WO2003014316A2 - Immunomodulatory compositions, formulations, and methods for use thereof - Google Patents
Immunomodulatory compositions, formulations, and methods for use thereof Download PDFInfo
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- WO2003014316A2 WO2003014316A2 PCT/US2002/025123 US0225123W WO03014316A2 WO 2003014316 A2 WO2003014316 A2 WO 2003014316A2 US 0225123 W US0225123 W US 0225123W WO 03014316 A2 WO03014316 A2 WO 03014316A2
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Definitions
- Antigen immunotherapy for allergic disorders involves the subcutaneous injection of small, but gradually increasing amounts, of antigen.
- Such immunization treatments present the risk of inducing IgE-mediated anaphylaxis and do not efficiently address the cytokine-mediated events of the allergic late phase response. Thus far, this approach has yielded only limited success.
- WO 98/52962 has described three hexameric oligonucleotides, 5'-GACGTT-3', 5'-GAGCTT-3', and 5'-TCCGGA-3', which are stated to have immunostimulatory effects. Liang et al. (J. Clin. Invest. 98:1119-29, 1996) disclose that the motif (TCG) n , where n > 3, is a minimal stimulatory element for human cells. [0009] An ISS-containing 27 base oligonucleotide bound to microparticles
- the invention relates to new compositions and methods for modulating immune responses in individuals, especially human individuals.
- the invention relates to compositions which comprise immunomodulatory oligonucleotide/microcarrier (IMO/MC) complexes and encapsulates.
- IMO/MC immunomodulatory oligonucleotide/microcarrier
- the IMO/MC complexes and encapsulates of the invention comprise IMOs having the sequence 5'-X 1 TCGX 2 -3' or 5'-X 1 UCGX 2 -3', where X is zero or one nucleotide, and X 2 is zero to three nucleotides and the IMO is no longer than six nucleotides.
- the complex or encapsulate does not comprise a oligonucleotide greater than six nucleotides in length.
- the IMO may be covalently or non-covalently linked to the microcarrier in the complex, and the IMO may be modified to facilitate complex formation.
- infectious diseases which may be treated in accordance with the invention include infectious diseases caused by a cellular pathogen (e.g., a mycobacterial disease, malaria, leishmaniasis, toxoplasmosis, schistosomiasis or clonorchiasis), and may include or exclude viral diseases.
- a cellular pathogen e.g., a mycobacterial disease, malaria, leishmaniasis, toxoplasmosis, schistosomiasis or clonorchiasis
- infectious diseases caused by a cellular pathogen e.g., a mycobacterial disease, malaria, leishmaniasis, toxoplasmosis, schistosomiasis or clonorchiasis
- infectious diseases caused by a cellular pathogen (e.g., a mycobacterial disease, malaria, leishmaniasis, toxoplasmosis, schistosomiasis or clonorchiasis), and may include or exclude
- kits of the invention comprise a container comprising an IMO/MC complex or encapsulate and may also contain instructions for use of the IMO/MC complex or encapsulate in immunomodulation of an individual, for example when the individual suffers from a disorder associated with a Th2-type immune response (e.g., allergies or allergy-induced asthma), is receiving vaccines such as therapeutic vaccines (e.g. , vaccines comprising an allergy epitope, a mycobacterial epitope, or a tumor associated epitope) or prophylactic vaccines, suffers from cancer, suffers from an infectious disease or is at risk of exposure to an infectious agent.
- a Th2-type immune response e.g., allergies or allergy-induced asthma
- the invention provides compositions comprising antigen-free IMO/MC complexes or encapsulates, i.e., IMO/MC complexes or encapsulates neither linked to (directly or indirectly) nor mixed with an antigen.
- the invention provides compositions comprising IMO/MC complexes or encapsulates mixed with one or more antigens.
- the invention provides compositions comprising IMO/MC complexes or encapsulates linked to antigen.
- the IMO sequences preferentially activate a Thl -type response.
- An IMO is a 3- 6mer oligonucleotide having the sequence 5'-X 1 CGX 2 -3', where X ⁇ is zero to four nucleotides, X 2 is zero to four nucleotides and excludes the sequences 5'-GACGTT-3', 5'-TCCGGA-3', and 5'-GAGCTT-3'.
- Microcarriers for use in the instant invention may be biodegradable or nonbiodegradable.
- Biodegradable solid phase microcarriers may be formed from polymers which are degradable (e.g., poly (lactic acid), poly(glycolic acid) and copolymers thereof) or erodible (e.g., poly(ortho) esters such as 3,9-diethylidene- 2,4,8,10-tetraoxaspiro[5.5]undecane (DETOSU), polymethylidene malonate, or poly(anhydrides), such as poly(anhydrides) of sebacic acid) under mammalian physiological conditions.
- degradable e.g., poly (lactic acid), poly(glycolic acid) and copolymers thereof
- erodible e.g., poly(ortho) esters such as 3,9-diethylidene- 2,4,8,10-tetraoxaspiro[5.5]undecane (DETOSU
- liquid phase microcarriers such as liposomes, ISCOMs (immune-stimulating complexes, which are stable complexes of cholesterol, phospholipid, and adjuvant-active saponin) without antigen, or droplets or micelles found in oil in water or water in oil emulsions, provided the liquid phase microcarriers are biodegradable.
- Biodegradable liquid phase microcarriers typically incorporate a biodegradable oil, a number of which are known in the art, including squalene and vegetable oils.
- Microcarriers are typically spherical in shape, but microcarriers which deviate from spherical shape are also acceptable (e.g., ellipsoid, rod-shaped, etc.). Due to their insoluble nature (with respect to water), microcarriers are filterable from water and water-based (aqueous) solutions.
- the "size" of a microcarrier is generally the "design size” or intended size of the particles stated by the manufacturer. Size may be a directly measured dimension, such as average or maximum diameter, or may be determined by an indirect assay such as a filtration screening assay. Direct measurement of microcarrier size is typically carried out by microscopy, generally light microscopy or scanning electron microscopy (SEM), in comparison with particles of known size or by reference to a micrometer. As minor variations in size arise during the manufacturing process, microcarriers are considered to be of a stated size if measurements show the microcarriers are + about 5-10% of the stated measurement. Size characteristics may also be determined by dynamic light scattering or obscuration techniques.
- the term "desensitization” refers to the process of the administration of increasing doses of an allergen to which the subject has demonstrated sensitivity.
- allergen doses used for desensitization are known in the art, see, for example, Fornadley (1998) Otolaryngol. Clin. North Am. 31:111-127.
- the IMO is a pentamer (5mer) having a sequence according to the formula 5'-X 1 TCGX 2 -3' or 5'-XiUCGX 2 -3' where X ! is A, C, G, T, U, or I and X 2 is A, C, G, T, U, or I, or according to the formula 5'-TCGX 3 -3' or 5'-UCGX 3 -3' where X 3 is AA, AC, AG, AT, AU, Al, CA, CC, CG, CT, CU, Cl, GA, GC, GG, GT, GU, GI, TA, TC, TG, TT, TU, TI, UA, UC, UG, UT, UU, UI, IA, IC, IG, IT, IU, or II.
- the link between the IMO and MC portions of the complex can be made at the 3' or 5' end of the IMO, or at a suitably modified base at an internal position in the IMO.
- the microcarrier is generally also modified to incorporate moieties through which a covalent link may be formed, although functional groups normally present on the microcarrier may also be utilized.
- the IMO/MC is formed by incubating the IMO with a microcarrier under conditions which permit the formation of a covalent complex (e.g., in the presence of a crosslinking agent or by use of an activated microcarrier comprising an activated moiety which will form a covalent bond with the IMO).
- Heterobifunctional crosslinkers utilize different moieties on the IMO and MC, (e.g., a maleimido-N-hydroxysuccinimide ester may be used to covalently link a free sulfhydryl on the IMO and a free amine on the MC), and are preferred to minimize formation of inter-microcarrier bonds. In most cases, it is preferable to crosslink through a first crosslinking moiety on the microcarrier and a second crosslinking moiety on the IMO, where the second crosslinking moiety is not present on the microcarrier.
- Non-covalent IMO/MC complexes are typically complexed by hydrophobic or electrostatic (ionic) interactions, or a combination thereof. Due to the hydrophilic nature of the backbone of polynucleotides, IMO/MC complexes which rely on hydrophobic interactions to form the complex generally require modification of the IMO portion of the complex to incorporate a highly hydrophobic moiety.
- the hydrophobic moiety is biocompatible, nonimmunogenic, and is naturally occurring in the individual for whom the composition is intended (e.g., is found in mammals, particularly humans). Examples of hydrophobic moieties include lipids, steroids, sterols such as cholesterol, and terpenes.
- microcarriers for use in IMO/MC complexes linked by hydrophobic bonding are made from hydrophobic materials, such as oil droplets or hydrophobic polymers, although hydrophilic materials modified to incorporate hydrophobic moieties may be utilized as well.
- the microcarrier is a liposome or other liquid phase microcarrier comprising a lumen
- the IMO/MC complex is formed by mixing the IMO and the MC after preparation of the MC, in order to avoid encapsulation of the IMO during the MC preparation process.
- Non-covalent IMO/MC complexes bound by electrostatic binding typically exploit the highly negative charge of the polynucleotide backbone.
- microcarriers may comprise a positively charged moiety.
- this portion of the conjugate can be attached to the 3 '-end of the IMO through solid support chemistry.
- the IMO portion can be added to a polypeptide portion that has been pre-synthesized on a support. Haralambidis et al. (1990a) Nucleic Acids Res. 18:493-499; and Haralambidis et al. (1990b) Nucleic Acids Res. 18:501-505.
- the IMO can be synthesized such that it is connected to a solid support through a cleavable linker extending from the 3 '-end.
- an IMO is encapsulated within a microcarrier ("IMO/MC encapsulate"), and preferably multiple molecules of IMO are encapsulated within each microcarrier.
- a mixture of different IMOs may be encapsulated with a microcarrier, such that the microcarrier encapsulates more than one IMO species.
- the IMO is a 3mer, 4mer or 5mer (3-5mer).
- the IMO may be any 6-mer described herein excluding the sequences 5'-TTCGAA-3', 5'-GACGTT-3', and/or 5'-GAGCTT-3', for example, the 6-mer IMO has the sequence 5'-X 1 TCGX 2 -3' or 5'-X 1 UCGX 2 -3', where X x is zero or one nucleotide, and X 2 is zero to three nucleotides. Additional examples of IMOs which may be utilized in IMO/MC encapsulates are described above.
- the invention provides methods of modulating an immune response in an individual, preferably a mammal, more preferably a human, comprising administering to the individual an IMO/MC complex or encapsulate (typically in a composition comprising the complex or encapsulate and a pharmaceutically acceptable excipient) such that the desired modulation of the immune response is achieved.
- Immunomodulation may include stimulating a Thl -type immune response and/or inhibiting or reducing a Th2-type immune response.
- the immune modulation comprises stimulating a (i.e. , one or more) Thl -associated cytokine, such as IFN- ⁇ , IL-12 and/or IFN- ⁇ .
- the immune modulation comprises suppressing production of a (t ' .e., one or more) Th2-associated cytokine, such as IL-4 and/or IL-5. Measuring these parameters uses methods standard in the art and has been discussed herein.
- administration of IMO/MC may further comprise administration of one or more additional immunotherapeutic agents (i.e., an agent which acts via the immune system and/or is derived from the immune system) including, but not limited to, cytokine, adjuvants and antibodies.
- additional immunotherapeutic agents i.e., an agent which acts via the immune system and/or is derived from the immune system
- therapeutic- antibodies include those used in the cancer context (e.g. , anti-tumor antibodies).
- Administration of such additional immunotherapeutic agents applies to all the methods described herein.
- administration of IMO/MC complex or encapsulate may further comprise administration of one or more additional therapeutic agents such as, for example, anti- tumor antibodies, chemotherapy regimens and/or radiation treatments.
- Anti-tumor antibodies including, but not limited to anti-tumor antibody fragments and/or derivatives thereof, and monoclonal anti-tumor antibodies, fragments and/or derivatives thereof, are known in the art and as is administration of such antibody reagents in cancer therapy (e.g., Rituximab; Herceptin). Administration of one or more additional therapeutic agents may occur before, after and/or concurrent with administration of the IMO/MC complexes or encapsulates.
- the antigen(s) of the vaccine is part of the IMO/MC complex or encapsulate, by either covalent or non-covalent linkage to the IMO/MC complex or encapsulate.
- Administration of IMO/MC complex or encapsulate therapy to an individual receiving a vaccine results in an immune response to the vaccine that is shifted towards a Thl -type response as compared to individuals which receive vaccine without IMO/MC complex or encapsulate.
- Shifting towards a Thl -type response may be recognized by a delayed-type hypersensitivity (DTH) response to the antigen(s) in the vaccine, increased IFN- ⁇ and other Thl -type response associated cytokines, increased IFN- ⁇ , production of CTLs specific for the antigen(s) of the vaccine, low or reduced levels of IgE specific for the antigen(s) of the vaccine, a reduction in Th2- associated antibodies specific for the antigen(s) of the vaccine, and/or an increase in Thl- associated antibodies specific for the antigen(s) of the vaccine.
- DTH delayed-type hypersensitivity
- administration of IMO/MC complex or encapsulate and vaccine also results in amelioration of the symptoms of the disorder which the vaccine is intended to treat.
- the exact symptoms and manner of their improvement will depend on the disorder sought to be treated.
- the therapeutic vaccine is for tuberculosis
- IMO/MC complex or encapsulate treatment with vaccine results in reduced coughing, pleural or chest wall pain, fever, and/or other symptoms known in the art.
- the vaccine is an allergen used in allergy desensitization therapy
- the treatment results in a reduction in one or more symptoms of allergy (e.g., reduction in rhinitis, allergic conjunctivitis, circulating levels of IgE, and/or circulating levels of histamine).
- the invention provides methods of increasing IFN- ⁇ in an individual, particularly in an individual in need of increased IFN- ⁇ levels, by administering an effective amount of an IMO/MC complex or encapsulate to the individual.
- Individuals in need of increased IFN- ⁇ are those having disorders which respond to the administration of IFN- ⁇ .
- Such disorders include a number of inflammatory disorders including, but not limited to, ulcerative colitis.
- the invention provides methods of increasing IFN- ⁇ in an individual, particularly in an individual in need of increased IFN- ⁇ levels, by administering an effective amount of an IMO/MC complex or encapsulate to the individual such that IFN- ⁇ levels are increased.
- Individuals in need of increased IFN- ⁇ are those having disorders which respond to the administration of IFN- ⁇ , including recombinant IFN- ⁇ , including, but not limited to, viral infections and cancer.
- Reduction in IgE results in an amelioration of symptoms of the IgE-related disorder.
- symptoms include allergy symptoms such as rhinitis, conjunctivitis, in decreased sensitivity to allergens, a reduction in the symptoms of allergy in an individual with allergies, or a reduction in severity of a allergic response.
- IMO/MC complex or encapsulate therapy may be administered in conjunction with anti-malarial drugs such as chloroquine for malaria patients, in conjunction with leishmanicidal drugs such as pentamidine and/or allopurinol for leishmaniasis patients, in conjunction with anti- mycobacterial drugs such as isoniazid, rifampin and/or ethambutol in tuberculosis patients, or in conjunction with allergen desensitization therapy for atopic (allergy) patients.
- anti-malarial drugs such as chloroquine for malaria patients
- leishmanicidal drugs such as pentamidine and/or allopurinol for leishmaniasis patients
- anti- mycobacterial drugs such as isoniazid, rifampin and/or ethambutol in tuberculosis patients
- allergen desensitization therapy for atopic (allergy) patients.
- the IMO/MC complex or encapsulate can be administered in combination with other pharmaceutical and/or immunogenic and/or immunostimulatory agents and can be combined with a physiologically acceptable carrier thereof.
- the IMO/MC complex or encapsulate can be administered in conjunction with other immunotherapeutic agents including, but not limited to, cytokine, adjuvants and antibodies.
- the IMO/MC complex or encapsulate may comprise any combination of the IMOs and MCs described above, so long as the IMO/MC is active.
- an IMO/MC complex or encapsulate will be considered active if it has an activity (i.e., affects a measurable immune response as measured in vitro, in vivo and/or ex vivo) of at least two times, preferably at least three times, more preferably at least five times, even more preferably ten times the activity of a negative control in at least one assay of activity.
- an activity i.e., affects a measurable immune response as measured in vitro, in vivo and/or ex vivo
- Methods of assessing a measurable immune response are well known in the art, and include the human PBMC assay disclosed herein.
- the immunologically effective amounts and method of administration of the particular IMO/MC complex or encapsulate formulation can vary based on the individual, what condition is to be treated and other factors evident to one skilled in the art. Factors to be considered include the antigenicity, whether or not the IMO/MC complex or encapsulate will be administered with or covalently attached to an adjuvant or delivery molecule, route of administration and the number of immunizing doses to be administered. Such factors are known in the art and it is well within the skill of those in the art to make such determinations without undue experimentation.
- a suitable dosage range is one that provides the desired modulation of immune response to the antigen.
- Preferred routes of dermal administration are those which are least invasive. Preferred among these means are transdermal transmission, epidermal administration and subcutaneous injection. Of these means, epidermal administration is preferred for the greater concentrations of APCs expected to be in intradermal tissue.
- Transdermal administration is accomplished by application of a cream, rinse, gel, etc. capable of allowing the IMO/MC complex or encapsulate to penetrate the skin and enter the blood stream.
- Compositions suitable for transdermal administration include, but are not limited to, pharmaceutically acceptable suspensions, oils, creams and ointments applied directly to the skin or incorporated into a protective carrier such as a transdermal device (so-called "patch"). Examples of suitable creams, ointments etc. can be found, for instance, in the Physician's Desk Reference.
- iontophoresis is a suitable method. Iontophoretic transmission can be accomplished using commercially available patches which deliver their product continuously through unbroken skin for periods of several days or more. Use of this method allows for controlled transmission of pharmaceutical compositions in relatively great concentrations, permits infusion of combination drugs and allows for contemporaneous use of an absorption promoter.
- Gastrointestinal routes of administration include, but are not limited to, ingestion and rectal.
- the invention includes IMO/MC complex or encapsulate formulations suitable for gastrointestinal administration including, but not limited to, pharmaceutically acceptable powders, pills or liquids for ingestion and suppositories for rectal administration.
- pills or suppositories will further comprise pharmaceutically acceptable solids, such as starch, to provide bulk for the composition.
- Naso-pharyngeal and pulmonary administration include are accomplished by inhalation, and include delivery routes such as intranasal, transbronchial and transalveolar routes.
- the invention includes IMO/MC complex or encapsulate formulations suitable for administration by inhalation including, but not limited to, liquid suspensions for forming aerosols as well as powder forms for dry powder inhalation delivery systems.
- Devices suitable for administration by inhalation of IMO/MC complex or encapsulate formulations include, but are not limited to, atomizers, vaporizers, nebulizers, and dry powder inhalation delivery devices.
- Th2-type biased cytokines refers to those associated with a Th2-type immune response, and include, but are not limited to, IL-4, IL-5, and IL-13.
- Cells useful for the determination of IMO/MC complex or encapsulate activity include cells of the immune system, primary cells isolated from a host and/or cell lines, preferably APCs and lymphocytes, even more preferably macrophages and T cells.
- Stimulating a Thl -type immune response can also be measured in a host treated with an IMO/MC complex or encapsulate formulation can be determined by any method known in the art including, but not limited to: (1) a reduction in levels of IL-4 or IL-5 measured before and after antigen-challenge; or detection of lower (or even absent) levels of IL-4 or IL-5 in an IMO/MC complex or encapsulate treated host as compared to an antigen-primed, or primed and challenged, control treated without IMO; (2) an increase in levels of IL-12, IL-18 and/or IFN ( ⁇ , ⁇ or ⁇ ) before and after antigen challenge; or detection of higher levels of IL-12, IL-18 and/or IFN ( ⁇ , ⁇ or ⁇ ) in an IMO/MC complex or encapsulate treated host as compared to an antigen-primed or, primed and challenged, control treated without IMO; (3) "Thl -type biased" antibody production in an IMO/MC complex or
- a variety of these determinations can be made by measuring cytokines made by APCs and/or lymphocytes, preferably macrophages and/or T cells, in vitro or ex vivo using methods described herein or any known in the art. Some of these determinations can be made by measuring the class and/or subclass of antigen-specific antibodies using methods described herein or any known in the art.
- Thl -type biased antibody production refers to the measurable increased production of antibodies associated with a Thl -type immune response (i.e., Thl -associated antibodies).
- Thl associated antibodies may be measured.
- Thl -type biased antibodies include, but are not limited to, human IgGl and/or IgG3 (see, e.g., Widhe et al. (1998) Scand. J. Immunol. 47:575-581 and de Martino et al.
- Th2-type biased antibodies refers to those associated with a Th2-type immune response, and include, but are not limited to, human IgG2, IgG4 and/or IgE (see, e.g., Widhe et al. (1998) and de Martino et al. (1999)) and murine IgGl and/or
- Kits which comprise materials for production of IMO/MC complex or encapsulate generally include separate containers of IMO and MC, although in certain, embodiments materials for producing the MC (particularly for IMO/MC encapsulates) are supplied rather than preformed MC.
- the IMO and MC are preferably supplied in a form which allows formation of IMO/MC complex or encapsulate upon mixing of the supplied IMO and MC. This configuration is preferred when the IMO/MC complex is linked by non-covalent bonding or when an IMO/MC encapsulate is desired.
- Oligonucleotides containing phosphodiester linkages (e.g., 6-12) were synthesized on a Perseptive Biosystems Expedite 8909 automated DNA synthesizer.
- the manufacturer's protocol for 15 umol phosphodiester DNA was used with the following changes: 1.6 ml of 3% dichloroacetic acid in dichloromethane over 2.5 min was used for the detritylation step; and 3.0 ml of oxidation reagent over 1.1 min followed by a 1.0 ml delivery over 1.0 min was used for the oxidation step.
- the nucleoside phosphoramidite monomers were dissolved in anhydrous acetonitrile to a concentration of 0.1 M.
- the instrument was programmed to add the nucleotide monomers in the desired order, with the synthesis occurring in the 3' to 5' direction.
- the synthesis cycle consisted of a detritylation step, a coupling step (phosphoramidite monomer plus lH-tetrazole), a capping step, an oxidation step, and a final capping step.
- IMOs were purified by RP-HPLC on a Polymer Labs PLRP-S column using an increasing gradient of acetonitrile in 0.1 M triethylammonium acetate.
- the purified IMOs were concentrated to dryness, the 4,4 , -dimethoxytrityl group was removed with 80% aqueous acetic acid, and then the compound was precipitated two times from 0.6 M aqueous sodium acetate/pH 5.0 with 3 volumes of isopropanol.
- the IMOs were dissolved in Milli Q water and the yield was determined from the absorbance at 260 nm. Finally, the IMOs were lyophilized to a powder.
- Cationic poly(lactic acid, glycolic acid) microspheres were prepared as follows. 0.875 g of poly (D,L-lactide-co-glycolide) 50:50 polymer with an intrinsic viscosity of 0.41 dl/g (0.1%, chloroform, 25 °C) was dissolved in 7.875 g of methylene chloride at 10% w/w concentration, along with 0.3 g of DOTAP. The clear organic phase was then emulsified into 500 ml of PVA aqueous solution (0.35% w/v) by homogenization at 4000 ⁇ m for 30 minutes at room temperature using a laboratory mixer (Silverson L4R, Silverson Instruments).
- System temperature was then raised to 40 °C by circulating hot water through the jacket of the mixing vessel. Simultaneously, the stirring rate was reduced to 1500 ⁇ m, and these conditions were maintained for 2 hours to extract and evaporate methylene chloride. The microsphere suspension was allowed to cool down to room temperature with the help of circulating cold water.
- the cells were resuspended and cultured in 48 well plates at 2 x 10 6 cells/mL at 37°C in RPMI 1640 with 10%> heat-inactivated human AB serum plus 50 units/mL penicillin, 50 ⁇ g/mL streptomycin, 300 ⁇ g/mL glutamine, 1 mM sodium pyruvate, and 1 x MEM non-essential amino acids (NEAA).
- Oligonucleotides were tested as single agents, or in combination with PLGA microspheres (unmodified or cationic). All oligonucleotides contained 100% phosphorothioate linkages and were tested at 20 ⁇ g/ml. The PLGA microcarriers were used at 250 ⁇ g/ml. When oligos were tested with PLGA microcarriers, the oligo and the microcarriers were added at the same time to the culture. The cells were cultured in the in the presence of test samples for 24 hours, then cell-free medium was collected from each well and assayed for IFN- ⁇ and IFN- ⁇ concentration. Two different oligonucleotides were used as controls: a first oligonucleotide known to have immunostimulatory activity (a 22mer oligonucleotide containing an ISS ("ISS+,"
- IFN- ⁇ and IFN- ⁇ were assayed using CYTOSCREENTM ELISA kits from BioSource International, Inc., according to the manufacturer's instructions.
- background levels of IFN- ⁇ can vary, even significantly, with the donor. Levels of IFN- ⁇ , however, demonstrate a generally stable pattern of activation and routinely exhibit low background levels under unstimulated conditions.
- Oligonucleotides 6-6 (5'-TCGAGA-3'), 6-
- oligonucleotides that contain the consensus sequence 5'-X 1 TCGX 2 -3', where the oligonucleotide is a hexamer or pentamer and Xi is 0-1 nucleotides and X 2 is 2-3 nucleotides, were highly active when delivered as IMO/MC complexes, while they were inactive when delivered alone (6-6, 6-1, 6-7, 6-8, 6-9, 6-2, 6-3, 5-1, and 5-2).
- Oligonucleotides 6-16 and 6-4 do not fit this consensus sequence, and exhibited variable activity in the assay.
- Oligonucleotides were tested for immunomodulatory activity in the human PBMC assay. Oligonucleotides were tested alone or in combination with cPLGA as described in Example 5.
- Table 8 also shows that pentameric oligonucleotides fitting the consensus sequence XiTCGX 2 , where Xi is zero or one nucleotide and X 2 is one to two nucleotides, are active in combination with cPLGA. Oligonucleotides 5-2 and 5- 3 were each active in two of four donors when combined with cPLGA.
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CA2456328C (en) | 2015-05-26 |
JP4607452B2 (en) | 2011-01-05 |
JP2005527465A (en) | 2005-09-15 |
US8586555B2 (en) | 2013-11-19 |
US20100291218A1 (en) | 2010-11-18 |
WO2003014316A3 (en) | 2004-03-11 |
CA2456328A1 (en) | 2003-02-20 |
EP1420829A4 (en) | 2006-05-17 |
US20030133988A1 (en) | 2003-07-17 |
AU2002326561B2 (en) | 2008-04-03 |
EP1420829A2 (en) | 2004-05-26 |
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