2)) segment
  	7 M1 (M1) gene, partial cds.
  AF222668	Influenza A virus (A/Chicken/Hong Kong/KC12/99(H9N2)) segment
  	7 M1 (M1) gene, partial cds.
  AF222669	Influenza A virus (A/Quail/Hong Kong/NT28/99(H9N2)) segment 7
  	M1 (M1) gene, partial cds.
  AF222670	Influenza A virus (A/Chicken/Hong Kong/SF2/99(H9N2)) segment 7
  	M1 (M1) gene, partial cds.

  Sequences used in analysis of Influenza A Nucleocapsid Protein (NP)

  AF156415	Influenza A virus (A/Turkey/California/189/66(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF523423	Influenza A virus (A/Duck/Hong Kong/86/76(H9N2)) nucleocapsid
  	protein (NP) gene, complete cds.
  AF523424	Influenza A virus (A/Duck/Hong Kong/366/78(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523421	Influenza A virus (A/Duck/Hong Kong/289/78(H9N2)) nucleocapsid
  	protein (NP) gene, complete cds.
  AF523422	Influenza A virus (A/Duck/Hong Kong/552/79(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY633279	Influenza A virus (A/mallard/Alberta/321/88(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY633295	Influenza A virus (A/mallard/Alberta/11/91(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY633167	Influenza A virus (A/mallard/Alberta/17/91(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AF156410	Influenza A virus (A/Quail/Hong Kong/AF157/92(H9N2)) segment 5
  	nucleoprotein (NP) gene, complete cds.
  AF156414	Influenza A virus (A/Quail/Arkansas/29209-1/93 (H9N2)) segment
  	5 nucleoprotein (NP) gene, partial cds.
  AF156408	Influenza A virus (A/Chicken/Hong Kong/739/94(H9N2)) segment 5
  	nucleoprotein (NP) gene, complete cds.
  AF156409	Influenza A virus (A/Chicken/Beijing/1/94(H9N2)) segment 5
  	nucleoprotein (NP) gene, complete cds.
  AF536699	Influenza A virus (A/Chicken/Beijing/1/95(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AF508596	Influenza A virus (A/Ostrich/South Africa/9508103/95(H9N2))
  	segment 5 nucleoprotein (NP) gene, partial cds.
  AF508600	Influenza A virus (A/Duck/Germany/113/95(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AB020778	Influenza A virus gene for nucleoprotein, complete cds.
  AF508613	Influenza A virus (A/Chicken/Shandong/6/96(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508617	Influenza A virus (A/Quail/Shanghai/8/96(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF536703	Influenza A virus (A/Chicken/Hebei/1/96(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AF156411	Influenza A virus (A/Chicken/Korea/38349-96323/96 (H9N2))
  	segment 5 nucleoprotein (NP) gene, complete cds.
  AF156412	Influenza A virus (A/Chicken/Korea/25232-96006/96 (H9N2))
  	segment 5 nucleoprotein (NP) gene, partial cds.
  M63779	Influenza A/FPV/Dobson/‘Dutch’/27 (H7N7) nucleoprotein mRNA,
  	complete cds.
  M63784	Influenza A/Teal/Iceland/29/80 (H7N7) nucleoprotein mRNA,
  	complete cds.
  AJ620352	Influenza A virus (A/Chicken/Germany/R28/03(H7N7)) NP gene for
  	nucleoprotein, genomic RNA.
  AY342425	Influenza A virus (A/Netherlands/219/03(H7N7)) nucleocapsid
  	protein gene, complete cds.
  AY342426	Influenza A virus (A/Netherlands/033/03(H7N7)) nucleocapsid
  	protein gene, complete cds.
  AY342427	Influenza A virus (A/chicken/Netherlands/1/03(H7N7))
  	nucleocapsid protein gene, complete cds.
  AF156413	Influenza A virus (A/Shorebird/Delaware/9/96 (H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF203787	Influenza A virus (A/Chicken/Korea/MS96/96(H9N2))
  	nucleoprotein mRNA, complete cds.
  AF156402	Influenza A virus (A/Chicken/Hong Kong/G9/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, complete cds.
  AF156403	Influenza A virus (A/Chicken/Hong Kong/G23/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, complete cds.
  AF156404	Influenza A virus (A/Pigeon/Hong Kong/Y233/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF156405	Influenza A virus (A/Duck/Hong Kong/Y280/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF156406	Influenza A virus (A/Duck/Hong Kong/Y439/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, complete cds.
  AF156407	Influenza A virus (A/Quail/Hong Kong/G1/97 (H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508612	Influenza A virus (A/Chicken/Sichuan/5/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF536702	Influenza A virus (A/Chicken/Guangdong/97(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AF536700	Influenza A virus (A/Chicken/Beijing/2/97(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AF508615	Influenza A virus (A/Chicken/Shenzhen/9/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508616	Influenza A virus (A/Duck/Nanjing/1/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AB049161	Influenza A virus (A/parakeet/Chiba/1/97(H9N2)) NP gene for
  	nucleoprotein, complete cds.
  AF508603	Influenza A virus (A/Pheasant/Ireland/PV18/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508607	Influenza A virus (A/Chicken/Guangdong/11/97(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508609	Influenza A virus (A/Chicken/Heilongjiang/10/97(H9N2)) segment
  	5 nucleoprotein (NP) gene, partial cds.
  AF508608	Influenza A virus (A/Chicken/Hebei/4/98(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508605	Influenza A virus (A/Chicken/Beijing/8/98(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508599	Influenza A virus (A/Chicken/Germany/R45/98 (H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF536708	Influenza A virus (A/Chicken/Shandong/98(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AY253753	Influenza A virus (A/Chicken/Shanghai/F/98(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AF536704	Influenza A virus (A/Chicken/Hebei/2/98(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AF536705	Influenza A virus (A/Chicken/Hebei/3/98(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AF536706	Influenza A virus (A/Chicken/Henan/98(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AB049162	Influenza A virus (A/parakeet/Narita/92A/98(H9N2)) NP gene for
  	nucleoprotein, complete cds.
  AF186270	Influenza A virus (A/Quail/Hong Kong/NT28/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF186271	Influenza A virus (A/Silkie Chicken/Hong Kong/SF43/99(H9N2))
  	segment 5 nucleoprotein (NP) gene, partial cds.
  AF186272	Influenza A virus (A/Chicken/Hong Kong/SF2/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF222614	Influenza A virus (A/Quail/Hong Kong/A17/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF222615	Influenza A virus (A/Pigeon/Hong Kong/FY6/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF222616	Influenza A virus (A/Chicken/Hong Kong/NT16/99(H9N2)) segment
  	5 nucleoprotein (NP) gene, partial cds.
  AF222617	Influenza A virus (A/Quail/Hong Kong/SSP10/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF222618	Influenza A virus (A/Pheasant/Hong Kong/SSP11/99(H9N2))
  	segment 5 nucleoprotein (NP) gene, partial cds.
  AF536707	Influenza A virus (A/Chicken/Liaoning/99(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AJ291394	Influenza A virus (A/Chicken/Pakistan/2/99 (H9N2)) NP gene for
  	Nucleoprotein, genomic RNA.
  AF536701	Influenza A virus (A/Chicken/Beijing/3/99(H9N2)) nucleoprotein
  	(NP) gene, partial cds.
  AF508611	Influenza A virus (A/Chicken/Ningxia/5/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508614	Influenza A virus (A/Chicken/Shijiazhuang/2/99(H9N2)) segment
  	5 nucleoprotein (NP) gene, partial cds.
  AF508604	Influenza A virus (A/Chicken/Korea/99029/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF222619	Influenza A virus (A/Chicken/Hong Kong/FY20/99(H9N2)) segment
  	5 nucleoprotein (NP) gene, partial cds.
  AF222620	Influenza A virus (A/Chicken/Hong Kong/KC12/99(H9N2)) segment
  	5 nucleoprotein (NP) gene, partial cds.
  AF222621	Influenza A virus (A/Silky Chicken/Hong Kong/SF44/99(H9N2))
  	segment 5 nucleoprotein (NP) gene, partial cds.
  AF508601	Influenza A virus (A/Chicken/Iran/11T/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508602	Influenza A virus (A/Chicken/Saudi Arabia/532/99(H9N2))
  	segment 5 nucleoprotein (NP) gene, partial cds.
  AF508597	Influenza A virus (A/Chicken/Pakistan/4/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508598	Influenza A virus (A/Chicken/Pakistan/5/99(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508606	Influenza A virus (A/Chicken/Guangdong/10/00(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF508610	Influenza A virus (A/Chicken/Henan/62/00(H9N2)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF523410	Influenza A virus (A/Duck/Shantou/1043/00(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523411	Influenza A virus (A/Duck/Shantou/2134/00(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523413	Influenza A virus (A/Duck/Shantou/1042/00(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523415	Influenza A virus (A/Duck/Shantou/2102/00(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523416	Influenza A virus (A/Duck/Shantou/830/00(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523417	Influenza A virus (A/Duck/Shantou/2144/00(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523419	Influenza A virus (A/Duck/Shantou/2143/00(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523420	Influenza A virus (A/Duck/Shantou/1881/00(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AJ427864	Influenza A virus (A/quail/Hong Kong/FY298/00 (H9N2)) partial
  	np gene for nucleoprotein, genomic RNA
  AY180525	Influenza A virus (A/Pigeon/Nanchang/2-0461/2000(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY180534	Influenza A virus strain A/Duck/Nanchang/7-092/2000 (H9N2)
  	nucleoprotein (NP) gene, partial cds.
  AY180537	Influenza A virus strain A/Duck/Nanchang/11-392/2000 (H9N2)
  	nucleoprotein (NP) gene, partial cds.
  AY180538	Influenza A virus (A/Pigeon/Nanchang/11-145/2000(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY180542	Influenza A virus strain A/Duck/Nanchang/11-197/2000 (H9N2)
  	nucleoprotein (NP) gene, partial cds.
  AY180544	Influenza A virus strain A/Duck/Nanchang/11-290/2000 (H9N2)
  	nucleoprotein (NP) gene, partial cds.
  AY180560	Influenza A virus (A/Pigeon/Nanchang/7-058/2000(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY180562	Influenza A virus strain A/Chicken/Nanchang/4-010/2000 (H9N2)
  	nucleoprotein (NP) gene, partial cds.
  AY180563	Influenza A virus strain A/Quail/Nanchang/4-040/2000 (H9N2)
  	nucleoprotein (NP) gene, partial cds.
  AY180564	Influenza A virus (A/Wild Duck/Nanchang/2-0480/2000(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY180575	Influenza A virus (A/Quail/Nanchang/2-0460/2000(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY496851	Influenza A virus (A/chicken/Mudanjiang/0823/2000(H9N2))
  	nucleoprotein (np) mRNA, complete cds.
  AY180581	Influenza A virus (A/Chicken/Nanchang/1-0016/2000(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY180583	Influenza A virus strain A/Duck/Nanchang/10-389/2000 (H9N2)
  	nucleoprotein (NP) gene, partial cds.
  AY180584	Influenza A virus strain A/Duck/Nanchang/1-0070/2000 (H9N2)
  	nucleoprotein (NP) gene, partial cds.
  AY768567	Influenza A virus (A/chicken/Korea/SNU0028/00(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY768568	Influenza A virus (A/chicken/Korea/SNU0037/00(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY768569	Influenza A virus (A/chicken/Korea/SNU0057/00(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY768570	Influenza A virus (A/chicken/Korea/SNU0073/00(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY768571	Influenza A virus (A/chicken/Korea/SNU0091/00(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY768572	Influenza A virus (A/chicken/Korea/SNU0140/00(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY768573	Influenza A virus (A/chicken/Korea/SNU0146/00(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY768574	Influenza A virus (A/chicken/Korea/SNU1035C/00(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY268949	Influenza A virus (A/chicken/Wangcheng/4/2001(H9N2))
  	nucleoprotein mRNA, complete cds.
  AY180578	Influenza A virus strain A/Chicken/Nanchang/4-301/2001 (H9N2)
  	nucleoprotein (NP) gene, partial cds.
  AY180551	Influenza A virus (A/Chicken/Nanchang/4-361/2001(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AF523418	Influenza A virus (A/Duck/Shantou/2088/01(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523414	Influenza A virus (A/Duck/Shantou/1605/01(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AF523412	Influenza A virus (A/Wild Duck/Shantou/4808/01(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY800236	Influenza A virus (A/chicken/Korea/S1/2003(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY862646	Influenza A virus (A/silky chicken/Korea/S3/03(H9N2))
  	nucleocapsid protein (NP) gene, partial cds.
  AY862647	Influenza A virus (A/chicken/Korea/S4/03(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862648	Influenza A virus (A/chicken/Korea/S5/03(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862649	Influenza A virus (A/chicken/Korea/S12/03(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862650	Influenza A virus (A/Duck/Korea/S13/03(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862651	Influenza A virus (A/dove/Korea/S14/03(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862652	Influenza A virus (A/chicken/Korea/S15/03(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862653	Influenza A virus (A/chicken/Korea/S16/03(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862654	Influenza A virus (A/chicken/Korea/S18/03(H9N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY664717	Influenza A virus (A/chicken/HongKong/CSW153/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664718	Influenza A virus (A/chicken/HongKong/AP45/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664719	Influenza A virus (A/chicken/HongKong/BD90/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664720	Influenza A virus (A/chicken/HongKong/CSW291/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664721	Influenza A virus (A/chicken/HongKong/CSW304/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664722	Influenza A virus (A/chicken/HongKong/FY23/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664723	Influenza A virus (A/guineafowl/HongKong/NT101/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664724	Influenza A virus (A/chicken/HongKong/NT142/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664725	Influenza A virus (A/chicken/HongKong/SF1/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664726	Influenza A virus (A/chicken/HongKong/SSP101/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664727	Influenza A virus (A/chicken/HongKong/TP38/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664728	Influenza A virus (A/chicken/HongKong/WF126/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664729	Influenza A virus (A/pigeon/HongKong/WF53/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664730	Influenza A virus (A/pheasant/HongKong/WF54/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664731	Influenza A virus (A/guineafowl/HongKong/NT184/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664732	Influenza A virus (A/chicken/HongKong/WF120/03(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY664733	Influenza A virus (A/chicken/HongKong/NT366/03(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY664734	Influenza A virus (A/chicken/HongKong/SSP418/03(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY664735	Influenza A virus (A/chicken/HongKong/YU427/03(H9N2))
  	nucleoprotein (NP) gene, partial cds.
  AY788915	Influenza A virus (A/chicken/China/HSS2004(H9N2))
  	nucleoprotein (NP) gene, complete cds.
  AY586423	Influenza A virus (A/mallard/Italy/33/01(H7N3)) nucleoprotein
  	gene, partial cds.
  AY586424	Influenza A Virus (A/mallard/Italy/43/01(H7N3)) nucleoprotein
  	gene, partial cds.
  AY586425	Influenza A virus (A/turkey/Italy/220158/2002(H7N3))
  	nucleoprotein gene, partial cds.
  AY586426	Influenza A Virus (A/turkey/Italy/214845/02(H7N3))
  	nucleoprotein gene, partial cds.
  AJ627486	Influenza A virus (A/turkey/Italy/214845/2002(H7N3)) NP gene
  	for nucleoprotein, genomic RNA.
  AJ627495	Influenza A virus (A/turkey/Italy/220158/2002(H7N3)) NP gene
  	for nucleoprotein, genomic RNA.
  AY303658	Influenza A virus (A/chicken/Chile/176822/02(H7N3))
  	nucleoprotein gene, complete cds.
  AY303659	Influenza A virus (A/chicken/Chile/4957/02(H7N3))
  	nucleoprotein gene, complete cds.
  AY611527	Influenza A virus (A/chicken/British Columbia/04(H7N3))
  	nucleoprotein (NP) gene, complete cds.
  AY646081	Influenza A virus (A/chicken/British
  	Columbia/GSC_human_B/04(H7N3)) nucleoprotein (NP) gene, complete cds.
  AY648290	Influenza A virus (A/GSC_chicken_B/British Columbia/04(H7N3))
  	nucleoprotein (NP) gene, complete cds.
  AY650273	Influenza A virus (A/GSC_chicken/British Columbia/04(H7N3))
  	nucleoprotein (NP) gene, complete cds.
  AF144303	Influenza A virus (A/Goose/Guangdong/1/96(H5N1)) nucleocapsid
  	protein (NP) gene, complete cds.
  AF046084	Influenza A virus (A/Chicken/Hong Kong/220/97 (H5N1))
  	nucleoprotein gene, complete cds.
  AF057293	Influenza A virus (A/chicken/Hong Kong/258/97(H5N1))
  	nucleoprotein mRNA, complete cds.
  AF098617	Influenza A virus (A/Chicken/Hong Kong/y388/97 (H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AF098618	Influenza A virus (A/Chicken/Hong Kong/728/97 (H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AF098619	Influenza A virus (A/Chicken/Hong Kong/786/97 (H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AF098620	Influenza A virus (A/Chicken/Hong Kong/915/97 (H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AF098621	Influenza A virus (A/Duck/Hong Kong/p46/97 (H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AF098622	Influenza A virus (A/Duck/Hong Kong/y283/97 (H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AF098623	Influenza A virus (A/Goose/Hong Kong/w355/97 (H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AF370122	Influenza A virus (A/Goose/Guangdong/3/97(H5N1)) nucleoprotein
  	gene, complete cds.
  AF216712	Influenza A virus (A/Environment/Hong Kong/437-4/99 (H5N1))
  	nucleoprotein gene, complete cds.
  AF216720	Influenza A virus (A/Environment/Hong Kong/437-6/99 (H5N1))
  	nucleoprotein gene, complete cds.
  AF216728	Influenza A virus (A/Environment/Hong Kong/437-8/99 (H5N1))
  	nucleoprotein gene, complete cds.
  AF216736	Influenza A virus (A/Environment/Hong Kong/437-10/99 (H5N1))
  	nucleoprotein gene, complete cds.
  AY585429	Influenza A virus (A/duck/Guangxi/07/1999(H5N1)) nucleoprotein
  	(NP) mRNA, complete cds.
  AY585439	Influenza A virus (A/duck/Zhejiang/11/2000(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585440	Influenza A virus (A/duck/Zhejiang/52/2000(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585428	Influenza A virus (A/duck/Guangdong/40/2000(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585423	Influenza A virus (A/duck/Fujian/19/2000(H5N1)) nucleoprotein
  	(NP) mRNA, complete cds.
  AY585425	Influenza A virus (A/duck/Guangdong/07/2000(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585426	Influenza A virus (A/duck/Guangdong/12/2000(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY059492	Influenza A virus (A/Goose/Hong Kong/ww26/2000(H5N1)) segment
  	5 nucleocapsid protein (NP) gene, partial cds.
  AY059493	Influenza A virus (A/Goose/Hong Kong/ww28/2000(H5N1)) segment
  	5 nucleocapsid protein (NP) gene, partial cds.
  AY059494	Influenza A virus (A/Duck/Hong Kong/ww381/2000(H5N1)) segment
  	5 nucleocapsid protein (NP) gene, partial cds.
  AY059495	Influenza A virus (A/Duck/Hong Kong/ww461/2000(H5N1)) segment
  	5 nucleocapsid protein (NP) gene, partial cds.
  AY059496	Influenza A virus (A/Goose/Hong Kong/ww491/2000(H5N1)) segment
  	5 nucleocapsid protein (NP) gene, partial cds.
  AY059497	Influenza A virus (A/Duck/Hong Kong/2986.1/2000(H5N1)) segment
  	5 nucleocapsid protein (NP) gene, partial cds.
  AY059498	Influenza A virus (A/Goose/Hong Kong/3014.8/2000(H5N1))
  	segment 5 nucleocapsid protein (NP) gene, partial cds.
  AF398419	Influenza A virus (A/Goose/Hong Kong/385.3/2000(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF398420	Influenza A virus (A/Goose/Hong Kong/385.5/2000(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF468842	Influenza A virus (A/Duck/Anyang/AVL-1/2001(H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AF509117	Influenza A virus (A/Chicken/Hong Kong/FY77/01 (H5N1))
  	nucleocapsid protein (NP) gene, complete cds.
  AF509118	Influenza A virus (A/Chicken/Hong Kong/YU562/01 (H5N1))
  	nucleocapsid protein (NP) gene, complete cds.
  AF509119	Influenza A virus (A/Chicken/Hong Kong/YU563/01 (H5N1))
  	nucleocapsid protein (NP) gene, complete cds.
  AY585438	Influenza A virus (A/duck/Shanghai/38/2001(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY221548	Influenza A virus (A/Chicken/HongKong/NT873.3/01-MB(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY221549	Influenza A virus (A/Chicken/HongKong/NT873.3/01(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY221550	Influenza A virus (A/Chicken/HongKong/FY150/01-MB(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY221551	Influenza A virus (A/Chicken/HongKong/FY150/01(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY221552	Influenza A virus (A/Pheasant/HongKong/FY155/01-MB(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY221553	Influenza A virus (A/Pheasant/HongKong/FY155/01(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY221554	Influenza A virus (A/Chicken/HongKong/YU822.2/01-MB(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY221555	Influenza A virus (A/Chicken/HongKong/YU822.2/01(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY221556	Influenza A virus (A/Chicken/HongKong/YU562/01(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509120	Influenza A virus (A/Chicken/Hong Kong/FY150/01 (H5N1))
  	nucleocapsid protein (NP) gene, complete cds.
  AF509121	Influenza A virus (A/Pheasant/Hong Kong/FY155/01 (H5N1))
  	nucleocapsid protein (NP) gene, complete cds.
  AF509122	Influenza A virus (A/Silky Chicken/Hong Kong/SF189/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509123	Influenza A virus (A/Quail/Hong Kong/SF203/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509124	Influenza A virus (A/Pigeon/Hong Kong/SF215/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509125	Influenza A virus (A/Chicken/Hong Kong/SF219/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509126	Influenza A virus (A/Chicken/Hong Kong/715.5/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509127	Influenza A virus (A/Chicken/Hong Kong/751.1/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509128	Influenza A virus (A/Chicken/Hong Kong/822.1/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509129	Influenza A virus (A/Chicken/Hong Kong/829.2/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509130	Influenza A virus (A/Chicken/Hong Kong/830.2/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509131	Influenza A virus (A/Chicken/Hong Kong/858.3/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509132	Influenza A virus (A/Chicken/Hong Kong/866.3/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509133	Influenza A virus (A/Chicken/Hong Kong/867.1/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509134	Influenza A virus (A/Chicken/Hong Kong/879.1/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509135	Influenza A virus (A/Chicken/Hong Kong/873.3/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509136	Influenza A virus (A/Chicken/Hong Kong/876.1/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509137	Influenza A virus (A/Chicken/Hong Kong/891.1/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509138	Influenza A virus (A/Chicken/Hong Kong/893.2/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509139	Influenza A virus (A/Goose/Hong Kong/76.1/01 (H5N1))
  	nucleocapsid protein (NP) gene, complete cds.
  AF509140	Influenza A virus (A/Goose/Hong Kong/ww100/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509141	Influenza A virus (A/Duck/Hong Kong/573.4/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AF509142	Influenza A virus (A/Duck/Hong Kong/646.3/01 (H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY585424	Influenza A virus (A/duck/Guangdong/01/2001(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585422	Influenza A virus (A/duck/Fujian/17/2001(H5N1)) nucleoprotein
  	(NP) mRNA, complete cds.
  AY585430	Influenza A virus (A/duck/Guangxi/22/2001(H5N1)) nucleoprotein
  	(NP) mRNA, complete cds.
  AY585431	Influenza A virus (A/duck/Guangxi/35/2001(H5N1)) nucleoprotein
  	(NP) mRNA, complete cds.
  AY585432	Influenza A virus (A/duck/Guangxi/50/2001(H5N1)) nucleoprotein
  	(NP) mRNA, complete cds.
  AY585434	Influenza A virus (A/duck/Shanghai/08/2001(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585435	Influenza A virus (A/duck/Shanghai/13/2001(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585436	Influenza A virus (A/duck/Shanghai/35/2002(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585437	Influenza A virus (A/duck/Shanghai/37/2002(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585433	Influenza A virus (A/duck/Guangxi/53/2002(H5N1)) nucleoprotein
  	(NP) mRNA, complete cds.
  AY585427	Influenza A virus (A/duck/Guangdong/22/2002(H5N1))
  	nucleoprotein (NP) mRNA, complete cds.
  AY585420	Influenza A virus (A/duck/Fujian/01/2002(H5N1)) nucleoprotein
  	(NP) mRNA, complete cds.
  AY585421	Influenza A virus (A/duck/Fujian/13/2002(H5N1)) nucleoprotein
  	(NP) mRNA, complete cds.
  AY575907	Influenza A virus (A/Gs/HK/739.2/02 (H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY575908	Influenza A virus (A/Eg/HK/757.3/02 (H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY575909	Influenza A virus (A/G.H/HK/793.1/02 (H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY575910	Influenza A virus (A/Dk/HK/821/02 (H5N1)) nucleocapsid protein
  	(NP) gene, partial cds.
  AY575911	Influenza A virus (A/Ck/HK/31.4/02 (H5N1)) nucleocapsid
  	protein (NP) gene, complete cds.
  AY575912	Influenza A virus (A/Ck/HK/61.9/02 (H5N1)) nucleocapsid
  	protein (NP) gene, complete cds.
  AY575913	Influenza A virus (A/Ck/HK/YU777/02 (H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY575914	Influenza A virus (A/Ck/HK/96.1/02 (H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY575915	Influenza A virus (A/Ck/HK/409.1/02 (H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY575916	Influenza A virus (A/Ph/HK/sv674.15/02 (H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  DQ023146	Influenza A virus (A/chicken/sd/1/02(H5N1)) nucleoprotein (NP)
  	mRNA, complete cds.
  AY676037	Influenza A virus (A/duck/Hong Kong/821/02(H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AY651510	Influenza A virus (A/Gf/HK/38/2002(H5N1)) nucleocapsid protein
  	(NP) gene, complete cds.
  AY651511	Influenza A virus (A/Ck/HK/31.2/2002(H5N1)) nucleocapsid
  	protein (NP) gene, complete cds.
  AY651512	Influenza A virus (A/Ck/HK/37.4/2002(H5N1)) nucleocapsid
  	protein (NP) gene, complete cds.
  AY651513	Influenza A virus (A/SCk/HK/YU100/2002(H5N1)) nucleocapsid
  	protein (NP) gene, complete cds.
  AY651514	Influenza A virus (A/Ck/HK/YU22/2002(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651521	Influenza A virus (A/Ck/HK/3176.3/2002(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651522	Influenza A virus (A/Ck/HK/3169.1/2002(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651524	Influenza A virus (A/feral pigeon/HK/862.7/2002(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY651525	Influenza A virus (A/tree sparrow/HK/864/2002(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY651526	Influenza A virus (A/grey heron/HK/861.1/2002(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY651527	Influenza A virus (A/teal/China/2978.1/2002(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY651523	Influenza A virus (A/black headed gull/HK/12.1/2003(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY651487	Influenza A virus (A/Ck/Indonesia/PA/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651515	Influenza A virus (A/Ck/HK/2133.1/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651516	Influenza A virus (A/Ck/HK/NT93/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651517	Influenza A virus (A/Ck/HK/SSP141/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651518	Influenza A virus (A/Ck/HK/WF157/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651519	Influenza A virus (A/Ck/HK/FY157/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651520	Influenza A virus (A/Ck/HK/YU324/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651490	Influenza A virus (A/Ck/Indonesia/2A/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY676038	Influenza A virus (A/egret/Hong Kong/757.2/03(H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AY676039	Influenza A virus (A/chicken/Korea/ES/03(H5N1)) nucleoprotein
  	(NP) gene, complete cds.
  AY676040	Influenza A virus (A/duck/Korea/ESD1/03(H5N1)) nucleoprotein
  	(NP) gene, complete cds.
  AY651529	Influenza A virus (A/Dk/HN/5806/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651532	Influenza A virus (A/Ck/ST/4231/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651534	Influenza A virus (A/Dk/ST/4003/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651535	Influenza A virus (A/Dk/YN/6255/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651536	Influenza A virus (A/Dk/YN/6445/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651485	Influenza A virus (A/Ck/Indonesia/BL/2003(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY518364	Influenza A virus (A/duck/China/E319-2/03(H5N1)) nucleocapsid
  	protein (NP) gene, complete cds.
  AY574189	Influenza A virus (A/chicken/Vietnam/HD1/2004(H5N1))
  	nucleoprotein gene, partial cds.
  AY574192	Influenza A virus (A/chicken/Vietnam/HD2/2004(H5N1))
  	nucleoprotein gene, partial cds.
  AJ867076	Influenza A virus (A/Hatay/2004/(H5N1)) NP gene for
  	nucleoprotein, genomic RNA
  AY651486	Influenza A virus (A/Dk/Indonesia/MS/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY590579	Influenza A virus (A/chicken/Nakorn-Patom/Thailand/CU-
  	K2/2004(H5N1)) nucleocapsid protein (NP) gene, complete cds.
  AY609313	Influenza A virus (A/chicken/Guangdong/174/04(H5N1)) segment
  	5, complete sequence.
  AY576929	Influenza A virus (A/chicken/Vietnam/CM/2004(H5N1)) segment 5
  	nucleoprotein gene, partial cds.
  AY576931	Influenza A virus (A/muscovy duck/Vietnam/MdGL/2004(H5N1))
  	segment 5 nucleoprotein gene, partial cds.
  AB166863	Influenza A virus (A/chicken/Yamaguchi/7/2004(H5N1)) NP gene
  	for nucleoprotein, complete cds.
  AB188817	Influenza A virus (A/chicken/Oita/8/2004(H5N1)) NP gene for
  	nucleoprotein, complete cds.
  AY651537	Influenza A virus (A/Ck/YN/374/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651538	Influenza A virus (A/Ck/YN/115/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY653196	Influenza A virus (A/chicken/Jilin/9/2004(H5N1)) segment 5,
  	complete sequence.
  AY651533	Influenza A virus (A/Ph/ST/44/2004(H5N1)) nucleocapsid protein
  	(NP) gene, partial cds.
  AY651530	Influenza A virus (A/Dk/HN/303/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651531	Influenza A virus (A/Dk/HN/101/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY684707	Influenza A virus (A/chicken/Hubei/327/2004(H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AY737290	Influenza A virus (A/chicken/Guangdong/191/04(H5N1)) segment
  	5, complete sequence.
  AY737297	Influenza A virus (A/chicken/Guangdong/178/04(H5N1)) segment
  	5, complete sequence.
  AY737305	Influenza A virus (A/duck/Guangdong/173/04(H5N1)) segment 5,
  	complete sequence.
  AY770081	Influenza A virus (A/chicken/Hubei/489/2004(H5N1))
  	nucleoprotein (NP) gene, complete cds.
  AY770996	Influenza A virus (A/chicken/Ayutthaya/Thailand/CU-
  	23/04(H5N1)) nucleoprotein gene, partial cds.
  AY818139	Influenza A virus (A/chicken/Vietnam/C58/04(H5N1))
  	nucleoprotein NP gene, complete cds.
  AY818140	Influenza A virus (A/quail/Vietnam/36/04(H5N1)) nucleoprotein
  	NP gene, complete cds.
  AY856864	Influenza A virus (A/duck/Shandong/093/2004(H5N1)) segment 5,
  	complete sequence.
  AB189046	Influenza A virus (A/chicken/Kyoto/3/2004(H5N1)) NP gene for
  	nucleoprotein, complete cds,.
  AB189054	Influenza A virus (A/crow/Kyoto/53/2004(H5N1)) NP gene for
  	nucleoprotein, complete cds,.
  AB189062	Influenza A virus (A/crow/Osaka/102/2004(H5N1)) NP gene for
  	nucleoprotein, complete cds,.
  AY651491	Influenza A virus (A/Ck/Thailand/1/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651492	Influenza A virus (A/Ck/Thailand/73/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651493	Influenza A virus (A/Ck/Thailand/9.1/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651494	Influenza A virus (A/Qa/Thailand/57/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651495	Influenza A virus (A/bird/Thailand/3.1/2004(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  AY651496	Influenza A virus (A/Dk/Thailand/71.1/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651497	Influenza A virus (A/Gs/Thailand/79/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651502	Influenza A virus (A/Ck/Viet Nam/33/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651503	Influenza A virus (A/Ck/Viet Nam/35/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651504	Influenza A virus (A/Ck/Viet Nam/36/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651505	Influenza A virus (A/Ck/Viet Nam/37/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651506	Influenza A virus (A/Ck/Viet Nam/38/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651507	Influenza A virus (A/Ck/Viet Nam/39/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651508	Influenza A virus (A/Ck/Viet Nam/C57/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651509	Influenza A virus (A/Dk/Viet Nam/11/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651488	Influenza A virus (A/Ck/Indonesia/4/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651489	Influenza A virus (A/Ck/Indonesia/5/2004(H5N1)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY651528	Influenza A virus (A/peregrine falcon/HK/D0028/2004(H5N1))
  	nucleocapsid protein (NP) gene, partial cds.
  M22573	Influenza A/duck/Hong Kong/7/75 (H3N2), nucleoprotein (seg 5),
  	RNA.
  AY180555	Influenza A virus (A/Chicken/Nanchang/3-120/2001(H3N2))
  	nucleoprotein (NP) gene, partial cds.
  AY779261	Influenza A virus (A/turkey/North Carolina/12344/03(H3N2))
  	nucleoprotein (NP) gene, partial cds.
  AY779262	Influenza A virus (A/turkey/Minnesota/764-2/03(H3N2))
  	nucleoprotein (NP) gene, partial cds.
  AY862655	Influenza A virus (A/chicken/Korea/S6/03(H3N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862656	Influenza A virus (A/duck/Korea/S7/03(H3N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862657	Influenza A virus (A/duck/Korea/S8/03(H3N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862658	Influenza A virus (A/duck/Korea/S9/03(H3N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862659	Influenza A virus (A/duck/Korea/S10/03(H3N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  AY862660	Influenza A virus (A/dove/Korea/S11/03(H3N2)) nucleocapsid
  	protein (NP) gene, partial cds.
  D00050	Influenza A virus gene for nucleoprotein, complete cds.
  M14921	Influenza A/Mallard/NY/6750/78 (H2N2) nucleoprotein (seg 5)
  	RNA, complete cds.
  AY422026	Influenza A virus (A/duck/Hokkaido/95/01(H2N2)) nucleoprotein
  	(NP) gene, partial cds.
  U49093	Influenza A virus nucleoprotein (NP) mRNA, partial cds.
  M22574	Influenza A/duck/Bavaria/2/77 (H1N1), nucleoprotein (seg 5),
  	RNA.
  M76603	Influenza A/turkey/England/647/77 (H1N1) mRNA, complete cds.
  M63783	Influenza A/Duck/Australia/749/80 (H1N1) nucleoprotein mRNA,
  	complete cds.
  M63778	Influenza A/Turkey/Minnesota/1661/81 (H1N1) nucleoprotein
  	mRNA, complete cds.
  Z26855	Influenza virus type A NP gene for nucleoprotein
  M76609	Influenza A/turkey/North Carolina/1790/88 (H1N1) mRNA,
  	complete cds.
  Z26857	Influenza virus type A NP gene for nucleoprotein
  AF213905	Influenza A virus (A/Mallard/Italy/24/95(H1N1)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AF213906	Influenza A virus (A/Chicken/Italy/24/95(H1N1)) segment 5
  	nucleoprotein (NP) gene, partial cds.
  AY633215	Influenza A virus (A/mallard/Alberta/211/98(H1N1))
  	nucleoprotein (NP) gene, complete cds.
  AY180543	Influenza A virus (A/Quail/Nanchang/12-340/2000(H1N1))
  	nucleoprotein (NP) gene, partial cds.

  Sequences used in analysis of Influenza A Polymerase Basic protein 1 (PB1)

  AY633218	Influenza A virus (A/mallard/Alberta/211/98(H1N1)) RNA-
  	directed RNA polymerase subunit P1 (PB1) gene, partial cds.
  U48284	Influenza A virus polymerase (PB1) mRNA, partial cds.
  AY180855	Influenza A virus strain A/Quail/Nanchang/12-340/2000 (H1N1)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY422038	Influenza A virus (A/duck/Hokkaido/95/01(H2N2)) polymerase
  	subunit (PB1) gene, partial cds.
  M25926	Influenza A/Mallard/New York/6750/78 (H2N2) PB1 gene, complete
  	cds.
  AY180871	Influenza A virus strain A/Chicken/Nanchang/3-120/2001 (H3N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY779265	Influenza A virus (A/turkey/North Carolina/12344/03(H3N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY779266	Influenza A virus (A/turkey/Minnesota/764-2/03(H3N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY862703	Influenza A virus (A/chicken/Korea/S6/03(H3N2)) PB1 (PB1)
  	gene, partial cds.
  AY862704	Influenza A virus (A/duck/Korea/S7/03(H3N2)) PB1 (PB1) gene,
  	partial cds.
  AY862705	Influenza A virus (A/duck/Korea/S8/03(H3N2)) PB1 (PB1) gene,
  	partial cds.
  AY862706	Influenza A virus (A/duck/Korea/S9/03(H3N2)) PB1 (PB1) gene,
  	partial cds.
  AY862707	Influenza A virus (A/duck/Korea/S10/03(H3N2)) PB1 (PB1) gene,
  	partial cds.
  AY862708	Influenza A virus (A/dove/Korea/S11/03(H3N2)) PB1 (PB1) gene,
  	partial cds.
  AF213911	Influenza A virus (A/Chicken/Italy/5945/95(H3N2)) segment 8
  	PB1 polymerase protein gene, partial cds.
  AB166860	Influenza A virus (A/chicken/Yamaguchi/7/2004(H5N1)) PB1 gene
  	for polymerase basic protein 1, complete cds.
  AB188814	Influenza A virus (A/chicken/Oita/8/2004(H5N1)) PB1 gene for
  	polymerase basic protein 1, complete cds.
  AF398423	Influenza A virus (A/Goose/Hong Kong/385.3/2000(H5N1))
  	polymerase (PB1) gene, partial cds.
  AF398424	Influenza A virus (A/Goose/Hong Kong/385.5/2000(H5N1))
  	polymerase (PB1) gene, partial cds.
  AF468839	Influenza A virus (A/Duck/Anyang/AVL-1/2001(H5N1)) polymerase
  	basic protein 1 (PB1) gene, complete cds.
  AF509169	Influenza A virus (A/Chicken/Hong Kong/FY77/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509170	Influenza A virus (A/Chicken/Hong Kong/YU562/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509171	Influenza A virus (A/Chicken/Hong Kong/YU563/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509172	Influenza A virus (A/Chicken/Hong Kong/FY150/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509173	Influenza A virus (A/Pheasant/Hong Kong/FY155/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509174	Influenza A virus (A/Silky Chicken/Hong Kong/SF189/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509175	Influenza A virus (A/Quail/Hong Kong/SF203/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509176	Influenza A virus (A/Pigeon/Hong Kong/SF215/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509177	Influenza A virus (A/Chicken/Hong Kong/SF219/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509178	Influenza A virus (A/Chicken/Hong Kong/715.5/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509179	Influenza A virus (A/Chicken/Hong Kong/751.1/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509180	Influenza A virus (A/Chicken/Hong Kong/822.1/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509181	Influenza A virus (A/Chicken/Hong Kong/829.2/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509182	Influenza A virus (A/Chicken/Hong Kong/830.2/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509183	Influenza A virus (A/Chicken/Hong Kong/858.3/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509184	Influenza A virus (A/Chicken/Hong Kong/866.3/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509185	Influenza A virus (A/Chicken/Hong Kong/867.1/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509186	Influenza A virus (A/Chicken/Hong Kong/879.1/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509187	Influenza A virus (A/Chicken/Hong Kong/873.3/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509188	Influenza A virus (A/Chicken/Hong Kong/876.1/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509189	Influenza A virus (A/Chicken/Hong Kong/891.1/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509190	Influenza A virus (A/Chicken/Hong Kong/893.2/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509191	Influenza A virus (A/Goose/Hong Kong/76.1/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509192	Influenza A virus (A/Goose/Hong Kong/ww100/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509193	Influenza A virus (A/Duck/Hong Kong/573.4/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AF509194	Influenza A virus (A/Duck/Hong Kong/646.3/01 (H5N1))
  	polymerase (PB1) gene, partial cds.
  AY035888	Influenza A virus (A/goose/Guangdong/3/97(H5N1)) polymerase
  	basic protein 1 (PB1) gene, complete cds.
  AY059513	Influenza A virus (A/Goose/Hong Kong/ww26/2000(H5N1)) segment
  	2 polymerase (PB1) gene, partial cds.
  AY059514	Influenza A virus (A/Goose/Hong Kong/ww28/2000(H5N1)) segment
  	2 polymerase (PB1) gene, partial cds.
  AY059515	Influenza A virus (A/Duck/Hong Kong/ww381/2000(H5N1)) segment
  	2 polymerase (PB1) gene, partial cds.
  AY059516	Influenza A virus (A/Duck/Hong Kong/ww461/2000(H5N1)) segment
  	2 polymerase (PB1) gene, partial cds.
  AY059517	Influenza A virus (A/Goose/Hong Kong/ww491/2000(H5N1)) segment
  	2 polymerase (PB1) gene, partial cds.
  AY059518	Influenza A virus (A/Duck/Hong Kong/2986.1/2000(H5N1)) segment
  	2 polymerase (PB1) gene, partial cds.
  AY059519	Influenza A virus (A/Goose/Hong Kong/3014.8/2000(H5N1))
  	segment 2 polymerase (PB1) gene, partial cds.
  AY221575	Influenza A virus (A/Chicken/HongKong/NT873.3/01-MB(H5N1))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY221576	Influenza A virus (A/Chicken/HongKong/NT873.3/01(H5N1))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY221577	Influenza A virus (A/Chicken/HongKong/FY150/01-MB(H5N1))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY221578	Influenza A virus (A/Chicken/HongKong/FY150/01(H5N1))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY221579	Influenza A virus (A/Pheasant/HongKong/FY155/01-MB(H5N1))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY221580	Influenza A virus (A/Pheasant/HongKong/FY155/01(H5N1))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY221581	Influenza A virus (A/Chicken/HongKong/YU822.2/01-MB(H5N1))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY221582	Influenza A virus (A/Chicken/HongKong/YU822.2/01(H5N1))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY221583	Influenza A virus (A/Chicken/HongKong/YU562/01(H5N1))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY518366	Influenza A virus (A/duck/China/E319-2/03(H5N1)) polymerase
  	subunit PB1 (PB1) gene, complete cds.
  AY576394	Influenza A virus (A/Gs/HK/739.2/02 (H5N1)) polymerase (PB1)
  	gene, partial cds.
  AY576395	Influenza A virus (A/Eg/HK/757.3/02 (H5N1)) polymerase (PB1)
  	gene, partial cds.
  AY576396	Influenza A virus (A/G.H/HK/793.1/02 (H5N1)) polymerase (PB1)
  	gene, partial cds.
  AY576397	Influenza A virus (A/Dk/HK/821/02 (H5N1)) polymerase (PB1)
  	gene, complete cds.
  AY576398	Influenza A virus (A/Ck/HK/31.4/02 (H5N1)) polymerase (PB1)
  	gene, partial cds.
  AY576399	Influenza A virus (A/Ck/HK/61.9/02 (H5N1)) polymerase (PB1)
  	gene, partial cds.
  AY576400	Influenza A virus (A/Ck/HK/YU777/02 (H5N1)) polymerase (PB1)
  	gene, partial cds.
  AY576401	Influenza A virus (A/Ck/HK/96.1/02 (H5N1)) polymerase (PB1)
  	gene, partial cds.
  AY576402	Influenza A virus (A/Ck/HK/409.1/02 (H5N1)) polymerase (PB1)
  	gene, partial cds.
  AY576403	Influenza A virus (A/Ph/HK/674.15/02 (H5N1)) polymerase (PB1)
  	gene, partial cds.
  AY585483	Influenza A virus (A/duck/Fujian/01/2002(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585484	Influenza A virus (A/duck/Fujian/13/2002(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585485	Influenza A virus (A/duck/Fujian/17/2001(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585486	Influenza A virus (A/duck/Fujian/19/2000(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585487	Influenza A virus (A/duck/Guangdong/01/2001(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585488	Influenza A virus (A/duck/Guangdong/07/2000(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585489	Influenza A virus (A/duck/Guangdong/12/2000(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585490	Influenza A virus (A/duck/Guangdong/22/2002(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585491	Influenza A virus (A/duck/Guangdong/40/2000(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585492	Influenza A virus (A/duck/Guangxi/07/1999(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585493	Influenza A virus (A/duck/Guangxi/22/2001(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585494	Influenza A virus (A/duck/Guangxi/35/2001(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585495	Influenza A virus (A/duck/Guangxi/50/2001(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585496	Influenza A virus (A/duck/Guangxi/53/2002(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585497	Influenza A virus (A/duck/Shanghai/08/2001(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585498	Influenza A virus (A/duck/Shanghai/13/2001(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585499	Influenza A virus (A/duck/Shanghai/35/2002(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585500	Influenza A virus (A/duck/Shanghai/37/2002(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585501	Influenza A virus (A/duck/Shanghai/38/2001(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585502	Influenza A virus (A/duck/Zhejiang/11/2000(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY585503	Influenza A virus (A/duck/Zhejiang/52/2000(H5N1)) polymerase
  	basic protein 1 (PB1) mRNA, complete cds.
  AY590582	Influenza A virus (A/chicken/Nakorn-Patom/Thailand/CU-
  	K2/2004(H5N1)) polymerase basic protein 1 (PBP1) gene, complete cds.
  AY609310	Influenza A virus (A/chicken/Guangdong/174/04 (H5N1)) segment
  	2, complete sequence.
  AY651651	Influenza A virus (A/Ck/Indonesia/BL/2003(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651652	Influenza A virus (A/Dk/Indonesia/MS/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651653	Influenza A virus (A/Ck/Indonesia/PA/2003(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651654	Influenza A virus (A/Ck/Indonesia/4/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651655	Influenza A virus (A/Ck/Indonesia/2A/2003(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651656	Influenza A virus (A/Ck/Indonesia/5/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651657	Influenza A virus (A/Ck/Thailand/1/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651658	Influenza A virus (A/Ck/Thailand/73/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651659	Influenza A virus (A/Ck/Thailand/9.1/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651660	Influenza A virus (A/Qa/Thailand/57/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651661	Influenza A virus (A/bird/Thailand/3.1/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651662	Influenza A virus (A/Dk/Thailand/71.1/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651663	Influenza A virus (A/Gs/Thailand/79/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651668	Influenza A virus (A/Ck/Viet Nam/33/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651669	Influenza A virus (A/Ck/Viet Nam/35/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651670	Influenza A virus (A/Ck/Viet Nam/36/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651671	Influenza A virus (A/Ck/Viet Nam/37/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651672	Influenza A virus (A/Ck/Viet Nam/38/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651673	Influenza A virus (A/Ck/Viet Nam/39/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651674	Influenza A virus (A/Ck/Viet Nam/C57/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651675	Influenza A virus (A/Dk/Viet Nam/11/2004(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651676	Influenza A virus (A/Gf/HK/38/2002(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651677	Influenza A virus (A/Ck/HK/31.2/2002(H5N1)) polymerase basic
  	subunit
  1 gene, partial cds.
  AY651678	Influenza A virus (A/Ck/HK/37.4/2002(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651679	Influenza A virus (A/SCk/HK/YU100/2002(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651680	Influenza A virus (A/Ck/HK/YU22/2002(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651681	Influenza A virus (A/Ck/HK/3176.3/2002(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651682	Influenza A virus (A/Ck/HK/3169.1/2002(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651683	Influenza A virus (A/Ck/HK/FY157/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651684	Influenza A virus (A/Ck/HK/YU324/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651685	Influenza A virus (A/Ck/HK/2133.1/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651686	Influenza A virus (A/Ck/HK/NT93/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651687	Influenza A virus (A/Ck/HK/SSP141/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651688	Influenza A virus (A/Ck/HK/WF157/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651689	Influenza A virus (A/black headed gull/HK/12.1/2003(H5N1))
  	polymerase basic subunit 1 (PB1) gene, partial cds.
  AY651690	Influenza A virus (A/feral pigeon/HK/862.7/2002(H5N1))
  	polymerase basic subunit 1 (PB1) gene, partial cds.
  AY651691	Influenza A virus (A/grey heron/HK/861.1/2002(H5N1))
  	polymerase basic subunit 1 (PB1) gene, partial cds.
  AY651692	Influenza A virus (A/tree sparrow/HK/864/2002(H5N1))
  	polymerase basic subunit 1 (PB1) gene, partial cds.
  AY651693	Influenza A virus (A/teal/China/2978.1/2002(H5N1)) polymerase
  	basic subunit 1 (PB1) gene, partial cds.
  AY651694	Influenza A virus (A/peregrine falcon/HK/D0028/2004(H5N1))
  	polymerase basic subunit 1 (PB1) gene, partial cds.
  AY651695	Influenza A virus (A/Dk/HN/5806/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651696	Influenza A virus (A/Dk/ST/4003/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651697	Influenza A virus (A/Ck/ST/4231/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651698	Influenza A virus (A/Dk/YN/6255/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651699	Influenza A virus (A/Dk/YN/6445/2003(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651700	Influenza A virus (A/Ph/ST/44/2004(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651701	Influenza A virus (A/Dk/HN/303/2004(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651702	Influenza A virus (A/Dk/HN/101/2004(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651703	Influenza A virus (A/Ck/YN/374/2004(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY651704	Influenza A virus (A/Ck/YN/115/2004(H5N1)) polymerase basic
  	subunit 1 (PB1) gene, partial cds.
  AY653199	Influenza A virus (A/chicken/Jilin/9/2004(H5N1)) segment 2,
  	complete sequence.
  AY676025	Influenza A virus strain (A/duck/Hong Kong/821/02(H5N1))
  	polymerase basic 1 (PB1) gene, complete cds.
  AY676026	Influenza A virus strain (A/egret/Hong Kong/757.2/03(H5N1))
  	polymerase basic 1 (PB1) gene, complete cds.
  AY676027	Influenza A virus strain (A/chicken/Korea/ES/03(H5N1))
  	polymerase basic 1 (PB1) gene, complete cds.
  AY676028	Influenza A virus strain (A/duck/Korea/ESD1/03(H5N1))
  	polymerase basic 1 (PB1) gene, complete cds.
  AY684704	Influenza A virus (A/chicken/Hubei/327/2004(H5N1)) polymerase
  	basic protein 1 (PB1) gene, complete cds.
  AY737287	Influenza A virus (A/chicken/Guangdong/191/04(H5N1)) segment
  	2, complete sequence.
  AY737294	Influenza A virus (A/chicken/Guangdong/178/04(H5N1)) segment
  	2, complete sequence.
  AY737302	Influenza A virus (A/duck/Guangdong/173/04(H5N1)) segment 2,
  	complete sequence.
  AY770083	Influenza A virus (A/chicken/Hubei/489/2004(H5N1))
  	nonfunctional polymerase basic protein 1 (PB1) gene, complete sequence.
  AY770994	Influenza A virus (A/chicken/Ayutthaya/Thailand/CU-
  	23/04(H5N1)) polymerase basic protein 1 gene, partial cds.
  AY818130	Influenza A virus (A/chicken/Vietnam/C58/04(H5N1)) polymerase
  	protein PB1 gene, complete cds.
  AY818131	Influenza A virus (A/quail/Vietnam/36/04(H5N1)) polymerase
  	protein PB1 gene, complete cds.
  AY856862	Influenza A virus (A/duck/Shandong/093/2004(H5N1)) segment 2,
  	complete sequence.
  AB188822	Influenza A virus (A/chicken/Kyoto/3/2004(H5N1)) PB1 gene for
  	polymerase basic protein 1, complete cds.
  AB189051	Influenza A virus (A/crow/Kyoto/53/2004(H5N1)) PB1 gene for
  	polymerase basic protein 1, complete cds,.
  AB189060	Influenza A virus (A/crow/Osaka/102/2004(H5N1)) PB1 gene for
  	polymerase basic protein 1, complete cds,.
  AF046085	Influenza A virus (A/Chicken/Hong Kong/220/97 (H5N1))
  	polymerase basic protein 1 (PB1) gene, complete cds.
  AF098590	Influenza A virus (A/Chicken/Hong Kong/258/97 (H5N1)) PB1
  	protein (PB1) gene, partial cds.
  AF098591	Influenza A virus (A/Chicken/Hong Kong/y388/97 (H5N1)) PB1
  	protein (PB1) gene, partial cds.
  AF098592	Influenza A virus (A/Chicken/Hong Kong/728/97 (H5N1)) PB1
  	protein (PB1) gene, partial cds.
  AF098593	Influenza A virus (A/Chicken/Hong Kong/786/97 (H5N1)) PB1
  	protein (PB1) gene, partial cds.
  AF098594	Influenza A virus (A/Chicken/Hong Kong/915/97 (H5N1)) PB1
  	protein (PB1) gene, partial cds.
  AF098595	Influenza A virus (A/Duck/Hong Kong/p46/97 (H5N1)) PB1 protein
  	(PB1) gene, partial cds.
  AF098596	Influenza A virus (A/Duck/Hong Kong/y283/97 (H5N1)) PB1
  	protein (PB1) gene, partial cds.
  AF098598	Influenza A virus (A/Goose/Hong Kong/w355/97 (H5N1)) PB1
  	protein (PB1) gene, partial cds.
  AF144301	Influenza A virus (A/Goose/Guangdong/1/96(H5N1)) polymerase
  	(PB1) gene, complete cds.
  AF216716	Influenza A virus (A/Environment/Hong Kong/437-4/99 (H5N1))
  	polymerase basic protein 1 gene, complete cds.
  AF216724	Influenza A virus (A/Environment/Hong Kong/437-6/99 (H5N1))
  	polymerase basic protein 1 gene, complete cds.
  AF216732	Influenza A virus (A/Environment/Hong Kong/437-8/99 (H5N1))
  	polymerase basic protein 1 gene, complete cds.
  AF216740	Influenza A virus (A/Environment/Hong Kong/437-10/99 (H5N1))
  	polymerase basic protein 1 gene, complete cds.
  AY303663	Influenza A virus (A/chicken/Chile/176822/02(H7N3)) polymerase
  	basic protein 1 gene, complete cds.
  AY303664	Influenza A virus (A/chicken/Chile/4957/02(H7N3)) polymerase
  	basic protein 1 gene, partial cds.
  AY586435	Influenza A Virus (A/turkey/Italy/214845/02(H7N3)) PB1 gene,
  	partial cds.
  AY586436	Influenza A virus (A/turkey/Italy/220158/2002(H7N3)) PB1 gene,
  	partial cds.
  AY586437	Influenza A virus (A/mallard/Italy/33/01(H7N3)) PB1 gene,
  	partial cds.
  AY586438	Influenza A Virus (A/mallard/Italy/43/01(H7N3)) PB1 gene,
  	partial cds.
  AY616765	Influenza A virus (A/chicken/British Columbia/04(H7N3)) PB1
  	polymerase subunit (PB1) gene, complete cds.
  AY646084	Influenza A virus (A/chicken/British
  	Columbia/GSC_human_B/04(H7N3)) polymerase basic protein 1 (PB1) gene,
  	complete cds.
  AY648293	Influenza A virus (A/GSC_chicken_B/British Columbia/04(H7N3))
  	PB1 polymerase subunit (PB1) gene, complete cds.
  AY653039	Influenza A virus (A/GSC_chicken/British Columbia/04(H7N3))
  	PB1 polymerase subunit (PB1) gene, complete cds.
  AJ620348	Influenza A virus (A/Chicken/Germany/R28/03(H7N7)) PB1 gene
  	for RNA polymerase, genomic RNA.
  AY340080	Influenza A virus (A/Netherlands/124/03(H7N7)) polymerase
  	(PB1) gene, partial cds.
  AY340081	Influenza A virus (A/Netherlands/126/03(H7N7)) polymerase
  	(PB1) gene, partial cds.
  AY340082	Influenza A virus (A/Netherlands/127/03(H7N7)) polymerase
  	(PB1) gene, partial cds.
  AY340083	Influenza A virus (A/Netherlands/219/03(H7N7)) polymerase
  	(PB1) gene, complete cds.
  AY340084	Influenza A virus (A/Netherlands/033/03(H7N7)) polymerase
  	(PB1) gene, complete cds.
  AY340085	Influenza A virus (A/chicken/Netherlands/1/03(H7N7))
  	polymerase (PB1) gene, complete cds.
  AB049155	Influenza A virus (A/parakeet/Chiba/1/97(H9N2)) PB1 gene for
  	polymerase basic protein 1, complete cds.
  AB049156	Influenza A virus (A/parakeet/Narita/92A/98(H9N2)) PB1 gene
  	for polymerase basic protein 1, complete cds.
  AF508618	Influenza A virus (A/Ostrich/South Africa/9508103/95(H9N2))
  	segment 2 polymerase PB1 (PB1) gene, partial cds.
  AF508619	Influenza A virus (A/Chicken/Pakistan/4/99(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508620	Influenza A virus (A/Chicken/Pakistan/5/99(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508621	Influenza A virus (A/Chicken/Germany/R45/98(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508622	Influenza A virus (A/Duck/Germany/113/95(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508623	Influenza A virus (A/Chicken/Iran/11T/99(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508624	Influenza A virus (A/Chicken/Saudi Arabia/532/99(H9N2))
  	segment 2 polymerase PB1 (PB1) gene, partial cds.
  AF508625	Influenza A virus (A/Pheasant/Ireland/PV18/97(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508626	Influenza A virus (A/Chicken/Korea/99029/99(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508627	Influenza A virus (A/Chicken/Beijing/8/98(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, complete cds.
  AF508628	Influenza A virus (A/Chicken/Guangdong/10/00(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508629	Influenza A virus (A/Chicken/Guangdong/11/97(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, complete cds.
  AF508630	Influenza A virus (A/Chicken/Hebei/4/98(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, complete cds.
  AF508631	Influenza A virus (A/Chicken/Heilongjiang/10/97(H9N2)) segment
  	2 polymerase PB1 (PB1) gene, partial cds.
  AF508632	Influenza A virus (A/Chicken/Henan/62/00(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, complete cds.
  AF508633	Influenza A virus (A/Chicken/Ningxia/5/99(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, complete cds.
  AF508634	Influenza A virus (A/Chicken/Sichuan/5/97(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508635	Influenza A virus (A/Chicken/Shandong/6/96(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, partial cds.
  AF508636	Influenza A virus (A/Chicken/Shijiazhuang/2/99(H9N2)) segment
  	2 polymerase PB1 (PB1) gene, complete cds.
  AF508637	Influenza A virus (A/Chicken/Shenzhen/9/97(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, complete cds.
  AF508638	Influenza A virus (A/Duck/Nanjing/1/97(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, complete cds.
  AF508639	Influenza A virus (A/Quail/Shanghai/8/96(H9N2)) segment 2
  	polymerase PB1 (PB1) gene, complete cds.
  AF523427	Influenza A virus (A/Duck/Shantou/830/00(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523428	Influenza A virus (A/Duck/Shantou/2102/00(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523429	Influenza A virus (A/Duck/Shantou/1043/00(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523430	Influenza A virus (A/Duck/Shantou/2134/00(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523431	Influenza A virus (A/Wild Duck/Shantou/4808/01(H9N2))
  	polymerase (PB1) gene, partial cds.
  AF523432	Influenza A virus (A/Duck/Shantou/2144/00(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523433	Influenza A virus (A/Duck/Shantou/2143/00(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523434	Influenza A virus (A/Duck/Shantou/1796/00(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523435	Influenza A virus (A/Duck/Shantou/2088/01(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523436	Influenza A virus (A/Duck/Shantou/1881/00(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523437	Influenza A virus (A/Duck/Hong Kong/366/78(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523438	Influenza A virus (A/Duck/Hong Kong/552/79(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523439	Influenza A virus (A/Duck/Hong Kong/86/76(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523440	Influenza A virus (A/Duck/Hong Kong/289/78(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523441	Influenza A virus (A/Duck/Hong Kong/610/79(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523442	Influenza A virus (A/Duck/Shantou/1605/01(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF523443	Influenza A virus (A/Duck/Shantou/1042/00(H9N2)) polymerase
  	(PB1) gene, partial cds.
  AF536659	Influenza A virus (A/Chicken/Beijing/1/95(H9N2)) PB1 gene,
  	partial cds.
  AF536660	Influenza A virus (A/Chicken/Beijing/2/97(H9N2)) PB1 gene,
  	partial cds.
  AF536661	Influenza A virus (A/Chicken/Beijing/3/99(H9N2)) PB1 gene,
  	partial cds.
  AF536662	Influenza A virus (A/Chicken/Guangdong/97(H9N2)) PB1 gene,
  	partial cds.
  AF536663	Influenza A virus (A/Chicken/Hebei/1/96(H9N2)) PB1 gene,
  	partial cds.
  AF536664	Influenza A virus (A/Chicken/Hebei/2/98(H9N2)) PB1 gene,
  	partial cds.
  AF536665	Influenza A virus (A/Chicken/Hebei/3/98(H9N2)) PB1 gene,
  	partial cds.
  AF536666	Influenza A virus (A/Chicken/Henan/98(H9N2)) PB1 gene, partial
  	cds.
  AF536667	Influenza A virus (A/Chicken/Liaoning/99(H9N2)) PB1 gene,
  	partial cds.
  AF536668	Influenza A virus (A/Chicken/Shandong/98(H9N2)) PB1 gene,
  	partial cds.
  AJ291396	Influenza A virus (A/Chicken/Pakistan/2/99 (H9N2)) PB1 gene
  	for polymerase PB1, genomic RNA.
  AJ427862	Influenza A virus (A/quail/Hong Kong/FY298/00 (H9N2)) partial
  	pb1 gene for PB1 polymerase protein, genomic RNA
  AY180840	Influenza A virus strain A/Pigeon/Nanchang/7-058/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180843	Influenza A virus strain A/Quail/Nanchang/2-0460/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180844	Influenza A virus strain A/Pigeon/Nanchang/2-0461/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180851	Influenza A virus strain A/Pigeon/Nanchang/11-145/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180852	Influenza A virus strain A/Duck/Nanchang/11-197/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180854	Influenza A virus strain A/Duck/Nanchang/11-290/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180856	Influenza A virus strain A/Duck/Nanchang/1-0070/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180866	Influenza A virus strain A/Duck/Nanchang/7-092/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180867	Influenza A virus strain A/Chicken/Nanchang/1-0016/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180873	Influenza A virus strain A/Chicken/Nanchang/4-010/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180874	Influenza A virus strain A/Chicken/Nanchang/4-301/2001 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180875	Influenza A virus strain A/Chicken/Nanchang/4-361/2001 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180892	Influenza A virus strain A/Quail/Nanchang/4-040/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180897	Influenza A virus strain A/Wild Duck/Nanchang/2-0480/2000
  	(H9N2) polymerase subunit PB1 (PB1) gene, partial cds.
  AY180900	Influenza A virus strain A/Duck/Nanchang/10-389/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY180901	Influenza A virus strain A/Duck/Nanchang/11-392/2000 (H9N2)
  	polymerase subunit PB1 (PB1) gene, partial cds.
  AY253751	Influenza A virus (A/Chicken/Shanghai/F/98(H9N2)) polymerase
  	basic protein 1 (PB1) gene, complete cds.
  AY307947	Influenza A virus (A/chicken/Beijing/1/00(H9N2)) polymerase
  	subunit (PB1) gene, partial cds.
  AY307948	Influenza A virus (A/chicken/Hebei/1/01(H9N2)) polymerase
  	subunit (PB1) gene, partial cds.
  AY633170	Influenza A virus (A/mallard/Alberta/17/91(H9N2)) RNA-directed
  	RNA polymerase subunit P1 (PB1) gene, partial cds.
  AY633282	Influenza A virus (A/mallard/Alberta/321/88(H9N2)) RNA-
  	directed RNA polymerase subunit P1 (PB1) gene, partial cds.
  AY633298	Influenza A virus (A/mallard/Alberta/11/91(H9N2)) RNA-directed
  	RNA polymerase subunit P1 (PB1) gene, partial cds.
  AY664774	Influenza A virus (A/chicken/HongKong/CSW153/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664775	Influenza A virus (A/chicken/HongKong/AP45/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664776	Influenza A virus (A/chicken/HongKong/BD90/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664777	Influenza A virus (A/chicken/HongKong/CSW291/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664778	Influenza A virus (A/chicken/HongKong/CSW304/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664779	Influenza A virus (A/chicken/HongKong/FY23/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664780	Influenza A virus (A/guineafowl/HongKong/NT101/03(H9N2)
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664781	Influenza A virus (A/chicken/HongKong/NT142/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664782	Influenza A virus (A/chicken/HongKong/SF1/03(H9N2)) polymerase
  	basic protein 1 (PB1) gene, partial cds.
  AY664783	Influenza A virus (A/chicken/HongKong/SSP101/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664784	Influenza A virus (A/chicken/HongKong/TP38/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664785	Influenza A virus (A/chicken/HongKong/WF126/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664786	Influenza A virus (A/pigeon/HongKong/WF53/03(H9N2)) polymerase
  	basic protein 1 (PB1) gene, partial cds.
  AY664787	Influenza A virus (A/pheasant/HongKong/WF54/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664788	Influenza A virus (A/guineafowl/HongKong/NT184/03(H9N2)
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664789	Influenza A virus (A/chicken/HongKong/WF120/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664790	Influenza A virus (A/chicken/HongKong/NT366/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY664791	Influenza A virus (A/chicken/HongKong/YU427/03(H9N2))
  	polymerase basic protein 1 (PB1) gene, partial cds.
  AY800239	Influenza A virus (A/chicken/Korea/S1/2003(H9N2)) polymerase
  	basic protein 1 (PB1) gene, partial cds.
  AY862694	Influenza A virus (A/silky chicken/Korea/S3/03(H9N2)) PB1
  	(PB1) gene, partial cds.
  AY862695	Influenza A virus (A/chicken/Korea/S4/03(H9N2)) PB1 (PB1)
  	gene, partial cds.
  AY862696	Influenza A virus (A/chicken/Korea/S5/03(H9N2)) PB1 (PB1)
  	gene, partial cds.
  AY862697	Influenza A virus (A/chicken/Korea/S12/03(H9N2)) PB1 (PB1)
  	gene, partial cds.
  AY862698	Influenza A virus (A/duck/Korea/S13/03(H9N2)) PB1 (PB1) gene,
  	partial cds.
  AY862699	Influenza A virus (A/dove/Korea/S14/03(H9N2)) PB1 (PB1) gene,
  	partial cds.
  AY862700	Influenza A virus (A/chicken/Korea/S15/03(H9N2)) PB1 (PB1)
  	gene, partial cds.
  AY862701	Influenza A virus (A/chicken/Korea/S16/03(H9N2)) PB1 (PB1)
  	gene, partial cds.
  AY862702	Influenza A virus (A/chicken/Korea/S18/03(H9N2)) PB1 (PB1)
  	gene, partial cds.
  AF156416	Influenza A virus (A/Chicken/Hong Kong/G9/97(H9N2)) segment 2
  	PB1 polymerase subunit (PB1) gene, partial cds.
  AF156417	Influenza A virus (A/Chicken/Hong Kong/G23/99 (H9N2)) segment
  	2 PB1 polymerase subunit (PB1) gene, partial cds.
  AF156418	Influenza A virus (A/Pigeon/Hong Kong/Y233/97(H9N2)) segment 2
  	PB1 polymerase subunit (PB1) gene, partial cds.
  AF156419	Influenza A virus (A/Duck/Hong Kong/Y280/97(H9N2)) segment 2
  	PB1 polymerase subunit (PB1) gene, partial cds.
  AF156420	Influenza A virus (A/Duck/Hong Kong/Y439/97(H9N2)) segment 2
  	PB1 polymerase subunit (PB1) gene, partial cds.
  AF156421	Influenza A virus (A/Quail/Hong Kong/G1/97 (H9N2)) segment 2
  	PB1 polymerase subunit (PB1) gene, partial cds.
  AF156422	Influenza A virus (A/Chicken/Hong Kong/739/94(H9N2)) segment 2
  	PB1 polymerase subunit (PB1) gene, partial cds.
  AF156423	Influenza A virus (A/Chicken/Beijing/1/94(H9N2)) segment 2 PB1
  	polymerase subunit (PB1) gene, partial cds.
  AF156424	Influenza A virus (A/Quail/Hong Kong/AF157/92(H9N2)) segment 2
  	PB1 polymerase subunit (PB1) gene, partial cds.
  AF156425	Influenza A virus (A/Chicken/Korea/38349-p96323/96(H9N2))
  	segment 2 PB1 polymerase subunit (PB1) gene, partial cds.
  AF156426	Influenza A virus (A/Chicken/Korea/25232-96006/96(H9N2))
  	segment 2 PB1 polymerase subunit (PB1) gene, partial cds.
  AF156427	Influenza A virus (A/Shorebird/Delaware/9/96(H9N2)) segment 2
  	PB1 polymerase subunit (PB1) gene, partial cds.
  AF156428	Influenza A virus (A/Quail/Arkansas/29209-1/93(H9N2)) segment
  	2 PB1 polymerase subunit (PB1) gene, partial cds.
  AF156429	Influenza A virus (A/Turkey/California/189/66(H9N2)) segment 2
  	PB1 polymerase subunit (PB1) gene, partial cds.
  AF222632	Influenza A virus (A/Quail/Hong Kong/A17/99(H9N2)) segment 2
  	polymerase 1 (PB1) gene, partial cds.
  AF222633	Influenza A virus (A/Pigeon/Hong Kong/FY6/99(H9N2)) segment 2
  	polymerase 1 (PB1) gene, partial cds.
  AF222634	Influenza A virus (A/Chicken/Hong Kong/NT16/99(H9N2)) segment
  	2 polymerase 1 (PB1) gene, partial cds.
  AF222635	Influenza A virus (A/Quail/Hong Kong/SSP10/99(H9N2)) segment 2
  	polymerase 1 (PB1) gene, partial cds.
  AF222636	Influenza A virus (A/Pheasant/Hong Kong/SSP11/99(H9N2))
  	segment 2 polymerase 1 (PB1) gene, partial cds.
  AF222637	Influenza A virus (A/Chicken/Hong Kong/FY20/99(H9N2)) segment
  	2 polymerase 1 (PB1) gene, partial cds.
  AF222638	Influenza A virus (A/Chicken/Hong Kong/KC12/99(H9N2)) segment
  	2 polymerase 1 (PB1) gene, partial cds.
  AF222639	Influenza A virus (A/Quail/Hong Kong/NT2899(H9N2)) segment 2
  	polymerase 1 (PB1) gene, partial cds.
  AF222640	Influenza A virus (A/Chicken/Hong Kong/SF2/99(H9N2)) segment 2
  	polymerase 1 (PB1) gene, partial cds.
  AF222641	Influenza A virus (A/Silky Chicken/Hong Kong/SF44/99(H9N2))
  	segment 2 polymerase 1 (PB1) gene, partial cds.

  Sequences used in analysis of Influenza A Polymerase Basic protein 2 (PB2)

  gi|49356919|AY633219|	Influenza A virus (A/mallard/Alberta/211/98(H1N1))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|27466107|AY180748|	Influenza A virus strain A/Quail/Nanchang/12-340/2000
  	(H1N1) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|45272173|AY422042|	Influenza A virus (A/duck/Hokkaido/95/01(H2N2))
  	polymerase subunit (PB2) gene, partial cds.
  gi|18091825|AF213910|	Influenza A virus (A/Chicken/Italy/5945/95(H3N2))
  	segment 1 PB2 polymerase protein gene, partial cds.
  gi|27466133|AY180761|	Influenza A virus strain A/Chicken/Nanchang/3-
  	120/2001 (H3N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|56160002|AY779267|	Influenza A virus (A/turkey/North
  	Carolina/12344/03(H3N2)) polymerase basic protein 2 (PB2) gene, partial
  	cds.
  gi|56160004|AY779268|	Influenza A virus (A/turkey/Minnesota/764-2/03(H3N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|58429704|AY862719|	Influenza A virus (A/chicken/Korea/S6/03(H3N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429706|AY862720|	Influenza A virus (A/duck/Korea/S7/03(H3N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429708|AY862721|	Influenza A virus (A/duck/Korea/S8/03(H3N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429710|AY862722|	Influenza A virus (A/duck/Korea/S9/03(H3N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429712|AY862723|	Influenza A virus (A/duck/Korea/S10/03(H3N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429714|AY862724|	Influenza A virus (A/dove/Korea/S11/03(H3N2)) PB2
  	(PB2) gene, partial cds.
  gi|5805276|AF144300|	Influenza A virus (A/Goose/Guangdong/1/96(H5N1))
  	polymerase (PB2) gene, complete cds.
  gi|3335416|AF046086|	Influenza A virus (A/Chicken/Hong Kong/220/97 (H5N1))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|6048841|AF098577|	Influenza A virus (A/Chicken/Hong Kong/258/97 (H5N1))
  	PB2 protein (PB2) gene, partial cds.
  gi|6048843|AF098578|	Influenza A virus (A/Chicken/Hong Kong/y388/97 (H5N1))
  	PB2 protein (PB2) gene, partial cds.
  gi|6048845|AF098579|	Influenza A virus (A/Chicken/Hong Kong/728/97 (H5N1))
  	PB2 protein (PB2) gene, partial cds.
  gi|6048847|AF098580|	Influenza A virus (A/Chicken/Hong Kong/786/97 (H5N1))
  	PB2 protein (PB2) gene, partial cds.
  gi|6048849|AF098581|	Influenza A virus (A/Chicken/Hong Kong/915/97 (H5N1))
  	PB2 protein (PB2) gene, partial cds.
  gi|6048851|AF098582|	Influenza A virus (A/Duck/Hong Kong/p46/97 (H5N1)) PB2
  	protein (PB2) gene, partial cds.
  gi|6048853|AF098583|	Influenza A virus (A/Duck/Hong Kong/y283/97 (H5N1))
  	PB2 protein (PB2) gene, partial cds.
  gi|6048855|AF098584|	Influenza A virus (A/Goose/Hong Kong/w355/97 (H5N1))
  	PB2 protein (PB2) gene, partial cds.
  gi|14860983|AY038798|	Influenza A virus (A/goose/Guangdong/3/1997(H5N1))
  	PB2 protein (PB2) gene, complete cds.
  gi|47156244|AY585513|	Influenza A virus (A/duck/Guangxi/07/1999(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|9863884|AF216717|	Influenza A virus (A/Environment/Hong Kong/437-4/99
  	(H5N1)) polymerase basic protein 2 gene, partial cds.
  gi|9863903|AF216725|	Influenza A virus (A/Environment/Hong Kong/437-6/99
  	(H5N1)) polymerase basic protein 2 gene, partial cds.
  gi|9863921|AF216733|	Influenza A virus (A/Environment/Hong Kong/437-8/99
  	(H5N1)) polymerase basic protein 2 gene, partial cds.
  gi|9863939|AF216741|	Influenza A virus (A/Environment/Hong Kong/437-10/99
  	(H5N1)) polymerase basic protein 2 gene, partial cds.
  gi|47156264|AY585523|	Influenza A virus (A/duck/Zhejiang/11/2000 (H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156266|AY585524|	Influenza A virus (A/duck/Zhejiang/52/2000 (H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156232|AY585507|	Influenza A virus (A/duck/Fujian/19/2000(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156236|AY585509|	Influenza A virus (A/duck/Guangdong/07/2000(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156238|AY585510|	Influenza A virus (A/duck/Guangdong/12/2000(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156242|AY585512|	Influenza A virus (A/duck/Guangdong/40/2000(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|19697849|AY059520|	Influenza A virus (A/Goose/Hong Kong/ww26/2000(H5N1))
  	segment 1 polymerase (PB2) gene, partial cds.
  gi|19697851|AY059521|	Influenza A virus (A/Goose/Hong Kong/ww28/2000(H5N1))
  	segment 1 polymerase (PB2) gene, partial cds.
  gi|19697853|AY059522|	Influenza A virus (A/Duck/Hong Kong/ww381/2000(H5N1))
  	segment 1 polymerase (PB2) gene, partial cds.
  gi|19697855|AY059523|	Influenza A virus (A/Duck/Hong Kong/ww461/2000(H5N1))
  	segment 1 polymerase (PB2) gene, partial cds.
  gi|19697857|AY059524|	Influenza A virus (A/Goose/Hong
  	Kong/ww491/2000(H5N1)) segment 1 polymerase (PB2) gene, partial cds.
  gi|19697859|AY059525|	Influenza A virus (A/Duck/Hong
  	Kong/2986.1/2000(H5N1)) segment 1 polymerase (PB2) gene, partial cds.
  gi|19697867|AY059529|	Influenza A virus (A/Goose/Hong
  	Kong/3014.8/2000(H5N1)) segment 1 polymerase (PB2) gene, partial cds.
  gi|18092181|AF398425|	Influenza A virus (A/Goose/Hong
  	Kong/385.3/2000(H5N1)) polymerase (PB2) gene, partial cds.
  gi|18092183|AF398426|	Influenza A virus (A/Goose/Hong
  	Kong/385.5/2000(H5N1)) polymerase (PB2) gene, partial cds.
  gi|21359665|AF468840|	Influenza A virus (A/duck/Anyang/AVL-1/2001(H5N1))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|28849606|AF509143|	Influenza A virus (A/Chicken/Hong Kong/FY77/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849608|AF509144|	Influenza A virus (A/Chicken/Hong Kong/YU562/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849610|AF509145|	Influenza A virus (A/Chicken/Hong Kong/YU563/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849612|AF509146|	Influenza A virus (A/Chicken/Hong Kong/FY150/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849614|AF509147|	Influenza A virus (A/Pheasant/Hong Kong/FY155/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849616|AF509148|	Influenza A virus (A/Silky Chicken/Hong Kong/SF189/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849618|AF509149|	Influenza A virus (A/Quail/Hong Kong/SF203/01 (H5N1)
  	polymerase (PB2) gene, partial cds.
  gi|28849620|AF509150|	Influenza A virus (A/Pigeon/Hong Kong/SF215/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849622|AF509151|	Influenza A virus (A/Chicken/Hong Kong/SF219/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849624|AF509152|	Influenza A virus (A/Chicken/Hong Kong/715.5/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849626|AF509153|	Influenza A virus (A/Chicken/Hong Kong/751.1/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849628|AF509154|	Influenza A virus (A/Chicken/Hong Kong/822.1/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849630|AF509155|	Influenza A virus (A/Chicken/Hong Kong/829.2/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849632|AF509156|	Influenza A virus (A/Chicken/Hong Kong/830.2/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849634|AF509157|	Influenza A virus (A/Chicken/Hong Kong/858.3/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849636|AF509158|	Influenza A virus (A/Chicken/Hong Kong/866.3/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849638|AF509159|	Influenza A virus (A/Chicken/Hong Kong/867.1/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849640|AF509160|	Influenza A virus (A/Chicken/Hong Kong/879.1/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849642|AF509161|	Influenza A virus (A/Chicken/Hong Kong/873.3/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849644|AF509162|	Influenza A virus (A/Chicken/Hong Kong/876.1/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849646|AF509163|	Influenza A virus (A/Chicken/Hong Kong/891.1/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849648|AF509164|	Influenza A virus (A/Chicken/Hong Kong/893.2/01
  	(H5N1)) polymerase (PB2) gene, partial cds.
  gi|28849650|AF509165|	Influenza A virus (A/Goose/Hong Kong/76.1/01 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|28849652|AF509166|	Influenza A virus (A/Goose/Hong Kong/ww100/01 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|28849654|AF509167|	Influenza A virus (A/Duck/Hong Kong/573.4/01 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|28849656|AF509168|	Influenza A virus (A/Duck/Hong Kong/646.3/01 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|28823262|AY221584|	Influenza A virus (A/Chicken/HongKong/NT873.3/01-
  	MB(H5N1)) polymerase basic protein 2 (PB2) gene, partial cds.
  gi|28823443|AY221585|	Influenza A virus
  	(A/Chicken/HongKong/NT873.3/01(H5N1)) polymerase basic protein 2 (PB2)
  	gene, partial cds.
  gi|28823612|AY221586|	Influenza A virus (A/Chicken/HongKong/FY150/01-
  	MB(H5N1)) polymerase basic protein 2 (PB2) gene, partial cds.
  gi|28823783|AY221587|	Influenza A virus (A/Chicken/HongKong/FY150/01(H5N1))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|28823961|AY221588|	Influenza A virus (A/Pheasant/HongKong/FY155/01-
  	MB(H5N1)) polymerase basic protein 2 (PB2) gene, partial cds.
  gi|28824143|AY221589|	Influenza A virus
  	(A/Pheasant/HongKong/FY155/01(H5N1)) polymerase basic protein 2 (PB2) gene,
  	partial cds.
  gi|28824334|AY221590|	Influenza A virus (A/Chicken/HongKong/YU822.2/01-
  	MB(H5N1)) polymerase basic protein 2 (PB2) gene, partial cds.
  gi|28824502|AY221591|	Influenza A virus
  	(A/Chicken/HongKong/YU822.2/01(H5N1)) polymerase basic protein 2 (PB2)
  	gene, partial cds.
  gi|28824684|AY221592|	Influenza A virus (A/Chicken/HongKong/YU562/01(H5N1))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|47156230|AY585506|	Influenza A virus (A/duck/Fujian/17/2001(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156234|AY585508|	Influenza A virus (A/duck/Guangdong/01/2001(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156246|AY585514|	Influenza A virus (A/duck/Guangxi/22/2001(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156248|AY585515|	Influenza A virus (A/duck/Guangxi/35/2001(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156250|AY585516|	Influenza A virus (A/duck/Guangxi/50/2001(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156254|AY585518|	Influenza A virus (A/duck/Shanghai/08/2001(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156256|AY585519|	Influenza A virus (A/duck/Shanghai/13/2001(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156262|AY585522|	Influenza A virus (A/duck/Shanghai/38/2001(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156258|AY585520|	Influenza A virus (A/duck/Shanghai/35/2002(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156260|AY585521|	Influenza A virus (A/duck/Shanghai/37/2002(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156252|AY585517|	Influenza A virus (A/duck/Guangxi/53/2002(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156240|AY585511|	Influenza A virus (A/duck/Guangdong/22/2002(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47834791|AY576382|	Influenza A virus (A/Gs/HK/739.2/02 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|47834793|AY576383|	Influenza A virus (A/Eg/HK/757.3/02 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|47834795|AY576384|	Influenza A virus (A/G.H/HK/793.1/02 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|47834797|AY576385|	Influenza A virus (A/Dk/HK/821/02 (H5N1)) polymerase
  	(PB2) gene, partial cds.
  gi|47834799|AY576386|	Influenza A virus (A/Ck/HK/31.4/02 (H5N1)) polymerase
  	(PB2) gene, partial cds.
  gi|47834801|AY576387|	Influenza A virus (A/Ck/HK/61.9/02 (H5N1)) polymerase
  	(PB2) gene, partial cds.
  gi|47834803|AY576388|	Influenza A virus (A/Ck/HK/YU777/02 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|47834805|AY576389|	Influenza A virus (A/Ck/HK/96.1/02 (H5N1)) polymerase
  	(PB2) gene, partial cds.
  gi|47834807|AY576390|	Influenza A virus (A/Ck/HK/409.1/02 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|47834809|AY576391|	Influenza A virus (A/Ph/HK/sv674.15/02 (H5N1))
  	polymerase (PB2) gene, partial cds.
  gi|47156226|AY585504|	Influenza A virus (A/duck/Fujian/01/2002(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|47156228|AY585505|	Influenza A virus (A/duck/Fujian/13/2002(H5N1))
  	polymerase basic protein 2 (PB2) mRNA, complete cds.
  gi|50296597|AY651744|	Influenza A virus (A/grey heron/HK/861.1/2002(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296599|AY651745|	Influenza A virus (A/feral
  	pigeon/HK/862.7/2002(H5N1)) polymerase basic subunit 2 (PB2) gene, partial
  	cds.
  gi|50296601|AY651746|	Influenza A virus (A/tree sparrow/HK/864/2002(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296603|AY651747|	Influenza A virus (A/teal/China/2978.1/2002(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|56548879|AY676021|	Influenza A virus (A/duck/Hong Kong/821/02(H5N1))
  	polymerase basic 2 (PB2) gene, complete cds.
  gi|50296569|AY651730|	Influenza A virus (A/Gf/HK/38/2002(H5N1)) polymerase
  	basic subunit 2 (PB2) gene, partial cds.
  gi|50296571|AY651731|	Influenza A virus (A/Ck/HK/31.2/2002(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296573|AY651732|	Influenza A virus (A/Ck/HK/37.4/2002(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296575|AY651733|	Influenza A virus (A/SCk/HK/YU100/2002(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296577|AY651734|	Influenza A virus (A/Ck/HK/YU22/2002(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296579|AY651735|	Influenza A virus (A/Ck/HK/3176.3/2002(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296581|AY651736|	Influenza A virus (A/Ck/HK/3169.1/2002(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296583|AY651737|	Influenza A virus (A/Ck/HK/FY157/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296585|AY651738|	Influenza A virus (A/Ck/HK/YU324/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296587|AY651739|	Influenza A virus (A/Ck/HK/2133.1/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296589|AY651740|	Influenza A virus (A/Ck/HK/NT93/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296591|AY651741|	Influenza A virus (A/Ck/HK/SSP141/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296593|AY651742|	Influenza A virus (A/Ck/HK/WF157/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296595|AY651743|	Influenza A virus (A/black headed
  	gull/HK/12.1/2003(H5N1)) polymerase basic subunit 2 (PB2) gene, partial
  	cds.
  gi|50296607|AY651749|	Influenza A virus (A/Dk/HN/5806/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296609|AY651750|	Influenza A virus (A/Dk/ST/4003/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296611|AY651751|	Influenza A virus (A/Ck/ST/4231/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296613|AY651752|	Influenza A virus (A/Dk/YN/6255/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296615|AY651753|	Influenza A virus (A/Dk/YN/6445/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296529|AY651710|	Influenza A virus (A/Ck/Indonesia/2A/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|56548881|AY676022|	Influenza A virus (A/egret/Hong Kong/757.2/03(H5N1))
  	polymerase basic 2 (PB2) gene, complete cds.
  gi|56548883|AY676023|	Influenza A virus (A/chicken/Korea/ES/03(H5N1))
  	polymerase basic 2 (PB2) gene, complete cds.
  gi|56548885|AY676024|	Influenza A virus (A/duck/Korea/ESD1/03(H5N1))
  	polymerase basic 2 (PB2) gene, complete cds.
  gi|50296519|AY651705|	Influenza A virus (A/Ck/Indonesia/PA/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296523|AY651707|	Influenza A virus (A/Ck/Indonesia/BL/2003(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|41207501|AY518367|	Influenza A virus (A/duck/China/E319-2/03(H5N1))
  	polymerase subunit PB2 (PB2) gene, complete cds.
  gi|45359369|AY550147|	Influenza A virus (A/chicken/Nakorn-Patom
  	Thailand/CU-K2/04(H5N1)) polymerase basic protein 2 (PB2) gene, partial
  	cds.
  gi|50296525|AY651708|	Influenza A virus (A/Ck/Indonesia/5/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296527|AY651709|	Influenza A virus (A/Ck/Indonesia/4/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296521|AY651706|	Influenza A virus (A/Dk/Indonesia/MS/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|51094103|AY590581|	Influenza A virus (A/chicken/Nakorn-
  	Patom/Thailand/CU-K2/2004(H5N1)) polymerase basic protein 2 (PBP2) gene,
  	partial cds.
  gi|47716766|AY609309|	Influenza A virus (A/chicken/Guangdong/174/04(H5N1))
  	segment 1, complete sequence.
  gi|58531082|AB166859|	Influenza A virus (A/chicken/Yamaguchi/7/2004(H5N1))
  	PB2 gene for polymerase basic protein 2, complete cds.
  gi|58531114|AB188813|	Influenza A virus (A/chicken/Oita/8/2004(H5N1)) PB2
  	gene for polymerase basic protein 2, complete cds.
  gi|50956621|AY684703|	Influenza A virus (A/chicken/Hubei/327/2004(H5N1))
  	polymerase basic protein 2 (PB2) gene, complete cds.
  gi|57915957|AY737286|	Influenza A virus (A/chicken/Guangdong/191/04(H5N1))
  	segment 1, complete sequence.
  gi|57916006|AY737293|	Influenza A virus (A/chicken/Guangdong/178/04(H5N1))
  	segment 1, complete sequence.
  gi|57916060|AY737301|	Influenza A virus (A/duck/Guangdong/173/04(H5N1))
  	segment 1, complete sequence.
  gi|55233237|AY770084|	Influenza A virus (A/chicken/Hubei/489/2004(H5N1))
  	polymerase basic protein 2 (PB2) gene, complete cds.
  gi|54873461|AY770993|	Influenza A virus (A/chicken/Ayutthaya/Thailand/CU-
  	23/04(H5N1)) polymerase basic protein 2 gene, partial cds.
  gi|58618421|AY818127|	Influenza A virus (A/chicken/Vietnam/C58/04(H5N1))
  	polymerase protein PB2 gene, complete cds.
  gi|58618423|AY818128|	Influenza A virus (A/quail/Vietnam/36/04(H5N1))
  	polymerase protein PB2 gene, complete cds.
  gi|58374183|AY856861|	Influenza A virus (A/duck/Shandong/093/2004(H5N1))
  	segment 1, complete sequence.
  gi|58531132|AB188821|	Influenza A virus (A/chicken/Kyoto/3/2004(H5N1)) PB2
  	gene for polymerase basic protein 2, complete cds.
  gi|58531150|AB189050|	Influenza A virus (A/crow/Kyoto/53/2004(H5N1)) PB2
  	gene for polymerase basic protein 2, complete cds,
  gi|58531168|AB189058|	Influenza A virus (A/crow/Osaka/102/2004(H5N1)) PB2
  	gene for polymerase basic protein 2, complete cds,
  gi|50296605|AY651748|	Influenza A virus (A/peregrine
  	falcon/HK/D0028/2004(H5N1)) polymerase basic subunit 2 (PB2) gene, complete
  	cds.
  gi|50296531|AY651711|	Influenza A virus (A/Ck/Thailand/1/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296533|AY651712|	Influenza A virus (A/Ck/Thailand/73/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296535|AY651713|	Influenza A virus (A/Ck/Thailand/9.1/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296537|AY651714|	Influenza A virus (A/Qa/Thailand/57/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296539|AY651715|	Influenza A virus (A/bird/Thailand/3.1/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296541|AY651716|	Influenza A virus (A/Dk/Thailand/71.1/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296543|AY651717|	Influenza A virus (A/Gs/Thailand/79/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|50296553|AY651722|	Influenza A virus (A/Ck/Viet Nam/33/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296555|AY651723|	Influenza A virus (A/Ck/Viet Nam/35/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296557|AY651724|	Influenza A virus (A/Ck/Viet Nam/36/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296559|AY651725|	Influenza A virus (A/Ck/Viet Nam/37/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296561|AY651726|	Influenza A virus (A/Ck/Viet Nam/38/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296563|AY651727|	Influenza A virus (A/Ck/Viet Nam/39/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296565|AY651728|	Influenza A virus (A/Ck/Viet Nam/C57/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296567|AY651729|	Influenza A virus (A/Dk/Viet Nam/11/2004(H5N1))
  	polymerase basic subunit 2 (PB2) gene, complete cds.
  gi|50296617|AY651754|	Influenza A virus (A/Ck/YN/374/2004(H5N1)) polymerase
  	basic subunit 2 (PB2) gene, partial cds.
  gi|50296619|AY651755|	Influenza A virus (A/Ck/YN/115/2004(H5N1)) polymerase
  	basic subunit 2 (PB2) gene, partial cds.
  gi|50296621|AY651756|	Influenza A virus (A/Ph/ST/44/2004(H5N1)) polymerase
  	basic subunit 2 (PB2) gene, partial cds.
  gi|50296623|AY651757|	Influenza A virus (A/Dk/HN/303/2004(H5N1)) polymerase
  	basic subunit 2 (PB2) gene, partial cds.
  gi|50296625|AY651758|	Influenza A virus (A/Dk/HN/101/2004(H5N1)) polymerase
  	basic subunit 2 (PB2) gene, partial cds.
  gi|50365712|AY653193|	Influenza A virus (A/chicken/Jilin/9/2004(H5N1))
  	segment 1, complete sequence.
  gi|47680940|AY586445|	Influenza A Virus (A/mallard/Italy/43/01(H7N3)) PB2
  	gene, partial cds.
  gi|47680930|AY586440|	Influenza A virus (A/mallard/Italy/33/01(H7N3)) PB2
  	gene, partial cds.
  gi|47680932|AY586441|	Influenza A virus (A/turkey/Italy/220158/2002(H7N3))
  	PB2 gene, partial cds.
  gi|45124743|AJ627485|	Influenza A virus (A/turkey/Italy/214845/2002(H7N3))
  	PB2 gene for RNA polymerase, genomic RNA.
  gi|45124767|AJ627496|	Influenza A virus (A/turkey/Italy/220158/2002(H7N3))
  	PB2 gene for RNA polymerase, genomic RNA.
  gi|34597782|AY303665|	Influenza A virus (A/chicken/Chile/176822/02(H7N3))
  	polymerase basic protein 2 gene, partial cds.
  gi|34597784|AY303666|	Influenza A virus (A/chicken/Chile/4957/02(H7N3))
  	polymerase basic protein 2 gene, partial cds.
  gi|47680928|AY586439|	Influenza A Virus (A/turkey/Italy/214845/02(H7N3))
  	PB2 gene, partial cds.
  gi|47834374|AY616766|	Influenza A virus (A/chicken/British
  	Columbia/04(H7N3)) PB2 polymerase subunit (PB2) gene, complete cds.
  gi|50542651|AY646085|	Influenza A virus (A/chicken/British
  	Columbia/GSC_human_B/04(H7N3)) polymerase basic protein 2 (PB2) gene,
  	complete cds.
  gi|50083053|AY648294|	Influenza A virus (A/GSC_chicken_B/British
  	Columbia/04(H7N3)) PB2 polymerase subunit (PB2) gene, complete cds.
  gi|50059194|AY650276|	Influenza A virus (A/GSC_chicken/British
  	Columbia/04(H7N3)) PB2 polymerase subunit (PB2) gene, complete cds.
  gi|60700|X58691|	Influenza A virus (A/FPV/Dobson/27 (H7N7)) gene for cap-
  	binding protein PB2, genomic RNA
  gi|325001|M38291|	Influenza virus A/FPV/Weybridge polymerase basic 2
  	protein (PB2) (seg 3) gene, complete cds.
  gi|9988661|AF268120|	Influenza A virus (A/RedKnot/Delaware/259/94(H7N7))
  	polymerase protein PB2 gene, partial cds.
  gi|40732893|AJ620347|	Influenza A virus ((A/Chicken/Germany/R28/03(H7N7))
  	A/Chicken/Germany/R28/03(H7N7)) PB2 gene for RNA polymerase, genomic RNA.
  gi|37813157|AY342410|	Influenza A virus (A/Netherlands/124/03(H7N7))
  	polymerase protein 2 gene, partial cds.
  gi|37813159|AY342411|	Influenza A virus (A/Netherlands/126/03(H7N7))
  	polymerase protein 2 gene, partial cds.
  gi|37813161|AY342412|	Influenza A virus (A/Netherlands/127/03(H7N7))
  	polymerase protein 2 gene, partial cds.
  gi|37813163|AY342413|	Influenza A virus (A/Netherlands/219/03(H7N7))
  	polymerase protein 2 gene, partial cds.
  gi|37813165|AY342414|	Influenza A virus (A/chicken/Netherlands/1/03(H7N7))
  	polymerase protein 2 gene, partial cds.
  gi|5732354|AF156443|	Influenza A virus (A/Turkey/California/189/66(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|31339587|AF523469|	Influenza A virus (A/Duck/Hong Kong/86/76(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339583|AF523467|	Influenza A virus (A/Duck/Hong Kong/366/78(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339605|AF523478|	Influenza A virus (A/Duck/Hong Kong/289/78(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339585|AF523468|	Influenza A virus (A/Duck/Hong Kong/552/79(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339589|AF523470|	Influenza A virus (A/Duck/Hong Kong/610/79(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|49356935|AY633283|	Influenza A virus (A/mallard/Alberta/321/88(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|49356939|AY633299|	Influenza A virus (A/mallard/Alberta/11/91(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|49356907|AY633171|	Influenza A virus (A/mallard/Alberta/17/91(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|5732342|AF156437|	Influenza A virus (A/Quail/Hong Kong/AF157/92(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|5732352|AF156442|	Influenza A virus (A/Quail/Arkansas/29209-1/93(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|5732340|AF156436|	Influenza A virus (A/Chicken/Hong Kong/739/94(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|5732344|AF156438|	Influenza A virus (A/Chicken/Beijing/1/94(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|22759060|AF536679|	Influenza A virus (A/Chicken/Beijing/1/95(H9N2)) PB2
  	gene, partial cds.
  gi|33318110|AF508640|	Influenza A virus (A/Ostrich/South
  	Africa/9508103/95(H9N2)) segment 1 polymerase PB2 (PB2) gene, complete cds.
  gi|33318118|AF508644|	Influenza A virus (A/Duck/Germany/113/95(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318144|AF508657|	Influenza A virus (A/Chicken/Shandong/6/96(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318152|AF508661|	Influenza A virus (A/Quail/Shanghai/8/96(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|5732346|AF156439|	Influenza A virus (A/Chicken/Korea/38349-
  	p96323/96(H9N2)) segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|5732348|AF156440|	Influenza A virus (A/Chicken/Korea/25232-
  	96006/96(H9N2)) segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|5732350|AF156441|	Influenza A virus (A/Shorebird/Delaware/9/96(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|22759068|AF536683|	Influenza A virus (A/Chicken/Hebei/1/96(H9N2)) PB2
  	gene, partial cds.
  gi|5732328|AF156430|	Influenza A virus (A/Chicken/Hong Kong/G9/97(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, complete cds.
  gi|5732330|AF156431|	Influenza A virus (A/Chicken/Hong Kong/G23/97(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|5732332|AF156432|	Influenza A virus (A/Pigeon/Hong Kong/Y233/97(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|5732334|AF156433|	Influenza A virus (A/Duck/Hong Kong/Y280/97(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|5732336|AF156434|	Influenza A virus (A/Duck/Hong Kong/Y439/97(H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|5732338|AF156435|	Influenza A virus (A/Quail/Hong Kong/G1/97 (H9N2))
  	segment 1 PB2 polymerase subunit (PB2) gene, partial cds.
  gi|33318148|AF508659|	Influenza A virus (A/Chicken/Shenzhen/9/97(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318150|AF508660|	Influenza A virus (A/Duck/Nanjing/1/97(H9N2)) segment
  	1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318124|AF508647|	Influenza A virus (A/Pheasant/Ireland/PV18/97(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|13383266|AB049153|	Influenza A virus (A/parakeet/Chiba/1/97(H9N2)) PB2
  	gene for polymerase basic protein 2, complete cds.
  gi|33318132|AF508651|	Influenza A virus (A/Chicken/Guangdong/11/97(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318136|AF508653|	Influenza A virus
  	(A/Chicken/Heilongjiang/10/97(H9N2)) segment 1 polymerase PB2 (PB2) gene,
  	partial cds.
  gi|22759062|AF536680|	Influenza A virus (A/Chicken/Beijing/2/97(H9N2)) PB2
  	gene, partial cds.
  gi|33318142|AF508656|	Influenza A virus (A/Chicken/Sichuan/5/97(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|22759066|AF536682|	Influenza A virus (A/Chicken/Guangdong/97(H9N2)) PB2
  	gene, partial cds.
  gi|22759078|AF536688|	Influenza A virus (A/Chicken/Shandong/98(H9N2)) PB2
  	gene, partial cds.
  gi|33318116|AF508643|	Influenza A virus (A/Chicken/Germany/R45/98(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318134|AF508652|	Influenza A virus (A/Chicken/Hebei/4/98(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318128|AF508649|	Influenza A virus (A/Chicken/Beijing/8/98(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, complete cds.
  gi|13383268|AB049154|	Influenza A virus (A/parakeet/Narita/92A/98(H9N2))
  	PB2 gene for polymerase basic protein 2, complete cds.
  gi|22759070|AF536684|	Influenza A virus (A/Chicken/Hebei/2/98(H9N2)) PB2
  	gene, partial cds.
  gi|22759072|AF536685|	Influenza A virus (A/Chicken/Hebei/3/98(H9N2)) PB2
  	gene, partial cds.
  gi|22759074|AF536686|	Influenza A virus (A/Chicken/Henan/98(H9N2)) PB2
  	gene, partial cds.
  gi|30025722|AY253750|	Influenza A virus (A/Chicken/Shanghai/F/98(H9N2)) RNA
  	polymerase (PB2) gene, complete cds.
  gi|12060631|AF222622|	Influenza A virus (A/Quail/Hong Kong/A17/99(H9N2))
  	segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|12060633|AF222623|	Influenza A virus (A/Pigeon/Hong Kong/FY6/99(H9N2))
  	segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|12060635|AF222624|	Influenza A virus (A/Chicken/Hong Kong/NT16/99(H9N2))
  	segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|12060637|AF222625|	Influenza A virus (A/Quail/Hong Kong/SSP10/99(H9N2))
  	segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|12060639|AF222626|	Influenza A virus (A/Pheasant/Hong
  	Kong/SSP11/99(H9N2)) segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|12060641|AF222627|	Influenza A virus (A/Chicken/Hong Kong/FY20/99(H9N2))
  	segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|12060643|AF222628|	Influenza A virus (A/Chicken/Hong Kong/KC12/99(H9N2))
  	segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|12060645|AF222629|	Influenza A virus (A/Quail/Hong Kong/NT28/99(H9N2))
  	segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|12060647|AF222630|	Influenza A virus (A/Chicken/Hong Kong/SF2/99(H9N2))
  	segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|12060649|AF222631|	Influenza A virus (A/Silky Chicken/Hong
  	Kong/SF44/99(H9N2)) segment 1 polymerase 2 (PB2) gene, partial cds.
  gi|22759076|AF536687|	Influenza A virus (A/Chicken/Liaoning/99(H9N2)) PB2
  	gene, partial cds.
  gi|33318112|AF508641|	Influenza A virus (A/Chicken/Pakistan/4/99(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, complete cds.
  gi|33318114|AF508642|	Influenza A virus (A/Chicken/Pakistan/5/99(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, complete cds.
  gi|33318126|AF508648|	Influenza A virus (A/Chicken/Korea/99029/99(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318120|AF508645|	Influenza A virus (A/Chicken/Iran/11T/99(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, complete cds.
  gi|33318122|AF508646|	Influenza A virus (A/Chicken/Saudi
  	Arabia/532/99(H9N2)) segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318140|AF508655|	Influenza A virus (A/Chicken/Ningxia/5/99(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318146|AF508658|	Influenza A virus (A/Chicken/Shijiazhuang/2/99(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|12038893|AJ291395|	Influenza A virus (A/Chicken/Pakistan/2/99(H9N2))
  	PB2 gene for polymerase PB2, genomic RNA.
  gi|22759064|AF536681|	Influenza A virus (A/Chicken/Beijing/3/99(H9N2)) PB2
  	gene, partial cds.
  gi|31339607|AF523479|	Influenza A virus (A/Duck/Shantou/1881/00(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339601|AF523476|	Influenza A virus (A/Duck/Shantou/830/00(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339603|AF523477|	Influenza A virus (A/Duck/Shantou/1796/00(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|18496117|AJ427861|	Influenza A virus (A/quail/Hong Kong/FY298/00(H9N2))
  	partial pb2 gene for PB2 polymerase protein, genomic RNA
  gi|27466041|AY180715|	Influenza A virus strain A/Wild Duck/Nanchang/2-
  	0480/2000 (H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466043|AY180716|	Influenza A virus strain A/Pigeon/Nanchang/2-
  	0461/2000 (H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466045|AY180717|	Influenza A virus strain A/Duck/Nanchang/1-0070/2000
  	(H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466055|AY180722|	Influenza A virus strain A/Duck/Nanchang/10-389/2000
  	(H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466057|AY180723|	Influenza A virus strain A/Pigeon/Nanchang/7-058/2000
  	(H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466067|AY180728|	Influenza A virus strain A/Quail/Nanchang/2-0460/2000
  	(H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466085|AY180737|	Influenza A virus strain A/Pigeon/Nanchang/11-
  	145/2000 (H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466087|AY180738|	Influenza A virus strain A/Duck/Nanchang/11-197/2000
  	(H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466091|AY180740|	Influenza A virus strain A/Duck/Nanchang/11-290/2000
  	(H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466093|AY180741|	Influenza A virus strain A/Duck/Nanchang/11-392/2000
  	(H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|31339575|AF523463|	Influenza A virus (A/Duck/Shantou/2134/00(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339579|AF523465|	Influenza A virus (A/Duck/Shantou/1043/00(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339581|AF523466|	Influenza A virus (A/Duck/Shantou/1042/00(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339593|AF523472|	Influenza A virus (A/Duck/Shantou/2102/00(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339595|AF523473|	Influenza A virus (A/Duck/Shantou/2144/00(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339597|AF523474|	Influenza A virus (A/Duck/Shantou/2143/00(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|33318138|AF508654|	Influenza A virus (A/Chicken/Henan/62/00(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|33318130|AF508650|	Influenza A virus (A/Chicken/Guangdong/10/00(H9N2))
  	segment 1 polymerase PB2 (PB2) gene, partial cds.
  gi|27466121|AY180755|	Influenza A virus strain A/Duck/Nanchang/7-092/2000
  	(H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466141|AY180765|	Influenza A virus strain A/Chicken/Nanchang/4-
  	010/2000 (H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466157|AY180773|	Influenza A virus strain A/Quail/Nanchang/4-040/2000
  	(H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|27466159|AY180774|	Influenza A virus strain A/Chicken/Nanchang/1-
  	0016/2000 (H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|55469788|AY768575|	Influenza A virus (A/chicken/Korea/SNU0028/00(H9N2))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|55469790|AY768576|	Influenza A virus (A/chicken/Korea/SNU0037/00(H9N2))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|55469792|AY768577|	Influenza A virus (A/chicken/Korea/SNU0073/00(H9N2))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|55469794|AY768578|	Influenza A virus (A/chicken/Korea/SNU0091/00(H9N2))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|55469796|AY768579|	Influenza A virus (A/chicken/Korea/SNU0140/00(H9N2))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|55469798|AY768580|	Influenza A virus (A/chicken/Korea/SNU0146/00(H9N2))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|55469800|AY768581|	Influenza A virus (A/chicken/Korea/SNU1035C/00(H9N2))
  	polymerase basic subunit 2 (PB2) gene, partial cds.
  gi|27466143|AY180766|	Influenza A virus strain A/Chicken/Nanchang/4-
  	301/2001 (H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|31339599|AF523475|	Influenza A virus (A/Duck/Shantou/2088/01(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339591|AF523471|	Influenza A virus (A/Duck/Shantou/1605/01(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|31339577|AF523464|	Influenza A virus (A/Wild Duck/Shantou/4808/01(H9N2))
  	polymerase (PB2) gene, partial cds.
  gi|27466097|AY180743|	Influenza A virus strain A/Chicken/Nanchang/4-
  	361/2001 (H9N2) polymerase subunit PB2 (PB2) gene, partial cds.
  gi|54398631|AY664792|	Influenza A virus
  	(A/chicken/HongKong/CSW153/03(H9N2)) polymerase basic protein 2 (PB2) gene,
  	partial cds.
  gi|54398633|AY664793|	Influenza A virus (A/chicken/HongKong/AP45/03(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|54398635|AY664794|	Influenza A virus (A/chicken/HongKong/BD90/03(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|54398637|AY664795|	Influenza A virus
  	(A/chicken/HongKong/CSW291/03(H9N2)) nonfunctional polymerase basic protein
  	2 (PB2) gene, partial sequence.
  gi|54398638|AY664796|	Influenza A virus
  	(A/chicken/HongKong/CSW304/03(H9N2)) nonfunctional polymerase basic protein
  	2 (PB2) gene, partial sequence.
  gi|54398639|AY664797|	Influenza A virus (A/chicken/HongKong/FY23/03(H9N2))
  	nonfunctional polymerase basic protein 2 (PB2) gene, partial sequence.
  gi|54398640|AY664798|	Influenza A virus
  	(A/guineafowl/HongKong/NT101/03(H9N2)) polymerase basic protein 2 (PB2)
  	gene, partial cds.
  gi|54398642|AY664799|	Influenza A virus (A/chicken/HongKong/NT142/03(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|54398644|AY664800|	Influenza A virus (A/chicken/HongKong/SF1/03(H9N2))
  	nonfunctional polymerase basic protein 2 (PB2) gene, partial sequence.
  gi|54398645|AY664801|	Influenza A virus
  	(A/chicken/HongKong/SSP101/03(H9N2)) nonfunctional polymerase basic protein
  	2 (PB2) gene, partial sequence.
  gi|54398646|AY664802|	Influenza A virus (A/chicken/HongKong/TP38/03(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|54398648|AY664803|	Influenza A virus (A/chicken/HongKong/WF126/03(H9N2))
  	nonfunctional polymerase basic protein 2 (PB2) gene, partial sequence.
  gi|54398649|AY664804|	Influenza A virus (A/pigeon/HongKong/WF53/03(H9N2))
  	nonfunctional polymerase basic protein 2 (PB2) gene, partial sequence.
  gi|54398650|AY664805|	Influenza A virus (A/pheasant/HongKong/WF54/03(H9N2))
  	nonfunctional polymerase basic protein 2 (PB2) gene, partial sequence.
  gi|54398651|AY664806|	Influenza A virus
  	(A/guineafowl/HongKong/NT184/03(H9N2)) polymerase basic protein 2 (PB2)
  	gene, partial cds.
  gi|54398653|AY664807|	Influenza A virus (A/chicken/HongKong/WF120/03(H9N2))
  	nonfunctional polymerase basic protein 2 (PB2) gene, partial sequence.
  gi|54398654|AY664808|	Influenza A virus (A/chicken/HongKong/NT366/03(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|54398656|AY664809|	Influenza A virus
  	(A/chicken/HongKong/SSP418/03(H9N2)) polymerase basic protein 2 (PB2) gene,
  	partial cds.
  gi|54398658|AY664810|	Influenza A virus (A/chicken/HongKong/YU427/03(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|55793686|AY800240|	Influenza A virus (A/chicken/Korea/S1/2003(H9N2))
  	polymerase basic protein 2 (PB2) gene, partial cds.
  gi|58429686|AY862710|	Influenza A virus (A/silky chicken/Korea/S3/03(H9N2))
  	PB2 (PB2) gene, partial cds.
  gi|58429688|AY862711|	Influenza A virus (A/chicken/Korea/S4/03(H9N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429690|AY862712|	Influenza A virus (A/chicken/Korea/S5/03(H9N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429692|AY862713|	Influenza A virus (A/chicken/Korea/S12/03(H9N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429694|AY862714|	Influenza A virus (A/duck/Korea/S13/03(H9N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429696|AY862715|	Influenza A virus (A/dove/Korea/S14/03(H9N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429698|AY862716|	Influenza A virus (A/chicken/Korea/S15/03(H9N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429700|AY862717|	Influenza A virus (A/chicken/Korea/S16/03(H9N2)) PB2
  	(PB2) gene, partial cds.
  gi|58429702|AY862718|	Influenza A virus (A/chicken/Korea/S18/03(H9N2)) PB2
  	(PB2) gene, partial cds.

  Sequences used in analysis of Influenza A Polymerase Acidic protein (PA)

  gi|27465935|AY180662|	Influenza A virus strain A/Quail/Nanchang/12-340/2000
  	(H1N1) polymerase subunit PA (PA) gene, partial cds.
  gi|49357063|AY633217|	Influenza A virus (A/mallard/Alberta/211/98(H1N1))
  	polymerase protein A (PA) gene, partial cds.
  gi|5918195|AJ243994|	Influenza A virus (STRAIN A/MALLARD/NEW YORK/6750/78)
  	partial mRNA for PA protein.
  gi|45272157|AY422034|	Influenza A virus (A/Duck/Hokkaido/95/01(H2N2)) PA
  	protein (PA) gene, partial cds.
  gi|27465965|AY180677|	Influenza A virus strain A/Chicken/Nanchang/3-
  	120/2001 (H3N2) polymerase subunit PA (PA) gene, partial cds.
  gi|56159994|AY779263|	Influenza A virus (A/turkey/North
  	Carolina/12344/03(H3N2)) polymerase acidic protein (PA) gene, partial cds.
  gi|56159996|AY779264|	Influenza A virus (A/turkey/Minnesota/764-2/03(H3N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|58429736|AY862687|	Influenza A virus (A/chicken/Korea/S6/03(H3N2)) PA
  	(PA) gene, partial cds.
  gi|58429738|AY862688|	Influenza A virus (A/duck/Korea/S7/03(H3N2)) PA (PA)
  	gene, partial cds.
  gi|58429740|AY862689|	Influenza A virus (A/duck/Korea/S8/03(H3N2)) PA (PA)
  	gene, partial cds.
  gi|58429742|AY862690|	Influenza A virus (A/duck/Korea/S9/03(H3N2)) PA (PA)
  	gene, partial cds.
  gi|58429744|AY862691|	Influenza A virus (A/duck/Korea/S10/03(H3N2)) PA (PA)
  	gene, partial cds.
  gi|58429746|AY862692|	Influenza A virus (A/dove/Korea/S11/03(H3N2)) PA (PA)
  	gene, partial cds.
  gi|18091833|AF213914|	Influenza A virus (A/Chicken/Italy/5945/95(H3N2))
  	segment 3 PA polymerase protein gene, partial cds.
  gi|58531086|AB166861|	Influenza A virus (A/chicken/Yamaguchi/7/2004(H5N1))
  	PA gene for polymerase acidic protein, complete cds.
  gi|58531118|AB188815|	Influenza A virus (A/chicken/Oita/8/2004(H5N1)) PA
  	gene for polymerase acidic protein, complete cds.
  gi|9863935|AF216739|	Influenza A virus (A/Environment/Hong Kong/437-10/99
  	(H5N1)) polymerase acidic protein gene, complete cds.
  gi|14165201|AF380163|	Influenza A virus (A/Goose/Guangdong/3/97(H5N1))
  	segment 3 polymerase (PA) gene, complete cds.
  gi|18092185|AF398427|	Influenza A virus (A/Goose/Hong
  	Kong/385.3/2000(H5N1)) polymerase (PA) gene, partial cds.
  gi|18092187|AF398428|	Influenza A virus (A/Goose/Hong
  	Kong/385.5/2000(H5N1)) polymerase (PA) gene, partial cds.
  gi|21359667|AF468841|	Influenza A virus (A/Duck/Anyang/AVL-1/2001(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|28849710|AF509195|	Influenza A virus (A/Chicken/Hong Kong/FY77/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849712|AF509196|	Influenza A virus (A/Chicken/Hong Kong/YU562/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849714|AF509197|	Influenza A virus (A/Chicken/Hong Kong/YU563/01
  	(H5N1)) polymerase (PA) gene, complete cds.
  gi|28849716|AF509198|	Influenza A virus (A/Chicken/Hong Kong/FY150/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849718|AF509199|	Influenza A virus (A/Pheasant/Hong Kong/FY155/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849720|AF509200|	Influenza A virus (A/Silky Chicken/Hong Kong/SF189/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849722|AF509201|	Influenza A virus (A/Quai1/Hong Kong/SF203/01 (H5N1))
  	polymerase (PA) gene, partial cds.
  gi|28849724|AF509202|	Influenza A virus (A/Pigeon/Hong Kong/SF215/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849726|AF509203|	Influenza A virus (A/Chicken/Hong Kong/SF219/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849728|AF509204|	Influenza A virus (A/Chicken/Hong Kong/715.5/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849730|AF509205|	Influenza A virus (A/Chicken/Hong Kong/751.1/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849732|AF509206|	Influenza A virus (A/Chicken/Hong Kong/822.1/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849734|AF509207|	Influenza A virus (A/Chicken/Hong Kong/829.2/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849736|AF509208|	Influenza A virus (A/Chicken/Hong Kong/830.2/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849738|AF509209|	Influenza A virus (A/Chicken/Hong Kong/858.3/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849740|AF509210|	Influenza A virus (A/Chicken/Hong Kong/866.3/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849742|AF509211|	Influenza A virus (A/Chicken/Hong Kong/867.1/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849744|AF509212|	Influenza A virus (A/Chicken/Hong Kong/879.1/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849746|AF509213|	Influenza A virus (A/Chicken/Hong Kong/873.3/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849748|AF509214|	Influenza A virus (A/Chicken/Hong Kong/876.1/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849750|AF509215|	Influenza A virus (A/Chicken/Hong Kong/891.1/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849752|AF509216|	Influenza A virus (A/Chicken/Hong Kong/893.1/01
  	(H5N1)) polymerase (PA) gene, partial cds.
  gi|28849754|AF509217|	Influenza A virus (A/Goose/Hong Kong/76.1/01 (H5N1))
  	polymerase (PA) gene, partial cds.
  gi|28849756|AF509218|	Influenza A virus (A/Goose/Hong Kong/ww100/01 (H5N1))
  	polymerase (PA) gene, partial cds.
  gi|28849758|AF509219|	Influenza A virus (A/Duck/Hong Kong/573.4/01 (H5N1))
  	polymerase (PA) gene, partial cds.
  gi|28849760|AF509220|	Influenza A virus (A/Duck/Hong Kong/646.3/01 (H5N1))
  	polymerase (PA) gene, partial cds.
  gi|19697861|AY059526|	Influenza A virus (A/Goose/Hong Kong/ww26/2000(H5N1))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|19697863|AY059527|	Influenza A virus (A/Goose/Hong Kong/ww28/2000(H5N1))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|19697865|AY059528|	Influenza A virus (A/Duck/Hong Kong/ww381/2000(H5N1))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|19697869|AY059530|	Influenza A virus (A/Duck/Hong Kong/ww461/2000(H5N1))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|19697871|AY059531|	Influenza A virus (A/Goose/Hong
  	Kong/ww491/2000(H5N1)) segment 3 polymerase (PA) gene, partial cds.
  gi|19697873|AY059532|	Influenza A virus (A/Duck/Hong
  	Kong/2986.1/2000(H5N1)) segment 3 polymerase (PA) gene, partial cds.
  gi|19697875|AY059533|	Influenza A virus (A/Goose/Hong
  	Kong/3014.8/2000(H5N1)) segment 3 polymerase (PA) gene, partial cds.
  gi|28821204|AY221566|	Influenza A virus (A/Chicken/HongKong/NT873.3/01-
  	MB(H5N1)) polymerase (PA) gene, partial cds.
  gi|28821206|AY221567|	Influenza A virus
  	(A/Chicken/HongKong/NT873.3/01(H5N1)) polymerase (PA) gene, partial cds.
  gi|28821208|AY221568|	Influenza A virus (A/Chicken/HongKong/FY150/01-
  	MB(H5N1)) polymerase (PA) gene, partial cds.
  gi|28821210|AY221569|	Influenza A virus (A/Chicken/HongKong/FY150/01(H5N1))
  	polymerase (PA) gene, partial cds.
  gi|28821212|AY221570|	Influenza A virus (A/Pheasant/HongKong/FY155/01-
  	MB(H5N1)) polymerase (PA) gene, partial cds.
  gi|28821214|AY221571|	Influenza A virus
  	(A/Pheasant/HongKong/FY155/01(H5N1)) polymerase (PA) gene, partial cds.
  gi|28821216|AY221572|	Influenza A virus (A/Chicken/HongKong/YU822.2/01-
  	MB(H5N1)) polymerase (PA) gene, partial cds.
  gi|28821218|AY221573|	Influenza A virus
  	(A/Chicken/HongKong/YU822.2/01(H5N1)) polymerase (PA) gene, partial cds.
  gi|28821220|AY221574|	Influenza A virus (A/Chicken/HongKong/YU562/01(H5N1))
  	polymerase (PA) gene, partial cds.
  gi|41207483|AY518365|	Influenza A virus (A/duck/China/E319-2/03(H5N1))
  	polymerase (PA) gene, complete cds.
  gi|51094114|AY551934|	Influenza A virus (A/chicken/Nakorn-Patom
  	Thailand/CU-K2/04(H5N1)) polymerase (PA) gene, complete cds.
  gi|47834839|AY576406|	Influenza A virus (A/Gs/HK/739.2/02 (H5N1))
  	polymerase (PA) gene, partial cds.
  gi|47834841|AY576407|	Influenza A virus (A/Eg/HK/757.3/02 (H5N1))
  	polymerase (PA) gene, partial cds.
  gi|47834843|AY576408|	Influenza A virus (A/G.H/HK/793.1/02 (H5N1))
  	polymerase (PA) gene, partial cds.
  gi|47834845|AY576409|	Influenza A virus (A/Dk/HK/821/02 (H5N1)) polymerase
  	(PA) gene, partial cds.
  gi|47834847|AY576410|	Influenza A virus (A/Ck/HK/31.4/02 (H5N1)) polymerase
  	(PA) gene, complete cds.
  gi|47834849|AY576411|	Influenza A virus (A/Ck/HK/61.9/02 (H5N1)) polymerase
  	(PA) gene, complete cds.
  gi|47834851|AY576412|	Influenza A virus (A/Ck/HK/YU777/02 (H5N1))
  	polymerase (PA) gene, complete cds.
  gi|47834853|AY576413|	Influenza A virus (A/Ck/HK/96.1/02 (H5N1)) polymerase
  	(PA) gene, partial cds.
  gi|47834855|AY576414|	Influenza A virus (A/Ck/HK/409.1/02 (H5N1))
  	polymerase (PA) gene, partial cds.
  gi|47834857|AY576415|	Influenza A virus (A/Ph/HK/sv674.15/02 (H5N1))
  	polymerase (PA) gene, complete cds.
  gi|47156478|AY585462|	Influenza A virus (A/duck/Fujian/01/2002(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156480|AY585463|	Influenza A virus (A/duck/Fujian/13/2002(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156482|AY585464|	Influenza A virus (A/duck/Fujian/17/2001(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156484|AY585465|	Influenza A virus (A/duck/Fujian/19/2000(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156486|AY585466|	Influenza A virus (A/duck/Guangdong/01/2001(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156488|AY585467|	Influenza A virus (A/duck/Guangdong/07/2000(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156490|AY585468|	Influenza A virus (A/duck/Guangdong/12/2000(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156492|AY585469|	Influenza A virus (A/duck/Guangdong/22/2002(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156494|AY585470|	Influenza A virus (A/duck/Guangdong/40/2000(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156496|AY585471|	Influenza A virus (A/duck/Guangxi/07/1999(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156498|AY585472|	Influenza A virus (A/duck/Guangxi/22/2001(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156500|AY585473|	Influenza A virus (A/duck/Guangxi/35/2001(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156502|AY585474|	Influenza A virus (A/duck/Guangxi/50/2001(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156504|AY585475|	Influenza A virus (A/duck/Guangxi/53/2002(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156506|AY585476|	Influenza A virus (A/duck/Shanghai/08/2001(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156508|AY585477|	Influenza A virus (A/duck/Shanghai/13/2001(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156510|AY585478|	Influenza A virus (A/duck/Shanghai/35/2002(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156512|AY585479|	Influenza A virus (A/duck/Shanghai/37/2002(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156514|AY585480|	Influenza A virus (A/duck/Shanghai/38/2001(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156516|AY585481|	Influenza A virus (A/duck/Zhejiang/11/2000(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47156518|AY585482|	Influenza A virus (A/duck/Zhejiang/52/2000(H5N1))
  	polymerase (PA) mRNA, complete cds.
  gi|47716770|AY609311|	Influenza A virus (A/chicken/Guangdong/174/04(H5N1))
  	segment 3, complete sequence.
  gi|50313026|AY651597|	Influenza A virus (A/Ck/Indonesia/4/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313028|AY651598|	Influenza A virus (A/Ck/Indonesia/5/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313030|AY651599|	Influenza A virus (A/Ck/Indonesia/2A/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313032|AY651600|	Influenza A virus (A/Dk/Indonesia/MS/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313034|AY651601|	Influenza A virus (A/Ck/Indonesia/BL/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313036|AY651602|	Influenza A virus (A/Ck/Indonesia/PA/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313038|AY651603|	Influenza A virus (A/Ck/Thailand/1/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313040|AY651604|	Influenza A virus (A/Ck/Thailand/73/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313042|AY651605|	Influenza A virus (A/Ck/Thailand/9.1/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313044|AY651606|	Influenza A virus (A/Qa/Thailand/57/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313046|AY651607|	Influenza A virus (A/bird/Thailand/3.1/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313048|AY651608|	Influenza A virus (A/Dk/Thailand/71.1/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313050|AY651609|	Influenza A virus (A/Gs/Thailand/79/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313060|AY651614|	Influenza A virus (A/Ck/Viet Nam/33/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313062|AY651615|	Influenza A virus (A/Ck/Viet Nam/35/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313064|AY651616|	Influenza A virus (A/Ck/Viet Nam/36/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313066|AY651617|	Influenza A virus (A/Ck/Viet Nam/37/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313068|AY651618|	Influenza A virus (A/Ck/Viet Nam/38/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313070|AY651619|	Influenza A virus (A/Ck/Viet Nam/39/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313072|AY651620|	Influenza A virus (A/Ck/Viet Nam/C57/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313074|AY651621|	Influenza A virus (A/Dk/Viet Nam/11/2004(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313076|AY651622|	Influenza A virus (A/Gf/HK/38/2002(H5N1)) polymerase
  	acidic protein (PA) gene, complete cds.
  gi|50313078|AY651623|	Influenza A virus (A/Ck/HK/31.2/2002(H5N1))
  	polymerase acidic protein (PA) gene, complete cds.
  gi|50313080|AY651624|	Influenza A virus (A/Ck/HK/37.4/2002(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313082|AY651625|	Influenza A virus (A/SCk/HK/YU100/2002(H5N1))
  	polymerase acidic protein (PA) gene, complete cds.
  gi|50313084|AY651626|	Influenza A virus (A/Ck/HK/YU22/2002(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313086|AY651627|	Influenza A virus (A/Ck/HK/3176.3/2002(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313088|AY651628|	Influenza A virus (A/Ck/HK/3169.1/2002(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313090|AY651629|	Influenza A virus (A/Ck/HK/FY157/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313092|AY651630|	Influenza A virus (A/Ck/HK/YU324/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313094|AY651631|	Influenza A virus (A/Ck/HK/2133.1/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313096|AY651632|	Influenza A virus (A/Ck/HK/NT93/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313098|AY651633|	Influenza A virus (A/Ck/HK/SSP141/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313100|AY651634|	Influenza A virus (A/Ck/HK/WF157/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313102|AY651635|	Influenza A virus (A/black headed
  	gull/HK/12.1/2003(H5N1)) polymerase acidic protein (PA) gene, partial cds.
  gi|50313104|AY651636|	Influenza A virus (A/grey heron/HK/861.1/2002(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313106|AY651637|	Influenza A virus (A/feral
  	pigeon/HK/862.7/2002(H5N1)) polymerase acidic protein (PA) gene, partial
  	cds.
  gi|50313108|AY651638|	Influenza A virus (A/tree sparrow/HK/864/2002(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313110|AY651639|	Influenza A virus (A/teal/China/2978.1/2002(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313112|AY651640|	Influenza A virus (A/peregrine
  	falcon/HK/D0028/2004(H5N1)) polymerase acidic protein (PA) gene, partial
  	cds.
  gi|50313114|AY651641|	Influenza A virus (A/Dk/HN/5806/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313116|AY651642|	Influenza A virus (A/Dk/HN/303/2004(H5N1)) polymerase
  	acidic protein (PA) gene, partial cds.
  gi|50313118|AY651643|	Influenza A virus (A/Dk/HN/101/2004(H5N1)) polymerase
  	acidic protein (PA) gene, partial cds.
  gi|50313120|AY651644|	Influenza A virus (A/Dk/ST/4003/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313122|AY651645|	Influenza A virus (A/Ph/ST/44/2004(H5N1)) polymerase
  	acidic protein (PA) gene, partial cds.
  gi|50313124|AY651646|	Influenza A virus (A/Ck/ST/4231/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313126|AY651647|	Influenza A virus (A/Dk/YN/6255/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313128|AY651648|	Influenza A virus (A/Dk/YN/6445/2003(H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|50313130|AY651649|	Influenza A virus (A/Ck/YN/115/2004(H5N1)) polymerase
  	acidic protein (PA) gene, partial cds.
  gi|50313132|AY651650|	Influenza A virus (A/Ck/YN/374/2004(H5N1)) polymerase
  	acidic protein (PA) gene, partial cds.
  gi|50365724|AY653198|	Influenza A virus (A/chicken/Jilin/9/2004(H5N1))
  	segment 3, complete sequence.
  gi|56548923|AY676029|	Influenza A virus (A/duck/Hong Kong/821/02(H5N1))
  	polymerase (PA) gene, complete cds.
  gi|56548925|AY676030|	Influenza A virus (A/egret/Hong Kong/757.2/03(H5N1))
  	polymerase (PA) gene, complete cds.
  gi|56548927|AY676031|	Influenza A virus (A/chicken/Korea/ES/03(H5N1))
  	polymerase (PA) gene, complete cds.
  gi|56548929|AY676032|	Influenza A virus (A/duck/Korea/ESD1/03(H5N1))
  	polymerase (PA) gene, complete cds.
  gi|50956625|AY684705|	Influenza A virus (A/chicken/Hubei/327/2004(H5N1))
  	polymerase (PA) gene, complete cds.
  gi|56119221|AY720944|	Influenza A virus (A/chicken/Viet Nam/DT-
  	171/2004(H5N1)) polymerase acidic protein (PA) gene, partial cds.
  gi|56119227|AY720947|	Influenza A virus (A/duck/Viet Nam/TG-
  	007A/2004(H5N1)) polymerase acidic protein (PA) gene, partial cds.
  gi|57924419|AY724784|	Influenza A virus (A/chicken/Viet Nam/HCM-
  	022/2004(H5N1)) polymerase (PA) gene, partial cds.
  gi|57924480|AY724786|	Influenza A virus (A/chicken/Viet Nam/DN-
  	045/2004(H5N1)) polymerase (PA) gene, partial cds.
  gi|57924569|AY724788|	Influenza A virus (A/chicken/Viet Nam/VL-
  	008/2004(H5N1)) polymerase (PA) gene, partial cds.
  gi|57924680|AY724790|	Influenza A virus (A/chicken/Viet Nam/AG-
  	010/2004(H5N1)) polymerase (PA) gene, partial cds.
  gi|57924765|AY724792|	Influenza A virus (A/chicken/Viet Nam/DT-
  	015/2004(H5N1)) polymerase (PA) gene, partial cds.
  gi|57924882|AY724796|	Influenza A virus (A/chicken/Viet Nam/LA-
  	024/2004(H5N1)) polymerase (PA) gene, partial cds.
  gi|57915971|AY737288|	Influenza A virus (A/chicken/Guangdong/191/04(H5N1))
  	segment 3, complete sequence.
  gi|57916018|AY737295|	Influenza A virus (A/chicken/Guangdong/178/04(H5N1))
  	segment 3, complete sequence.
  gi|57916074|AY737303|	Influenza A virus (A/duck/Guangdong/173/04(H5N1))
  	segment 3, complete sequence.
  gi|55233234|AY770082|	Influenza A virus (A/chicken/Hubei/489/2004(H5N1))
  	polymerase (PA) gene, complete cds.
  gi|54873465|AY770995|	Influenza A virus (A/chicken/Ayutthaya/Thailand/CU-
  	23/04(H5N1)) polymerase gene, partial cds.
  gi|58618433|AY818133|	Influenza A virus (A/chicken/Vietnam/C58/04(H5N1))
  	polymerase protein PA gene, complete cds.
  gi|58618435|AY818134|	Influenza A virus (A/quail/Vietnam/36/04(H5N1))
  	polymerase protein PA gene, complete cds.
  gi|58374187|AY856863|	Influenza A virus (A/duck/Shandong/093/2004(H5N1))
  	segment 3, complete sequence.
  gi|58531136|AB188823|	Influenza A virus (A/chicken/Kyoto/3/2004(H5N1)) PA
  	gene for polymerase acidic protein, complete cds.
  gi|58531154|AB189052|	Influenza A virus (A/crow/Kyoto/53/2004(H5N1)) PA
  	gene for polymerase acidic protein, complete cds,
  gi|58531170|AB189059|	Influenza A virus (A/crow/Osaka/102/2004(H5N1)) PA
  	gene for polymerase acidic protein, complete cds,.
  gi|3335418|AF046087|	Influenza A virus (A/Chicken/Hong Kong/220/97 (H5N1))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|6048895|AF098604|	Influenza A virus (A/Chicken/Hong Kong/258/97 (H5N1))
  	PA protein (PA) gene, complete cds.
  gi|6048897|AF098605|	Influenza A virus (A/Chicken/Hong Kong/y388/97 (H5N1))
  	PA protein (PA) gene, complete cds.
  gi|6048899|AF098606|	Influenza A virus (A/Chicken/Hong Kong/728/97 (H5N1))
  	PA protein (PA) gene, complete cds.
  gi|6048901|AF098607|	Influenza A virus (A/Chicken/Hong Kong/786/97 (H5N1))
  	PA protein (PA) gene, complete cds.
  gi|6048903|AF098608|	Influenza A virus (A/Chicken/Hong Kong/915/97 (H5N1))
  	PA protein (PA) gene, complete cds.
  gi|6048905|AF098609|	Influenza A virus (A/Duck/Hong Kong/p46/97 (H5N1)) PA
  	protein (PA) gene, complete cds.
  gi|6048907|AF098610|	Influenza A virus (A/Duck/Hong Kong/y283/97 (H5N1)) PA
  	protein (PA) gene, complete cds.
  gi|6048909|AF098611|	Influenza A virus (A/Goose/Hong Kong/w355/97 (H5N1))
  	PA protein (PA) gene, complete cds.
  gi|5805280|AF144302|	Influenza A virus (A/Goose/Guangdong/1/96(H5N1))
  	polymerase (PA) gene, complete cds.
  gi|9863880|AF216715|	Influenza A virus (A/Environment/Hong Kong/437-4/99
  	(H5N1)) polymerase acidic protein gene, complete cds.
  gi|9863899|AF216723|	Influenza A virus (A/Environment/Hong Kong/437-6/99
  	(H5N1)) polymerase acidic protein gene, complete cds.
  gi|9863917|AF216731|	Influenza A virus (A/Environment/Hong Kong/437-8/99
  	(H5N1)) polymerase acidic protein gene, complete cds.
  gi|34597776|AY303660|	Influenza A virus (A/chicken/Chile/176822/02(H7N3))
  	polymerase acidic protein gene, complete cds.
  gi|34597778|AY303661|	Influenza A virus (A/chicken/Chile/4957/02(H7N3))
  	polymerase acidic protein gene, complete cds.
  gi|34597780|AY303662|	Influenza A virus (A/chicken/Chile/4322/02(H7N3))
  	polymerase acidic protein gene, partial cds.
  gi|47680912|AY586431|	Influenza A Virus (A/mallard/Italy/43/01(H7N3)) PA
  	gene, partial cds.
  gi|47680914|AY586432|	Influenza A virus (A/mallard/Italy/33/01(H7N3)) PA
  	gene, partial cds.
  gi|47680916|AY586433|	Influenza A virus (A/turkey/Italy/220158/2002(H7N3))
  	PA gene, partial cds.
  gi|47680918|AY586434|	Influenza A Virus (A/turkey/Italy/214845/02(H7N3)) PA
  	gene, partial cds.
  gi|47834370|AY616764|	Influenza A virus (A/chicken/British
  	Columbia/04(H7N3)) polymerase acidic protein 2 (PA) gene, complete cds.
  gi|50542647|AY646083|	Influenza A virus (A/chicken/British
  	Columbia/GSC_human_B/04(H7N3)) polymerase acidic protein 2 (PA) gene,
  	complete cds.
  gi|50083049|AY648292|	Influenza A virus (A/GSC_chicken_B/British
  	Columbia/04(H7N3)) polymerase acidic protein 2 (PA) gene, complete cds.
  gi|50059192|AY650275|	Influenza A virus (A/GSC_chicken/British
  	Columbia/04(H7N3)) polymerase acidic protein 2 (PA) gene, complete cds.
  gi|9988639|AF268109|	Influenza A virus (A/RedKnot/Delaware/259/94(H7N7))
  	polymerase protein PA gene, partial cds.
  gi|40353080|AJ619677|	Influenza A virus (A/chicken/Germany/R28/03(H7N7)) PA
  	gene for polymerase complex subunit PA, genomic RNA.
  gi|37813167|AY342415|	Influenza A virus (A/Netherlands/124/03(H7N7))
  	polymerase protein A gene, partial cds.
  gi|37813169|AY342416|	Influenza A virus (A/Netherlands/126/03(H7N7))
  	polymerase protein A gene, partial cds.
  gi|37813171|AY342417|	Influenza A virus (A/Netherlands/127/03(H7N7))
  	polymerase protein A gene, partial cds.
  gi|37813173|AY342418|	Influenza A virus (A/Netherlands/219/03(H7N7))
  	polymerase protein A gene, complete cds.
  gi|37813175|AY342419|	Influenza A virus (A/Netherlands/033/03(H7N7))
  	polymerase protein A gene, complete cds.
  gi|37813177|AY342420|	Influenza A virus (A/chicken/Netherlands/1/03(H7N7))
  	polymerase protein A gene, complete cds.
  gi|13383274|AB049157|	Influenza A virus (A/parakeet/Chiba/1/97(H9N2)) PA
  	gene for polymerase acidic protein, complete cds.
  gi|13383276|AB049158|	Influenza A virus (A/parakeet/Narita/92A/98(H9N2)) PA
  	gene for polymerase acidic protein, complete cds.
  gi|33318154|AF508662|	Influenza A virus (A/Ostrich/South
  	Africa/9508103/95(H9N2)) segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318156|AF508663|	Influenza A virus (A/Chicken/Pakistan/4/99(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318158|AF508664|	Influenza A virus (A/Chicken/Pakistan/5/99(H9N2))
  	segment 3 polymerase PA (PA) gene, partial cds.
  gi|33318160|AF508665|	Influenza A virus (A/Chicken/Germany/R45/98(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318162|AF508666|	Influenza A virus (A/Duck/Germany/113/95(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318164|AF508667|	Influenza A virus (A/Chicken/Iran/11T/99(H9N2))
  	segment 3 polymerase PA (PA) gene, partial cds.
  gi|33318166|AF508668|	Influenza A virus (A/Chicken/Saudi
  	Arabia/532/99(H9N2)) segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318168|AF508669|	Influenza A virus (A/Pheasant/Ireland/PV18/97(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318170|AF508670|	Influenza A virus (A/Chicken/Korea/99029/99(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318172|AF508671|	Influenza A virus (A/Chicken/Beijing/8/98(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318174|AF508672|	Influenza A virus (A/Chicken/Guangdong/10/00(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318176|AF508673|	Influenza A virus (A/Chicken/Guangdong/11/97(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318178|AF508674|	Influenza A virus (A/Chicken/Hebei/4/98(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318180|AF508675|	Influenza A virus
  	(A/Chicken/Heilongjiang/10/97(H9N2)) segment 3 polymerase PA (PA) gene,
  	complete cds.
  gi|33318182|AF508676|	Influenza A virus (A/Chicken/Henan/62/00(H9N2))
  	segment 3 polymerase PA (PA) gene, partial cds.
  gi|33318184|AF508677|	Influenza A virus (A/Chicken/Ningxia/5/99(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318186|AF508678|	Influenza A virus (A/Chicken/Sichuan/5/97(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318188|AF508679|	Influenza A virus (A/Chicken/Shandong/6/96(H9N2))
  	segment 3 polymerase PA (PA) gene, partial cds.
  gi|33318190|AF508680|	Influenza A virus (A/Chicken/Shijiazhuang/2/99(H9N2))
  	segment 3 polymerase PA (PA) gene, partial cds.
  gi|33318192|AF508681|	Influenza A virus (A/Chicken/Shenzhen/9/97(H9N2))
  	segment 3 polymerase PA (PA) gene, complete cds.
  gi|33318194|AF508682|	Influenza A virus (A/Duck/Nanjing/1/97(H9N2)) segment
  	3 polymerase PA (PA) gene, complete cds.
  gi|33318196|AF508683|	Influenza A virus (A/Quail/Shanghai/8/96(H9N2))
  	segment 3 polymerase PA (PA) gene, partial cds.
  gi|31339541|AF523446|	Influenza A virus (A/Duck/Shantou/1043/00(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339543|AF523447|	Influenza A virus (A/Duck/Shantou/1042/00(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339545|AF523448|	Influenza A virus (A/Duck/Shantou/2088/01(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339547|AF523449|	Influenza A virus (A/Duck/Shantou/830/00(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339549|AF523450|	Influenza A virus (A/Duck/Shantou/1796/00(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339551|AF523451|	Influenza A virus (A/Duck/Shantou/2143/00(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339553|AF523452|	Influenza A virus (A/Duck/Shantou/2134/00(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339555|AF523453|	Influenza A virus (A/Duck/Shantou/2144/00(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339557|AF523454|	Influenza A virus (A/Wild Duck/Shantou/4808/01(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339559|AF523455|	Influenza A virus (A/Duck/Shantou/1881/00(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339561|AF523456|	Influenza A virus (A/Duck/Shantou/2102/00(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339563|AF523457|	Influenza A virus (A/Duck/Hong Kong/289/78(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339565|AF523458|	Influenza A virus (A/Duck/Hong Kong/610/79(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339567|AF523459|	Influenza A virus (A/Duck/Hong Kong/86/76(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|31339569|AF523460|	Influenza A virus (A/Duck/Hong Kong/366/78(H9N2))
  	polymerase (PA) gene, partial cds.
  gi|22759040|AF536669|	Influenza A virus (A/Chicken/Beijing/1/95(H9N2)) PA
  	gene, partial cds.
  gi|22759042|AF536670|	Influenza A virus (A/Chicken/Beijing/2/97(H9N2)) PA
  	gene, partial cds.
  gi|22759044|AF536671|	Influenza A virus (A/Chicken/Beijing/3/99(H9N2)) PA
  	gene, partial cds.
  gi|22759046|AF536672|	Influenza A virus (A/Chicken/Guangdong/97(H9N2)) PA
  	gene, partial cds.
  gi|22759048|AF536673|	Influenza A virus (A/Chicken/Hebei/1/96(H9N2)) PA
  	gene, partial cds.
  gi|22759050|AF536674|	Influenza A virus (A/Chicken/Hebei/2/98(H9N2)) PA
  	gene, partial cds.
  gi|22759052|AF536675|	Influenza A virus (A/Chicken/Hebei/3/98(H9N2)) PA
  	gene, partial cds.
  gi|22759054|AF536676|	Influenza A virus (A/Chicken/Henan/98(H9N2)) PA gene,
  	partial cds.
  gi|22759056|AF536677|	Influenza A virus (A/Chicken/Liaoning/99(H9N2)) PA
  	gene, partial cds.
  gi|22759058|AF536678|	Influenza A virus (A/Chicken/Shandong/98(H9N2)) PA
  	gene, partial cds.
  gi|12038897|AJ291397|	Influenza A virus (A/Chicken/Pakistan/2/99 (H9N2)) PA
  	gene for polymerase PA, genomic RNA.
  gi|18496121|AJ427863|	Influenza A virus (A/quail/Hong Kong/FY298/00 (H9N2))
  	partial pa gene for PA polymerase protein, genomic RNA
  gi|27465911|AY180650|	Influenza A virus strain A/Duck/Nanchang/11-392/2000
  	(H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465913|AY180651|	Influenza A virus strain A/Duck/Nanchang/11-290/2000
  	(H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465915|AY180652|	Influenza A virus strain A/Chicken/Nanchang/1-
  	0016/2000 (H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465917|AY180653|	Influenza A virus strain A/Duck/Nanchang/11-197/2000
  	(H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465937|AY180663|	Influenza A virus strain A/Pigeon/Nanchang/2-
  	0461/2000 (H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465941|AY180665|	Influenza A virus strain A/Chicken/Nanchang/4-
  	301/2001 (H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465943|AY180666|	Influenza A virus strain A/Chicken/Nanchang/4-
  	361/2001 (H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465961|AY180675|	Influenza A virus strain A/Wild Duck/Nanchang/2-
  	0480/2000 (H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465983|AY180686|	Influenza A virus strain A/Duck/Nanchang/1-0070/2000
  	(H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465989|AY180689|	Influenza A virus strain A/Duck/Nanchang/10-389/2000
  	(H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27465993|AY180691|	Influenza A virus strain A/Pigeon/Nanchang/11-
  	145/2000 (H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27466001|AY180695|	Influenza A virus strain A/Quail/Nanchang/2-0460/2000
  	(H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27466003|AY180696|	Influenza A virus strain A/Quail/Nanchang/4-040/2000
  	(H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27466009|AY180699|	Influenza A virus strain A/Chicken/Nanchang/4-
  	010/2000 (H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27466015|AY180702|	Influenza A virus strain A/Duck/Nanchang/7-092/2000
  	(H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|27466019|AY180704|	Influenza A virus strain A/Pigeon/Nanchang/7-058/2000
  	(H9N2) polymerase subunit PA (PA) gene, partial cds.
  gi|30025973|AY253752|	Influenza A virus (A/Chicken/Shanghai/F/98(H9N2))
  	polymerase acidic protein (PA) gene, complete cds.
  gi|49357051|AY633169|	Influenza A virus (A/mallard/Alberta/17/91(H9N2))
  	polymerase protein A (PA) gene, partial cds.
  gi|49357079|AY633281|	Influenza A virus (A/mallard/Alberta/321/88(H9N2))
  	polymerase protein A (PA) gene, partial cds.
  gi|49357083|AY633297|	Influenza A virus (A/mallard/Alberta/11/91(H9N2))
  	polymerase protein A (PA) gene, partial cds.
  gi|54301528|AY664755|	Influenza A virus
  	(A/chicken/HongKong/CSW153/03(H9N2)) polymerase acidic protein (PA) gene,
  	partial cds.
  gi|54301530|AY664756|	Influenza A virus (A/chicken/HongKong/AP45/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301532|AY664757|	Influenza A virus (A/chicken/HongKong/BD90/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301534|AY664758|	Influenza A virus
  	(A/chicken/HongKong/CSW291/03(H9N2)) polymerase acidic protein (PA) gene,
  	partial cds.
  gi|54301536|AY664759|	Influenza A virus
  	(A/chicken/HongKong/CSW304/03(H9N2)) polymerase acidic protein (PA) gene,
  	partial cds.
  gi|54301538|AY664760|	Influenza A virus (A/chicken/HongKong/FY23/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301540|AY664761|	Influenza A virus
  	(A/guineafowl/HongKong/NT101/03(H9N2)) polymerase acidic protein (PA) gene,
  	partial cds.
  gi|54301542|AY664762|	Influenza A virus (A/chicken/HongKong/NT142/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301544|AY664763|	Influenza A virus (A/chicken/HongKong/SF1/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301546|AY664764|	Influenza A virus
  	(A/chicken/HongKong/SSP101/03(H9N2)) polymerase acidic protein (PA) gene,
  	partial cds.
  gi|54301548|AY664765|	Influenza A virus (A/chicken/HongKong/TP38/03(H9N2))
  	polymerase acidic protein-like (PA) gene, complete sequence.
  gi|54301549|AY664766|	Influenza A virus (A/chicken/HongKong/WF126/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301551|AY664767|	Influenza A virus (A/pigeon/HongKong/WF53/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301553|AY664768|	Influenza A virus (A/pheasant/HongKong/WF54/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301555|AY664769|	Influenza A virus
  	(A/guineafowl/HongKong/NT184/03(H9N2)) polymerase acidic protein (PA) gene,
  	partial cds.
  gi|54301557|AY664770|	Influenza A virus (A/chicken/HongKong/WF120/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301559|AY664771|	Influenza A virus (A/chicken/HongKong/NT366/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|54301561|AY664772|	Influenza A virus
  	(A/chicken/HongKong/SSP418/03(H9N2)) polymerase acidic protein (PA) gene,
  	partial cds.
  gi|54301563|AY664773|	Influenza A virus (A/chicken/HongKong/YU427/03(H9N2))
  	polymerase acidic protein (PA) gene, partial cds.
  gi|55793682|AY800238|	Influenza A virus (A/chicken/Korea/S1/2003(H9N2))
  	polymerase acidic protein (PA) gene, complete cds.
  gi|58429718|AY862678|	Influenza A virus (A/silky chicken/Korea/S3/03(H9N2))
  	PA (PA) gene, partial cds.
  gi|58429720|AY862679|	Influenza A virus (A/chicken/Korea/S4/03(H9N2)) PA
  	(PA) gene, partial cds.
  gi|58429722|AY862680|	Influenza A virus (A/chicken/Korea/S5/03(H9N2)) PA
  	(PA) gene, complete cds.
  gi|58429724|AY862681|	Influenza A virus (A/chicken/Korea/S12/03(H9N2)) PA
  	(PA) gene, partial cds.
  gi|58429726|AY862682|	Influenza A virus (A/duck/Korea/S13/03(H9N2)) PA (PA)
  	gene, partial cds.
  gi|58429728|AY862683|	Influenza A virus (A/dove/Korea/S14/03(H9N2)) PA (PA)
  	gene, partial cds.
  gi|58429730|AY862684|	Influenza A virus (A/chicken/Korea/S15/03(H9N2)) PA
  	(PA) gene, partial cds.
  gi|58429732|AY862685|	Influenza A virus (A/chicken/Korea/S16/03(H9N2)) PA
  	(PA) gene, partial cds.
  gi|58429734|AY862686|	Influenza A virus (A/chicken/Korea/S18/03(H9N2)) PA
  	(PA) gene, partial cds.
  gi|5732356|AF156444|	Influenza A virus (A/Chicken/Hong Kong/G9/97(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732358|AF156445|	Influenza A virus (A/Chicken/Hong Kong/G23/97(H9N2))
  	segment 3 polymerase (PA) gene, complete cds.
  gi|5732360|AF156446|	Influenza A virus (A/Pigeon/Hong Kong/Y233/97(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732362|AF156447|	Influenza A virus (A/Duck/Hong Kong/Y280/97(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732364|AF156448|	Influenza A virus (A/Duck/Hong Kong/Y439/97(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732366|AF156449|	Influenza A virus (A/Quail/Hong Kong/G1/97 (H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732368|AF156450|	Influenza A virus (A/Chicken/Hong Kong/739/94(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732370|AF156451|	Influenza A virus (A/Quail/Hong Kong/AF157/92(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732372|AF156452|	Influenza A virus (A/Chicken/Beijing/1/94(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732374|AF156453|	Influenza A virus (A/Chicken/Korea/38349-
  	p96323/96(H9N2)) segment 3 polymerase (PA) gene, partial cds.
  gi|5732376|AF156454|	Influenza A virus (A/Chicken/Korea/25232-
  	96006/96(H9N2)) segment 3 polymerase (PA) gene, partial cds.
  gi|5732378|AF156455|	Influenza A virus (A/Shorebird/Delaware/9/96(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732380|AF156456|	Influenza A virus (A/Quail/Arkansas/29209-1/93(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|5732382|AF156457|	Influenza A virus (A/Turkey/California/189/66(H9N2))
  	segment 3 polymerase (PA) gene, partial cds.
  gi|12060671|AF222642|	Influenza A virus (A/Quail/Hong Kong/A17/99(H9N2))
  	segment 3 PA (PA) gene, partial cds.
  gi|12060673|AF222643|	Influenza A virus (A/Pigeon/Hong Kong/FY6/99(H9N2))
  	segment 3 PA (PA) gene, partial cds.
  gi|12060675|AF222644|	Influenza A virus (A/Chicken/Hong Kong/NT16/99(H9N2))
  	segment 3 PA (PA) gene, partial cds.
  gi|12060677|AF222645|	Influenza A virus (A/Quail/Hong Kong/SSP10/99(H9N2))
  	segment 3 PA (PA) gene, partial cds.
  gi|12060679|AF222646|	Influenza A virus (A/Pheasant/Hong
  	Kong/SSP11/99(H9N2)) segment 3 PA (PA) gene, partial cds.
  gi|12060681|AF222647|	Influenza A virus (A/Chicken/Hong Kong/FY20/99(H9N2))
  	segment 3 PA (PA) gene, partial cds.
  gi|12060683|AF222648|	Influenza A virus (A/Chicken/Hong Kong/KC12/99(H9N2))
  	segment 3 PA (PA) gene, partial cds.
  gi|12060685|AF222649|	Influenza A virus (A/Quail/Hong Kong/NT28/99(H9N2))
  	segment 3 PA (PA) gene, partial cds.
  gi|12060687|AF222650|	Influenza A virus (A/Chicken/Hong Kong/SF2/99(H9N2))
  	segment 3 PA (PA) gene, partial cds.
  gi|12060689|AF222651|	Influenza A virus (A/Silky Chicken/Hong
  	Kong/SF44/99(H9N2)) segment 3 PA (PA) gene, partial cds.

Claims (23)

1. An iRNA agent comprising a sense strand, wherein the sense strand comprises at least 15 contiguous nucleotides that differ by no more than 1, 2, or 3 nucleotides from the sense strand sequences of any one of the agents provided in Tables 1A-1H, agents numbered AL-DP-2241-AL-DP-8631, and an antisense strand, wherein the antisense strand comprises at least 15 contiguous nucleotides that differ by no more than 1, 2, or 3 nucleotides from the antisense sequences of any one of the agents provided in Tables 1A-1H, agents numbered AL-DP-2241-AL-DP-8631.

2. An iRNA agent including a sense strand, wherein the sense strand comprises at least 15 contiguous nucleotides that differ by no more than 1, 2, or 3 nucleotides from the sense strand sequences of any one of the agents provided in Tables 1A-1H, agents numbered AL-DP-2241-AL-DP-8631, and an antisense strand wherein the antisense strand comprises at least 15 contiguous nucleotides of the antisense sequences of any one of the agents provided in Tables 1A-1H, agents numbered AL-DP-2241-AL-DP-8631, and wherein the iRNA agent reduces the expression of its respective target gene in Cos-7 cells engineered to express the respective target gene by more than 20%, 30%, 40%, 50%, 60%, 70%, or 80% compared to cells which have not been incubated with the iRNA agent.

3. An iRNA agent comprising a sense strand and an antisense strand each comprising a sequence of at least 16, 17 or 18 nucleotides which is essentially identical to one of the sequences of any one of the agents provided in Tables 1A-1H, agents numbered AL-DP-2241-AL-DP-8631, except that not more than 1, 2 or 3 nucleotides per strand, respectively, have been substituted by other nucleotides (e.g. adenosine replaced by uracil), while essentially retaining the ability to reduce the amount of influenza A plaques formed in cells in a plaque forming assay.

4. The iRNA agent of claim 1, wherein the antisense RNA strand is 30 or fewer nucleotides in length, and the duplex region of the iRNA agent is 15-30 nucleotide pairs in length.

5. The iRNA agent of any of claim 1, comprising a modification that causes the iRNA agent to have increased stability in a biological sample.

6. The iRNA agent of claim 1, comprising a phosphorothioate or a 2′-modified nucleotide.

7. The iRNA agent of claim 1, comprising at least one 5′-uridine-adenine-3′ (5′-ua-3′) dinucleotide wherein the uridine is a 2′-modified nucleotide; at least one 5′-uridine-guanine-3′ (5′-ug-3′) dinucleotide, wherein the 5′-uridine is a 2′-modified nucleotide; at least one 5′-cytidine-adenine-3′ (5′-ca-3′) dinucleotide, wherein the 5′-cytidine is a 2′-modified nucleotide; or at least one 5′-uridine-uridine-3′ (5′-uu-3′) dinucleotide, wherein the 5′-uridine is a 2′-modified nucleotide.

8. The iRNA agent of claim 6, wherein the 2′-modification is selected from the group consisting of: 2′-deoxy, 2′-deoxy-2′-fluoro, 2′-O-methyl, 2′-O-methoxyethyl (2′-O-MOE), 2′-O-aminopropyl (2′-O-AP), 2′-O-dimethylaminoethyl (2′-O-DMAOE), 2′-O-dimethylaminopropyl (2′-O-DMAP), 2′-O-dimethylaminoethyloxyethyl (2′-O-DMAEOE), and 2′-O—N-methylacetamido (2′-O-NMA).

9. The iRNA agent of any of claim 1, comprising a nucleotide overhang having 1 to 4 unpaired nucleotides.

10. The iRNA agent of claim 9, wherein the nucleotide overhang has 2 or 3 unpaired nucleotides.

11. The iRNA agent of claim 9, wherein the nucleotide overhang is at the 3′-end of the antisense strand of the iRNA agent.

12. The iRNA agent of claim 1, comprising a cholesterol moiety.

13. The iRNA agent of claim 12, wherein the cholesterol moiety is conjugated to the 3′-end of the sense strand of the iRNA agent.

14. The iRNA agent of claim 1, wherein the iRNA agent is targeted for uptake by cells of the lung.

15. The iRNA agent of claim 1, wherein the iRNA agent comprises at least one non-natural nucleobase.

16. The iRNA agent of claim 15, wherein the non-natural nucleobase is difluorotolyl, nitroindolyl, nitropyrrolyl, or nitroimidazolyl.

17. The iRNA agent of claim 15, wherein the non-natural nucleobase is difluorotolyl.

18. The iRNA agent of claim 15, wherein only one of the two oligonucleotide strands comprising the double-stranded oligonucleotide contains a non-natural nucleobase.

19. The iRNA agent of claim 15, wherein both of the oligonucleotide strands comprising the double-stranded oligonucleotide independently contain a non-natural nucleobase.

20. A method of treating a human subject having a pathological process mediated in part by the replication of influenza A virus, wherein the iRNA agent comprises a sense strand wherein the sense strand comprises at least 15 contiguous nucleotides that differ by no more than 1, 2, or 3 nucleotides from the sense strand sequences any one of the agents provided in Tables 1A-1H, agents numbered AL-DP-2241-AL-DP-8631, and an antisense strand, wherein the antisense strand comprises at least 15 contiguous nucleotides that differ by no more than 1, 2, or 3 nucleotides from the antisense strand sequences of any one of the agents provided in Tables 1A-1H, agents numbered AL-DP-2241-AL-DP-8631.

21. The method of claim 20, wherein the iRNA agent is administered in an amount sufficient to reduce the replication of influenza virus in a cell or tissue of the subject.

22. The method of claim 20, wherein the subject is a human.

23. A pharmaceutical composition, comprising:

a.) an iRNA agent of claim 1; and

b.) a pharmaceutically acceptable carrier.

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