WO2008021928A2 - Hepatitis c virus inhibitors - Google Patents

Hepatitis c virus inhibitors Download PDF

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Publication number
WO2008021928A2
WO2008021928A2 PCT/US2007/075545 US2007075545W WO2008021928A2 WO 2008021928 A2 WO2008021928 A2 WO 2008021928A2 US 2007075545 W US2007075545 W US 2007075545W WO 2008021928 A2 WO2008021928 A2 WO 2008021928A2
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WO
WIPO (PCT)
Prior art keywords
imidazol
pyrrolidinyl
phenyl
mmol
methyl
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Ceased
Application number
PCT/US2007/075545
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English (en)
French (fr)
Other versions
WO2008021928A3 (en
Inventor
Carol Bachand
Makonen Belema
Daniel H. Deon
Andrew C. Good
Jason Goodrich
Clint A. James
Rico Lavoie
Omar D. Lopez
Alain Martel
Nicholas A. Meanwell
Van N. Nguyen
Jeffrey Lee Romine
Edward H. Ruediger
Lawrence B. Snyder
Denis R. St. Laurent
Fukang Yang
David R. Langley
Lawrence G. Hamann
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Bristol Myers Squibb Co
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Bristol Myers Squibb Co
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Filing date
Publication date
Priority to AU2007286223A priority Critical patent/AU2007286223B2/en
Priority to AT07813923T priority patent/ATE547103T1/de
Priority to NZ574769A priority patent/NZ574769A/en
Priority to JP2009524737A priority patent/JP5306203B2/ja
Priority to CA2660628A priority patent/CA2660628C/en
Priority to ES07813923T priority patent/ES2382005T3/es
Priority to KR1020097004995A priority patent/KR101438851B1/ko
Priority to HK09104398.1A priority patent/HK1125576B/en
Priority to MX2009001436A priority patent/MX2009001436A/es
Priority to EA200900297A priority patent/EA017348B1/ru
Priority to CN200780037399.9A priority patent/CN101528232B/zh
Priority to EP07813923A priority patent/EP2049116B1/en
Application filed by Bristol Myers Squibb Co filed Critical Bristol Myers Squibb Co
Priority to BRPI0716220-0A2A priority patent/BRPI0716220A2/pt
Publication of WO2008021928A2 publication Critical patent/WO2008021928A2/en
Publication of WO2008021928A3 publication Critical patent/WO2008021928A3/en
Priority to NO20090453A priority patent/NO20090453L/no
Priority to IL196815A priority patent/IL196815A/en
Anticipated expiration legal-status Critical
Ceased legal-status Critical Current

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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D401/00Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom
    • C07D401/14Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing three or more hetero rings
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/495Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with two or more nitrogen atoms as the only ring heteroatoms, e.g. piperazine or tetrazines
    • A61K31/505Pyrimidines; Hydrogenated pyrimidines, e.g. trimethoprim
    • A61K31/506Pyrimidines; Hydrogenated pyrimidines, e.g. trimethoprim not condensed and containing further heterocyclic rings
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P1/00Drugs for disorders of the alimentary tract or the digestive system
    • A61P1/16Drugs for disorders of the alimentary tract or the digestive system for liver or gallbladder disorders, e.g. hepatoprotective agents, cholagogues, litholytics
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P31/00Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics
    • A61P31/12Antivirals
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P31/00Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics
    • A61P31/12Antivirals
    • A61P31/14Antivirals for RNA viruses
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P31/00Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics
    • A61P31/12Antivirals
    • A61P31/14Antivirals for RNA viruses
    • A61P31/18Antivirals for RNA viruses for HIV
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P31/00Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics
    • A61P31/12Antivirals
    • A61P31/20Antivirals for DNA viruses
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P43/00Drugs for specific purposes, not provided for in groups A61P1/00-A61P41/00
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D403/00Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, not provided for by group C07D401/00
    • C07D403/14Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, not provided for by group C07D401/00 containing three or more hetero rings

Definitions

  • the present disclosure is generally directed to antiviral compounds, and more specifically directed to compounds which can inhibit the function of the NS5A protein encoded by Hepatitis C virus (HCV), compositions comprising such compounds, and methods for inhibiting the function of the NS5A protein.
  • HCV Hepatitis C virus
  • HCV is a major human pathogen, infecting an estimated 170 million persons worldwide - roughly five times the number infected by human immunodeficiency virus type 1. A substantial fraction of these HCV infected individuals develop serious progressive liver disease, including cirrhosis and hepatocellular carcinoma.
  • HCV Hepatitis C virus
  • the most effective HCV therapy employs a combination of alpha- interferon and ribavirin, leading to sustained efficacy in 40% of patients.
  • HCV is a positive-stranded RNA virus. Based on a comparison of the deduced amino acid sequence and the extensive similarity in the 5' untranslated region, HCV has been classified as a separate genus in the Flaviviridae family. All members of the Flaviviridae family have enveloped virions that contain a positive stranded RNA genome encoding all known virus-specific proteins via translation of a single, uninterrupted, open reading frame.
  • HCV RNA genome is approximately 9500 nucleotides in length and has a single open reading frame (ORF) encoding a single large polyprotein of about 3000 amino acids. In infected cells, this polyprotein is cleaved at multiple sites by cellular and viral proteases to produce the structural and non-structural (NS) proteins.
  • ORF open reading frame
  • NS2, NS3, NS4A, NS4B, NS5A, and NS5B are effected by two viral proteases.
  • the first one is believed to be a metalloprotease and cleaves at the NS2-NS3 junction; the second one is a serine protease contained within the N-terminal region of NS3 (also referred to herein as NS3 protease) and mediates all the subsequent cleavages downstream of NS3, both in cis, at the NS3-NS4A cleavage site, and in trans, for the remaining NS4A-NS4B, NS4B-NS5A, NS5A-NS5B sites.
  • the NS4A protein appears to serve multiple functions, acting as a cofactor for the NS3 protease and possibly assisting in the membrane localization of NS3 and other viral replicase components.
  • the complex formation of the NS3 protein with NS4A seems necessary to the processing events, enhancing the proteolytic efficiency at all of the sites.
  • the NS3 protein also exhibits nucleoside triphosphatase and RNA helicase activities.
  • NS5B (also referred to herein as HCV polymerase) is a RNA-dependent RNA polymerase that is involved in the replication of HCV.
  • HCV NS5A protein is described, for example, in Tan, S. -L., Katzel, M.G. Virology 2001, 284, 1- 12; and in Park, K. -J.; Choi, S.-H, J. Biological Chemistry 2003.
  • a and B are selected from phenyl and a six-membered heteroaromatic ring containing one, two, or three nitrogen atoms; provided that at least one of A and B is other than phenyl;
  • X is selected from O, S, S(O), SO 2 , CH 2 , CHR 5 , and C(R 5 ) 2 ; provided that when n is O, X is selected from CH 2 , CHR 5 , and C(R 5 ) 2 ;
  • Y is selected from O, S, S(O), SO 2 , CH 2 , CHR 6 , and C(R 6 ) 2 ; provided that when m is O, Y is selected from CH 2 , CHR 6 , and C(R 6 ) 2 ; each R 1 and R 2 is independently selected from alkoxy, alkoxyalkyl, alkoxycarbonyl, alkyl, arylalkoxycarbonyl, carboxy, formyl, halo, haloalkyl, hydroxy, hydroxyalkyl, -NR a R b , (NR a R b )alkyl, and (NR a R b )carbonyl;
  • R 3 and R 4 are each independently selected from hydrogen, R 9 -C(O)-, and R 9 - C(S)-; each R 5 and R 6 is independently selected from alkoxy, alkyl, aryl, halo, haloalkyl, hydroxy, and -NR a R , wherein the alkyl can optionally form a fused three- to six-membered ring with an adjacent carbon atom, wherein the three- to six- membered ring is optionally substituted with one or two alkyl groups;
  • R 7 and R 8 are each independently selected from hydrogen, alkoxycarbonyl, alkyl, arylalkoxycarbonyl, carboxy, haloalkyl, (NR a R )carbonyl, and trialkylsilylalkoxyalkyl; and each R 9 is independently selected from alkoxy, alkoxyalkyl, alkoxycarbonyl, alkoxycarbonylalkyl, alkyl, alkylcarbonylalkyl, aryl, arylalkenyl, arylalkoxy, arylalkyl, aryloxyalkyl, cycloalkyl, (cycloalkyl)alkenyl, (cycloalkyl)alkyl, cycloalkyloxyalkyl, haloalkyl, heterocyclyl, heterocyclylalkenyl, heterocyclylalkoxy, heterocyclylalkyl, heterocyclyloxyalkyl, hydroxyalkyl, -NR c R d
  • m and n are each 1.
  • u and v are each independently 0 or 1; and each R 1 and R 2 is independently selected from alkyl and halo.
  • u and v are each independently 0 or 1; and when present, R 1 and/or R 2 are halo.
  • the halo is fluoro.
  • X is selected from CH 2 , CHR 5 , and C(R 5 ) 2 ; and Y is selected from CH 2 , CHR 6 , and C(R 6 ) 2 .
  • R 7 and R 8 are independently selected from hydrogen, haloalkyl, and trialkylsilylalkoxyalkyl. In a seventh embodiment of the first aspect R 7 and R 8 are each hydrogen.
  • q and s are independently 0, 1, or 2; and when present, R 5 and/or R 6 are halo. In a ninth embodiment of the first aspect each halo is fluoro.
  • At least one of R 3 and R 4 is hydrogen.
  • R 3 and R 4 are each R 9 -C(O)-.
  • each R 9 is independently selected from alkoxy, alkoxyalkyl, alkyl, alkylcarbonylalkyl, aryl, arylalkenyl, arylalkoxy, arylalkyl, aryloxyalkyl, cycloalkyl, (cycloalkyl)alkyl, cycloalkyloxyalkyl, heterocyclyl, heterocyclylalkyl, hydroxyalkyl, -NR c R d , (NR c R d )alkenyl,
  • each R 9 is independently selected from alkoxy, arylalkyl, (cycloalkyl)alkyl, heterocyclyl, heterocyclylalkyl, and (NR C R )alkyl.
  • X is selected from CH 2 , CHR 5 and C(R 5 ) 2 ;
  • Y is selected from CH 2 , CHR 6 , and C(R 6 ) 2 ; when present, R 1 and/or R 2 are halo, wherein each halo is fluoro;
  • R 3 and R 4 are each R 9 -C(O)-; when present, R 5 and/or R 6 are halo, wherein each halo is fluoro; and each R 9 is independently selected from alkoxy, alkoxyalkyl, alkoxycarbonyl, alkoxycarbonylalkyl, alkyl, alkylcarbonylalkyl, aryl, arylalkenyl, arylalkoxy, arylalkyl, aryloxyalkyl, cycloalkyl, (cycloalkyl)alkenyl, (cycloalkyl)alkyl, cycloalkyloxyalkyl, haloalkyl, heterocyclyl, heterocyclylalkenyl, heterocyclylalkoxy, heterocyclylalkyl, heterocyclyloxyalkyl, hydroxyalkyl, -NR c R d , (NR c R d )alkenyl, (NR c R d )al
  • a and B are selected from phenyl and a six-membered heteroaromatic ring containing one or two nitrogen atoms; provided that at least one of A and B is other han phenyl; each R 1 and R 2 is independently selected from alkyl and halo; R 3 and R 4 are each independently selected from hydrogen and R 9 -C(O)-; R 7 and R 8 are each independently selected from hydrogen, haloalkyl, and trialkylsilylalkoxyalkyl; and each R 9 is independently selected from alkoxy, arylalkyl, (cycloalkyl)alkyl, heterocyclyl, heterocyclylalkyl, and (NR C R )alkyl.
  • the present disclosure provides a composition comprising a compound of Formula (I), or a pharmaceutically acceptable salt thereof, and a pharmaceutically acceptable carrier.
  • the composition further comprises one or two additional compounds having anti-HCV activity.
  • at least one of the additional compounds is an interferon or a ribavirin.
  • the interferon is selected from interferon alpha 2B, pegylated interferon alpha, consensus interferon, interferon alpha 2A, and lymphoblastiod interferon tau.
  • composition further comprises one or two additional compounds having anti-HCV activity wherein at least one of the additional compounds is selected from interleukin 2, interleukin 6, interleukin 12, a compound that enhances the development of a type 1 helper T cell response, interfering RNA, anti-sense RNA, Imiqimod, ribavirin, an inosine 5'- monophospate dehydrogenase inhibitor, amantadine, and rimantadine.
  • interleukin 2 interleukin 6, interleukin 12
  • a compound that enhances the development of a type 1 helper T cell response interfering RNA, anti-sense RNA, Imiqimod, ribavirin, an inosine 5'- monophospate dehydrogenase inhibitor, amantadine, and rimantadine.
  • composition further comprises one or two additional compounds having anti-HCV activity wherein at least one of the additional compounds is effective to inhibit the function of a target selected from HCV metalloprotease, HCV serine protease, HCV polymerase, HCV helicase, HCV NS4B protein, HCV entry, HCV assembly, HCV egress, HCV NS5A protein, and IMPDH for the treatment of an HCV infection.
  • a target selected from HCV metalloprotease, HCV serine protease, HCV polymerase, HCV helicase, HCV NS4B protein, HCV entry, HCV assembly, HCV egress, HCV NS5A protein, and IMPDH for the treatment of an HCV infection.
  • the present disclosure provides a method of treating an HCV infection in a patient, comprising administering to the patient a therapeutically effective amount of a compound of Formula (I), or a pharmaceutically acceptable salt thereof.
  • the method further comprises administering one or two additional compounds having anti-HCV activity prior to, after or simultaneously with the compound of Formula (I), or a pharmaceutically acceptable salt thereof.
  • at least one of the additional compounds is an interferon or a ribavirin.
  • the interferon is selected from interferon alpha 2B, pegylated interferon alpha, consensus interferon, interferon alpha 2A, and lymphoblastiod interferon tau.
  • the method further comprises administering one or two additional compounds having anti-HCV activity prior to, after or simultaneously with the compound of Formula (I), or a pharmaceutically acceptable salt thereof, wherein at least one of the additional compounds is selected from interleukin 2, interleukin 6, interleukin 12, a compound that enhances the development of a type 1 helper T cell response, interfering RNA, anti-sense RNA, Imiqimod, ribavirin, an inosine 5 '-monophospate dehydrogenase inhibitor, amantadine, and rimantadine.
  • interleukin 2 interleukin 6, interleukin 12
  • a compound that enhances the development of a type 1 helper T cell response interfering RNA, anti-sense RNA, Imiqimod, ribavirin, an inosine 5 '-monophospate dehydrogenase inhibitor, amantadine, and rimantadine.
  • the method further comprises administering one or two additional compounds having anti-HCV activity prior to, after or simultaneously with the compound of Formula (I), or a pharmaceutically acceptable salt thereof, wherein at least one of the additional compounds is effective to inhibit the function of a target selected from HCV metalloprotease, HCV serine protease, HCV polymerase, HCV helicase, HCV NS4B portein, HCV entry, HCV assembly, HCV egress, HCV NS5A protein, and IMPDH for the treatment of an HCV infection.
  • a target selected from HCV metalloprotease, HCV serine protease, HCV polymerase, HCV helicase, HCV NS4B portein, HCV entry, HCV assembly, HCV egress, HCV NS5A protein, and IMPDH for the treatment of an HCV infection.
  • Other embodiments of the present disclosure may comprise suitable combinations of two or more of embodiments and/or aspects disclosed herein.
  • the compounds of the present disclosure also exist as tautomers; therefore the present disclosure also encompasses all tautomeric forms.
  • R 8 may be attached to either the carbon atom in the imidazole ring or, alternatively,
  • R 8 may take the place of the hydrogen atom on the nitrogen ring to form an N- substituted imidazole.
  • R 6 at a particular location in a molecule be independent of its definitions elsewhere in that molecule.
  • each of the two R 1 groups may be the same or different.
  • aryl, cycloalkyl, and heterocyclyl groups of the present disclosure may be substituted as described in each of their respective definitions.
  • aryl part of an arylalkyl group may be substituted as described in the definition of the term 'aryl'.
  • alkenyl refers to a straight or branched chain group of two to six carbon atoms containing at least one carbon-carbon double bond.
  • alkenyloxy refers to an alkenyl group attached to the parent molecular moiety through an oxygen atom.
  • alkenyloxycarbonyl refers to an alkenyloxy group attached to the parent molecular moiety through a carbonyl group.
  • alkoxy refers to an alkyl group attached to the parent molecular moiety through an oxygen atom.
  • alkoxyalkyl refers to an alkyl group substituted with one, two, or three alkoxy groups.
  • alkoxyalkylcarbonyl refers to an alkoxyalkyl group attached to the parent molecular moiety through a carbonyl group.
  • alkoxycarbonyl refers to an alkoxy group attached to the parent molecular moiety through a carbonyl group.
  • alkoxycarbonylalkyl refers to an alkyl group substituted with one, two, or three alkoxycarbonyl groups.
  • alkyl refers to a group derived from a straight or branched chain saturated hydrocarbon containing from one to six carbon atoms.
  • m and/or n is 1 or 2;
  • X and/or Y is CHR 5 and/or CHR 6 , respectively, and
  • R 5 and/or R 6 is alkyl, each alkyl can optionally form a fused three- to six-membered ring with an adjacent carbon atom to provide one of the structures shown below:
  • alkylcarbonyl refers to an alkyl group attached to the parent molecular moiety through a carbonyl group.
  • alkylcarbonylalkyl refers to an alkyl group substituted with one, two, or three alkylcarbonyl groups.
  • alkylcarbonyloxy refers to an alkylcarbonyl group attached to the parent molecular moiety through an oxygen atom.
  • alkylsulfanyl refers to an alkyl group attached to the parent molecular moiety through a sulfur atom.
  • alkylsulfonyl refers to an alkyl group attached to the parent molecular moiety through a sulfonyl group.
  • aryl refers to a phenyl group, or a bicyclic fused ring system wherein one or both of the rings is a phenyl group.
  • Bicyclic fused ring systems consist of a phenyl group fused to a four- to six-membered aromatic or non- aromatic carbocyclic ring.
  • the aryl groups of the present disclosure can be attached to the parent molecular moiety through any substitutable carbon atom in the group.
  • Representative examples of aryl groups include, but are not limited to, indanyl, indenyl, naphthyl, phenyl, and tetrahydronaphthyl.
  • the aryl groups of the present disclosure are optionally substituted with one, two, three, four, or five substituents independently selected from alkoxy, alkoxyalkyl, alkoxycarbonyl, alkyl, alkylcarbonyl, a second aryl group, arylalkoxy, arylalkyl, arylcarbonyl, cyano, halo, haloalkoxy, haloalkyl, heterocyclyl, heterocyclylalkyl, heterocyclylcarbonyl, hydroxy, hydroxyalkyl, nitro, -NR x R y , (NR x R y )alkyl, oxo, and -P(O)OR 2 , wherein each R is independently selected from hydrogen and alkyl; and wherein the alkyl part of the arylalkyl and the heterocyclylalkyl are unsubstituted and wherein the second aryl group, the aryl part of the arylalkyl, the
  • arylalkenyl refers to an alkenyl group substituted with one, two, or three aryl groups.
  • arylalkoxy refers to an aryl group attached to the parent molecular moiety through an alkoxy group.
  • arylalkoxyalkyl refers to an alkyl group substituted with one, two, or three arylalkoxy groups.
  • arylalkoxyalkylcarbonyl refers to an arylalkoxyalkyl group attached to the parent molecular moiety through a carbonyl group.
  • arylalkoxycarbonyl refers to an arylalkoxy group attached to the parent molecular moiety through a carbonyl group.
  • arylalkyl refers to an alkyl group substituted with one, two, or three aryl groups.
  • the alkyl part of the arylalkyl is further optionally substituted with one or two additional groups independently selected from alkoxy, alkylcarbonyloxy, halo, haloalkoxy, haloalkyl, heterocyclyl, hydroxy, and -NR c R d , wherein the heterocyclyl is further optionally substitued with one or two substituents independently selected from alkoxy, alkyl, unsubstituted aryl, unsubstituted arylalkoxy, unsubstituted arylalkoxycarbonyl, halo, haloalkoxy, haloalkyl, hydroxy, and -NR x R y .
  • arylalkylcarbonyl refers to an arylalkyl group attached to the parent molecular moiety through a carbonyl group.
  • arylcarbonyl refers to an aryl group attached to the parent molecular moiety through a carbonyl group.
  • aryloxy refers to an aryl group attached to the parent molecular moiety through an oxygen atom.
  • aryloxyalkyl refers to an alkyl group substituted with one, two, or three aryloxy groups.
  • aryloxycarbonyl refers to an aryloxy group attached to the parent molecular moiety through a carbonyl group.
  • arylsulfonyl refers to an aryl group attached to the parent molecular moiety through a sulfonyl group.
  • Cap and “cap” as used herein, refer to the group which is placed on the nitrogen atom of the terminal nitrogen-containing ring, i.e., the pyrrolidine rings of compound 1 e. It should be understood that “Cap” or “cap” can refer to the reagent used to append the group to the terminal nitrogen-containing ring or to the fragment in the final product, i.e., "Cap-51” or "The Cap-51 fragment found in LS- 19".
  • carbonyl refers to -C(O)-.
  • cycloalkyl refers to a saturated monocyclic, hydrocarbon ring system having three to seven carbon atoms and zero heteroatoms.
  • Representative examples of cycloalkyl groups include, but are not limited to, cyclopropyl, cyclopentyl, and cyclohexyl.
  • the cycloalkyl groups of the present disclosure are optionally substituted with one, two, three, four, or five substituents independently selected from alkoxy, alkyl, aryl, cyano, halo, haloalkoxy, haloalkyl, heterocyclyl, hydroxy, hydroxyalkyl, nitro, and -NR x R y , wherein the aryl and the heterocyclyl are futher optionally substituted with one, two, or three substituents independently selected from alkoxy, alkyl, cyano, halo, haloalkoxy, haloalkyl, hydroxy, and nitro.
  • (cycloalkyl)alkenyl refers to an alkenyl group substituted with one, two, or three cycloalkyl groups.
  • (cycloalkyl)alkyl refers to an alkyl group substituted with one, two, or three cycloalkyl groups.
  • the alkyl part of the (cycloalkyl)alkyl is further optionally substituted with one or two groups independently selected from hydroxy and -NR c R d .
  • cycloalkyloxy refers to a cycloalkyl group attached to the parent molecular moiety through an oxygen atom.
  • cycloalkyloxyalkyl refers to an alkyl group substituted with one, two, or three cycloalkyloxy groups.
  • cycloalkylsulfonyl refers to a cycloalkyl group attached to the parent molecular moiety through a sulfonyl group.
  • halo and halogen, as used herein, refer to F, Cl, Br, or I.
  • haloalkoxy refers to a haloalkyl group attached to the parent molecular moiety through an oxygen atom.
  • haloalkoxycarbonyl refers to a haloalkoxy group attached to the parent molecular moiety through a carbonyl group.
  • haloalkyl refers to an alkyl group substituted by one, two, three, or four halogen atoms.
  • heterocyclyl refers to a four-, five-, six-, or seven- membered ring containing one, two, three, or four heteroatoms independently selected from nitrogen, oxygen, and sulfur.
  • the four-membered ring has zero double bonds
  • the five-membered ring has zero to two double bonds
  • the six- and seven- membered rings have zero to three double bonds.
  • heterocyclyl also includes bicyclic groups in which the heterocyclyl ring is fused to another monocyclic heterocyclyl group, or a four- to six-membered aromatic or non-aromatic carbocyclic ring; as well as bridged bicyclic groups such as 7-azabicyclo[2.2.
  • heterocyclyl groups of the present disclosure can be attached to the parent molecular moiety through any carbon atom or nitrogen atom in the group.
  • heterocyclyl groups include, but are not limited to, benzothienyl, furyl, imidazolyl, indolinyl, indolyl, isothiazolyl, isoxazolyl, morpholinyl, oxazolyl, piperazinyl, piperidinyl, pyrazolyl, pyridinyl, pyrrolidinyl, pyrrolopyridinyl, pyrrolyl, thiazolyl, thienyl, thiomorpholinyl, 7-azabicyclo[2.2.1]hept-7-yl, 2-azabicyclo[2.2.2]oc-2-tyl, and 2- azabicyclo[2.2.2]oc-3-tyl.
  • heterocyclyl groups of the present disclosure are optionally substituted with one, two, three, four, or five substituents independently selected from alkoxy, alkoxyalkyl, alkoxycarbonyl, alkyl, alkylcarbonyl, aryl, arylalkyl, arylcarbonyl, cyano, halo, haloalkoxy, haloalkyl, a second heterocyclyl group, heterocyclylalkyl, heterocyclylcarbonyl, hydroxy, hydroxyalkyl, nitro, - NR x R y , (NR x R y )alkyl, and oxo, wherein the alkyl part of the arylalkyl and the heterocyclylalkyl are unsubstituted and wherein the aryl, the aryl part of the arylalkyl, the aryl part of the arylcarbonyl, the second heterocyclyl group, and the heterocyclyl part of the heterocycly
  • heterocyclylalkenyl refers to an alkenyl group substituted with one, two, or three heterocyclyl groups.
  • heterocyclylalkoxy refers to a heterocyclyl group attached to the parent molecular moiety through an alkoxy group.
  • heterocyclylalkoxycarbonyl refers to a heterocyclylalkoxy group attached to the parent molecular moiety through a carbonyl group.
  • heterocyclylalkyl refers to an alkyl group substituted with one, two, or three heterocyclyl groups.
  • the alkyl part of the heterocyclylalkyl is further optionally substituted with one or two additional groups independently selected from alkoxy, alkylcarbonyloxy, aryl, halo, haloalkoxy, haloalkyl, hydroxy, and -NR c R d , wherein the aryl is further optionally substitued with one or two substituents independently selected from alkoxy, alkyl, unsubstituted aryl, unsubstitued arylalkoxy, unsubstituted arylalkoxycarbonyl, halo, haloalkoxy, haloalkyl, hydroxy, and -NR x R y .
  • heterocyclylalkylcarbonyl refers to a heterocyclylalkyl group attached to the parent molecular moiety through a carbonyl group.
  • heterocyclylcarbonyl refers to a heterocyclyl group attached to the parent molecular moiety through a carbonyl group.
  • heterocyclyloxy refers to a heterocyclyl group attached to the parent molecular moiety through an oxygen atom.
  • heterocyclyloxyalkyl refers to an alkyl group substituted with one, two, or three heterocyclyloxy groups.
  • heterocyclyloxycarbonyl refers to a heterocyclyloxy group attached to the parent molecular moiety through a carbonyl group.
  • hydroxy refers to -OH.
  • hydroxyalkyl refers to an alkyl group substituted with one, two, or three hydroxy groups.
  • hydroxyalkylcarbonyl refers to a hydroxyalkyl group attached to the parent molecular moiety through a carbonyl group.
  • nitro refers to -NO 2 .
  • -NR a R b refers to two groups, R a and R b , which are attached to the parent molecular moiety through a nitrogen atom.
  • R a and R b are independently selected from hydrogen, alkenyl, and alkyl.
  • (NR a R )alkyl refers to an alkyl group substituted with one, two, or three -NR a R b groups.
  • (NR a R b )carbonyl refers to an -NR a R b group attached to the parent molecular moiety through a carbonyl group.
  • R c and R are independently selected from hydrogen, alkenyloxycarbonyl, alkoxyalkylcarbonyl, alkoxycarbonyl, alkyl, alkylcarbonyl, alkylsulfonyl, aryl, arylalkoxycarbonyl, arylalkyl, arylalkylcarbonyl, arylcarbonyl, aryloxycarbonyl, arylsulfonyl, cycloalkyl, cycloalkylsulfonyl, formyl, haloalkoxycarbonyl, heterocyclyl, heterocyclylalkoxycarbonyl, heterocyclylalkyl, heterocyclylalkylcarbonyl, heterocyclylcarbonyl, heterocyclyloxycarbonyl, hydroxyalkyl
  • (NR c R d )alkenyl refers to an alkenyl group substituted with one, two, or three -NR c R d groups.
  • (NR c R d )alkyl refers to an alkyl group substituted with one, two, or three -NR c R d groups.
  • the alkyl part of the (NR c R d )alkyl is further optionally substituted with one or two additional groups selected from alkoxy, alkoxyalkylcarbonyl, alkoxycarbonyl, alkylsulfanyl, arylalkoxyalkylcarbonyl, carboxy, heterocyclyl, heterocyclylcarbonyl, hydroxy, and (NR e R f )carbonyl; wherein the heterocyclyl is further optionally substituted with one, two, three, four, or five substituents independently selected from alkoxy, alkyl, cyano, halo, haloalkoxy, haloalkyl, and nitro.
  • (NR C R )carbonyl refers to an -NR C R group attached to the parent molecular moiety through a carbonyl group.
  • -NR e R f refers to two groups, R e and R f , which are attached to the parent molecular moiety through a nitrogen atom.
  • R e and R are independently selected from hydrogen, alkyl, unsubstituted aryl, unsubstituted arylalkyl, unsubstituted cycloalkyl, unsubstituted (cyclolalkyl)alkyl, unsubstituted heterocyclyl, unsubstituted heterocyclylalkyl, (NR x R y )alkyl, and (NR x R y )carbonyl.
  • (NR e R f )alkyl refers to an alkyl group substituted with one, two, or three -NR e R f groups.
  • (NR e R f )aikylcarbonyl refers to an (NR e R f )alkyl group attached to the parent molecular moiety through a carbonyl group.
  • (NR e R f )carbonyl refers to an -NR e R f group attached to the parent molecular moiety through a carbonyl group.
  • (NR e R f )sulfonyl refers to an -NR e R f group attached to the parent molecular moiety through a sulfonyl group.
  • -NR x R y refers to two groups, R x and R y , which are attached to the parent molecular moiety through a nitrogen atom.
  • R x and R y are independently selected from hydrogen, alkoxycarbonyl, alkyl, alkylcarbonyl, unsubstituted aryl, unsubstituted arylalkoxycarbonyl, unsubstituted arylalkyl, unsubstituted cycloalkyl, unsubstituted heterocyclyl, and (NR X R y )carbonyl, wherein R x and R y are independently selected from hydrogen and alkyl.
  • (NR x R y )alkyl refers to an alkyl group substituted with one, two, or three -NR x R y groups.
  • sulfonyl refers to -SO 2 -.
  • Trialkylsilyl refers to -SiR3, wherein R is alkyl.
  • R groups may be the same or different.
  • Trialkylsilylalkyl refers to an alkyl group substituted with one, two, or three trialkylsilyl groups.
  • trialkylsilylalkoxy refers to a trialkylsilylalkyl group attached to the parent molecular moiety through an oxygen atom.
  • trialkylsilylalkoxyalkyl refers to an alkyl group substituted with one, two, or three trialkylsilylalkoxy groups.
  • Certain compounds of the present disclosure may also exist in different stable conformational forms which may be separable. Torsional asymmetry due to restricted rotation about an asymmetric single bond, for example because of steric hindrance or ring strain, may permit separation of different conformers.
  • the present disclosure includes each conformational isomer of these compounds and mixtures thereof.
  • the compounds of the present disclosure can exist as pharmaceutically acceptable salts.
  • pharmaceutically acceptable salt represents salts or zwitterionic forms of the compounds of the present disclosure which are water or oil-soluble or dispersible, which are, within the scope of sound medical judgment, suitable for use in contact with the tissues of patients without excessive toxicity, irritation, allergic response, or other problem or complication commensurate with a reasonable benefit/risk ratio, and are effective for their intended use
  • the salts can be prepared during the final isolation and purification of the compounds or separately by reacting a suitable nitrogen atom with a suitable acid.
  • Representative acid addition salts include acetate, adipate, alginate, citrate, aspartate, benzoate, benzenesulfonate, bisulfate, butyrate, camphorate, camphorsulfonate; digluconate, dihydrobromide, diydrochloride, dihydroiodide, glycerophosphate, hemisulfate, heptanoate, hexanoate, formate, fumarate, hydrochloride, hydrobromide, hydroiodide, 2 -hydroxy ethanesulfonate, lactate, maleate, mesitylenesulfonate, methanesulfonate, naphthylenesulfonate, nicotinate, 2-naphthalenesulfonate, oxalate, palmoate, pectinate, persulfate, 3-phenylproprionate, picrate, pivalate, propionate, succinate, tartrate,
  • Basic addition salts can be prepared during the final isolation and purification of the compounds by reacting a carboxy group with a suitable base such as the hydroxide, carbonate, or bicarbonate of a metal cation or with ammonia or an organic primary, secondary, or tertiary amine.
  • a suitable base such as the hydroxide, carbonate, or bicarbonate of a metal cation or with ammonia or an organic primary, secondary, or tertiary amine.
  • the cations of pharmaceutically acceptable salts include lithium, sodium, potassium, calcium, magnesium, and aluminum, as well as nontoxic quaternary amine cations such as ammonium, tetramethylammonium, tetraethylammonium, methylamine, dimethylamine, trimethylamine, triethylamine, diethylamine, ethylamine, tributylamine, pyridine, N,N-dimethylaniline, N-methylpiperidine, N-methylmorpholine, dicyclohexylamine, procaine, dibenzylamine, N,N-dibenzylphenethylamine, and N,N'- dibenzylethylenediamine.
  • Other representative organic amines useful for the formation of base addition salts include ethylenediamine, ethanolamine, diethanolamine, piperidine, and piperazine.
  • compositions which include therapeutically effective amounts of compounds of formula (I) or pharmaceutically acceptable salts thereof, and one or more pharmaceutically acceptable carriers, diluents, or excipients.
  • therapeutically effective amount refers to the total amount of each active component that is sufficient to show a meaningful patient benefit, e.g., a reduction in viral load. When applied to an individual active ingredient, administered alone, the term refers to that ingredient alone.
  • the term refers to combined amounts of the active ingredients that result in the therapeutic effect, whether administered in combination, serially, or simultaneously.
  • the compounds of formula (I) and pharmaceutically acceptable salts thereof are as described above.
  • the carrier(s), diluent(s), or excipient(s) must be acceptable in the sense of being compatible with the other ingredients of the formulation and not deleterious to the recipient thereof.
  • a process for the preparation of a pharmaceutical formulation including admixing a compound of formula (I), or a pharmaceutically acceptable salt thereof, with one or more pharmaceutically acceptable carriers, diluents, or excipients.
  • pharmaceutically acceptable refers to those compounds, materials, compositions, and/or dosage forms which are, within the scope of sound medical judgment, suitable for use in contact with the tissues of patients without excessive toxicity, irritation, allergic response, or other problem or complication commensurate with a reasonable benefit/risk ratio, and are effective for their intended use.
  • Pharmaceutical formulations may be presented in unit dose forms containing a predetermined amount of active ingredient per unit dose. Dosage levels of between about 0.01 and about 250 milligram per kilogram (“mg/kg”) body weight per day, preferably between about 0.05 and about 100 mg/kg body weight per day of the compounds of the present disclosure are typical in a monotherapy for the prevention and treatment of HCV mediated disease.
  • the pharmaceutical compositions of this disclosure will be administered from about 1 to about 5 times per day or alternatively, as a continuous infusion. Such administration can be used as a chronic or acute therapy.
  • the amount of active ingredient that may be combined with the carrier materials to produce a single dosage form will vary depending on the condition being treated, the severity of the condition, the time of administration, the route of administration, the rate of excretion of the compound employed, the duration of treatment, and the age, gender, weight, and condition of the patient.
  • Preferred unit dosage formulations are those containing a daily dose or sub-dose, as herein above recited, or an appropriate fraction thereof, of an active ingredient. Treatment may be initiated with small dosages substantially less than the optimum dose of the compound. Thereafter, the dosage is increased by small increments until the optimum effect under the circumstances is reached.
  • the compound is most desirably administered at a concentration level that will generally afford antivirally effective results without causing any harmful or deleterious side effects.
  • compositions of this disclosure comprise a combination of a compound of the present disclosure and one or more additional therapeutic or prophylactic agent
  • both the compound and the additional agent are usually present at dosage levels of between about 10 to 150%, and more preferably between about 10 and 80% of the dosage normally administered in a monotherapy regimen.
  • compositions may be adapted for administration by any appropriate route, for example by the oral (including buccal or sublingual), rectal, nasal, topical (including buccal, sublingual, or transdermal), vaginal, or parenteral (including subcutaneous, intracutaneous, intramuscular, intra-articular, intrasynovial, intrasternal, intrathecal, intralesional, intravenous, or intradermal injections or infusions) route.
  • Such formulations may be prepared by any method known in the art of pharmacy, for example by bringing into association the active ingredient with the carrier(s) or excipient(s). Oral administration or administration by injection are preferred.
  • compositions adapted for oral administration may be presented as discrete units such as capsules or tablets; powders or granules; solutions or suspensions in aqueous or non-aqueous liquids; edible foams or whips; or oil-in- water liquid emulsions or water-in-oil emulsions.
  • the active drug component can be combined with an oral, non-toxic pharmaceutically acceptable inert carrier such as ethanol, glycerol, water, and the like.
  • Powders are prepared by comminuting the compound to a suitable fine size and mixing with a similarly comminuted pharmaceutical carrier such as an edible carbohydrate, as, for example, starch or mannitol. Flavoring, preservative, dispersing, and coloring agent can also be present.
  • Capsules are made by preparing a powder mixture, as described above, and filling formed gelatin sheaths.
  • Glidants and lubricants such as colloidal silica, talc, magnesium stearate, calcium stearate, or solid polyethylene glycol can be added to the powder mixture before the filling operation.
  • a disintegrating or solubilizing agent such as agar-agar, calcium carbonate, or sodium carbonate can also be added to improve the availability of the medicament when the capsule is ingested.
  • suitable binders, lubricants, disintegrating agents, and coloring agents can also be incorporated into the mixture.
  • Suitable binders include starch, gelatin, natural sugars such as glucose or beta- lactose, corn sweeteners, natural and synthetic gums such as acacia, tragacanth or sodium alginate, carboxymethylcellulose, polyethylene glycol, and the like.
  • Lubricants used in these dosage forms include sodium oleate, sodium chloride, and the like.
  • Disintegrators include, without limitation, starch, methyl cellulose, agar, betonite, xanthan gum, and the like. Tablets are formulated, for example, by preparing a powder mixture, granulating or slugging, adding a lubricant and disintegrant, and pressing into tablets.
  • a powder mixture is prepared by mixing the compound, suitable comminuted, with a diluent or base as described above, and optionally, with a binder such as carboxymethylcellulose, an aliginate, gelating, or polyvinyl pyrrolidone, a solution retardant such as paraffin, a resorption accelerator such as a quaternary salt and/or and absorption agent such as betonite, kaolin, or dicalcium phosphate.
  • the powder mixture can be granulated by wetting with a binder such as syrup, starch paste, acadia mucilage, or solutions of cellulosic or polymeric materials and forcing through a screen.
  • the powder mixture can be run through the tablet machine and the result is imperfectly formed slugs broken into granules.
  • the granules can be lubricated to prevent sticking to the tablet forming dies by means of the addition of stearic acid, a stearate salt, talc, or mineral oil.
  • the lubricated mixture is then compressed into tablets.
  • the compounds of the present disclosure can also be combined with a free flowing inert carrier and compressed into tablets directly without going through the granulating or slugging steps.
  • a clear or opaque protective coating consisting of a sealing coat of shellac, a coating of sugar or polymeric material, and a polish coating of wax can be provided. Dyestuffs can be added to these coatings to distinguish different unit dosages.
  • Oral fluids such as solution, syrups, and elixirs can be prepared in dosage unit form so that a given quantity contains a predetermined amount of the compound.
  • Syrups can be prepared by dissolving the compound in a suitably flavored aqueous solution, while elixirs are prepared through the use of a non-toxic vehicle.
  • Solubilizers and emulsifiers such as ethoxylated isostearyl alcohols and polyoxyethylene sorbitol ethers, preservatives, flavor additive such as peppermint oil or natural sweeteners, or saccharin or other artificial sweeteners, and the like can also be added.
  • dosage unit formulations for oral administration can be microencapsulated.
  • the formulation can also be prepared to prolong or sustain the release as for example by coating or embedding particulate material in polymers, wax, or the like.
  • the compounds of formula (I), and pharmaceutically acceptable salts thereof, can also be administered in the form of liposome delivery systems, such as small unilamellar vesicles, large unilamellar vesicles, and multilamellar vesicles.
  • liposomes can be formed from a variety of phopholipids, such as cholesterol, stearylamine, or phophatidylcholines.
  • the compounds of formula (I) and pharmaceutically acceptable salts thereof may also be delivered by the use of monoclonal antibodies as individual carriers to which the compound molecules are coupled.
  • the compounds may also be coupled with soluble polymers as targetable drug carriers.
  • Such polymers can include polyvinylpyrrolidone, pyran copolymer, polyhydroxypropylmethacrylamidephenol, polyhydroxyethylaspartamidephenol, or polyethyleneoxidepolylysine substituted with palitoyl residues.
  • the compounds may be coupled to a class of biodegradable polymers useful in achieving controlled release of a drug, for example, polylactic acid, polepsilon caprolactone, polyhydroxy butyric acid, polyorthoesters, polyacetals, polydihydropyrans, polycyanoacrylates, and cross-linked or amphipathic block copolymers of hydrogels.
  • a class of biodegradable polymers useful in achieving controlled release of a drug, for example, polylactic acid, polepsilon caprolactone, polyhydroxy butyric acid, polyorthoesters, polyacetals, polydihydropyrans, polycyanoacrylates, and cross-linked or amphipathic block copolymers of hydrogels.
  • compositions adapted for transdermal administration may be presented as discrete patches intended to remain in intimate contact with the epidermis of the recipient for a prolonged period of time.
  • the active ingredient may be delivered from the patch by iontophoresis as generally described in Pharmaceutical Research 1986, 3(6), 318.
  • compositions adapted for topical administration may be formulated as ointments, creams, suspensions, lotions, powders, solutions, pastes, gels, sprays, aerosols, or oils.
  • Pharmaceutical formulations adapted for rectal administration may be presented as suppositories or as enemas.
  • compositions adapted for nasal administration wherein the carrier is a solid include a course powder having a particle size for example in the range 20 to 500 microns which is administered in the manner in which snuff is taken, i.e., by rapid inhalation through the nasal passage from a container of the powder held close up to the nose.
  • suitable formulations wherein the carrier is a liquid, for administration as a nasal spray or nasal drops, include aqueous or oil solutions of the active ingredient.
  • Fine particle dusts or mists which may be generated by means of various types of metered, dose pressurized aerosols, nebulizers, or insufflators.
  • compositions adapted for vaginal administration may be presented as pessaries, tampons, creams, gels, pastes, foams, or spray formulations.
  • compositions adapted for parenteral administration include aqueous and non-aqueous sterile injection solutions which may contain anti-oxidants, buffers, bacteriostats, and soutes which render the formulation isotonic with the blood of the intended recipient; and aqueous and non-aqueous sterile suspensions which may include suspending agents and thickening agents.
  • the formulations may be presented in unit-dose or multi-dose containers, for example sealed ampoules and vials, and may be stored in a freeze-dried (lyophilized) condition requiring only the addition of the sterile liquid carrier, for example water for injections, immediately prior to use.
  • Extemporaneous injection solutions and suspensions may be prepared from sterile powders, granules, and tablets.
  • formulations may include other agents conventional in the art having regard to the type of formulation in question, for example those suitable for oral administration may include flavoring agents.
  • formulations may include other agents conventional in the art having regard to the type of formulation in question, for example those suitable for oral administration may include flavoring agents.
  • patient includes both human and other mammals.
  • treating refers to: (i) preventing a disease, disorder or condition from occurring in a patient that may be predisposed to the disease, disorder, and/or condition but has not yet been diagnosed as having it; (ii) inhibiting the disease, disorder, or condition, i.e., arresting its development; and (iii) relieving the disease, disorder, or condition, i.e., causing regression of the disease, disorder, and/or condition.
  • the compounds of the present disclosure can also be administered with a cyclosporin, for example, cyclosporin A.
  • Cyclosporin A has been shown to be active against HCV in clinical trials (Hepatology 2003, 38, 1282; Biochem. Biophys. Res. Commun. 2004, 313, 42; J. Gastroenterol. 2003, 38, 567).
  • Table 1 lists some illustrative examples of compounds that can be administered with the compounds of this disclosure.
  • the compounds of the disclosure can be administered with other anti-HCV activity compounds in combination therapy, either jointly or separately, or by combining the compounds into a composition.
  • the compounds of the present disclosure may also be used as laboratory reagents.
  • Compounds may be instrumental in providing research tools for designing of viral replication assays, validation of animal assay systems and structural biology studies to further enhance knowledge of the HCV disease mechanisms. Further, the compounds of the present disclosure are useful in establishing or determining the binding site of other antiviral compounds, for example, by competitive inhibition.
  • the compounds of this disclosure may also be used to treat or prevent viral contamination of materials and therefore reduce the risk of viral infection of laboratory or medical personnel or patients who come in contact with such materials, e.g., blood, tissue, surgical instruments and garments, laboratory instruments and garments, and blood collection or transfusion apparatuses and materials.
  • materials e.g., blood, tissue, surgical instruments and garments, laboratory instruments and garments, and blood collection or transfusion apparatuses and materials.
  • This disclosure is intended to encompass compounds having formula (I) when prepared by synthetic processes or by metabolic processes including those occurring in the human or animal body (in vivo) or processes occurring in vitro.
  • HATU O-(7- azabenzotriazol-l-yl)-N,N,N',N'-tetramethyluronium hexafluorophosphate
  • Boc or BOC for tert-butoxycarbonyl
  • NBS for N-bromosuccinimide
  • tBu or t-Bu for tert- butyl
  • SEM for -(trimethylsilyl)ethoxymethyl
  • DMSO dimethylsulfoxide
  • MeOH for methanol
  • TFA trifluoroacetic acid
  • RT room temperature or retention time (context will dictate); t R for retention time
  • EDCI for l-(3-dimethylaminopropyl)-3- ethylcarbodiimide hydrochloride
  • DMAP for 4-dimethyla
  • a coupling reagent such as HATU in combination with an amine base such as Hunig's base can be used in this regard.
  • 4 may be reacted with an isocyanate or carbamoyl chloride to provide compounds of formula 5 where R 9 is an amine.
  • Further deprotection of 5 can be accomplished by treatment with strong acid such as HCl or trifluoroacetic acid. Standard conditions analogous to those used to convert 4 to 5 can be used to prepare 7 from 6.
  • Scheme 2 Asymmetrically Capped Biphenyls Conversion of 6 (from Scheme 1) to 10 can be done using standard amide coupling conditions such as HATU with an amine base, such as Hunig's base. Deprotection can be accomplished with strong acid such as HCl or trifluoroacetic acid affording 11. Compound 11 can then be converted to 12, 13, or 14 using an acid chloride, an isocyanate or carbamoyl chloride, or a chloroformate respectively.
  • Compounds 17, 18, and 19 can be prepared from 16 by treating 16 with an appropriate chloroformate, isocyanate or carbamoyl chloride, or an acid chloride respectively.
  • Symmetrical biphenyl analogs (compounds of formula 7 where both halves of the molecule are equivalent) can be synthesized starting from bromoketone 20. Amination by displacement with a nucleophile such as azide, phthalimide or preferably sodium diformylamide (Yinglin and Hongwen, Synthesis 1990, 122) followed by deprotection affords 21. Condensation under standard amination conditions such as HATU and Hunig's base with an appropriately protected amino acid provides 22.
  • Acylation can be affected with a carboxylic acid (R 9 CChH) in a manner similar to the conversion of 21 to 22.
  • Keto-amide 24 (analogous to 1 in Scheme 1) is prepared from keto-amide 24 or keto-ester 27 via heating with ammonium acetate under thermal or microwave conditions.
  • Keto-amide 24 can be prepared from 23 via condensation with an appropriate cyclic or acyclic amino acid under standard amide formation conditions.
  • Bromide 26 can give rise to 23 by treatment with a nucleophile such as azide, phthalimide or sodium diformylamide (Synthesis 1990, 122) followed by deprotection.
  • Bromide 26 can also be converted to 27 by reacting with an appropriate cyclic or acyclic N-protected amino acid in the presence of base such as potassium carbonate or sodium bicarbonate.
  • Bromide 25 can be converted to boronic ester 2 via treatment with bis-pinacalotodiboron under palladium catalysis according to the method described in Journal of Organic Chemistry 1995, 60, 7508, or variations thereof.
  • starting materials such as 31a (analogous to 25 in Scheme 5 and 1 in Scheme 1) may be prepared by reacting bromoimidazole derivatives 31 under Suzuki-type coupling conditions with a variety of chloro- substituted aryl boronic acids which can either be prepared by Standard methodologies (see, for example, Organic Letters 2006, 8, 305 and references cited therein) or purchased from commercial suppliers.
  • Bromoimidazole 31 can be obtained by brominating imidazole 30 with a source of bromonium ion such as bromine, CBr 4 , or N-bromosuccinimide.
  • Imidazole 30 can be prepared from N- protected amino acids which are appropriately substituted by reacting with glyoxal in a methanolic solution of ammonium hydroxide.
  • aryl halide 32 can be coupled under Suzuki-Miyaura palladium catalyzed conditions to form the heteroaryl derivative 34.
  • Acylation of the resulting amine in 37 to give 38 can be accomplished as in the transformation of 35 to 36.
  • Acylation of 39 can be accomplished in analogous fashion to that described for the transformation of 35 to 36.
  • Heteroaryl chloride 29 can be converted to symmetrical analog 40 via treatment with a source of palladium such as dichlorobis(benzonitrile) palladium in the presence of tetrakis(dimethylamino)ethylene at elevated temperature. Removal of the SEM ether and Boc carbamates found in 40 can be accomplished in one step by treatment with a strong acid such as HCl or trifluoroacetic acid providing 41. Conversion to 42 can be accomplished in similar fashion to the conditions used to convert 38 to 39 in Scheme 7.
  • a source of palladium such as dichlorobis(benzonitrile) palladium in the presence of tetrakis(dimethylamino)ethylene at elevated temperature.
  • Removal of the SEM ether and Boc carbamates found in 40 can be accomplished in one step by treatment with a strong acid such as HCl or trifluoroacetic acid providing 41. Conversion to 42 can be accomplished in similar fashion to the conditions used to convert 38 to 39 in Scheme 7.
  • Heteroaryl bromides 54 may be reacted with a vinyl stannane such as tributyl(l-ethoxyvinyl)tin in the presence of a source of palladium such as dichlorobis(triphenylphosphine)palladium (II) to provide 55 which can be subsequently transformed into bromoketone 51 via treatment with a source of bromonium ion such as N-bormosuccinimide, CBr 4 , or bromine.
  • a source of bromonium ion such as N-bormosuccinimide, CBr 4 , or bromine.
  • keto- substituted heteroaryl bromides 53 may be directly converted to 51 via treatment with a source of bromonium ion such as bromine, CBr 4 , or N-bromosuccinimide.
  • Bromide 51 can be converted to aminoketone 48 via addition of sodium azide, potassium phthalimide or sodium diformylamide (Synthesis 1990 122) followed by deprotection.
  • Aminoketone 48 can then be coupled with an appropriately substituted amino acid under standard amide formation conditions (i.e.; a coupling reagent such as HATU in the presence of a mild base such as Hunig's base) to provide 49.
  • Compound 49 can then be further transformed into imidazole 50 via reacting with ammonium acetate under thermal or microwave conditions.
  • 51 can be directly reacted with an appropriately substituted amino acid in the presence of a base such as sodium bicarbonate or potassium carbonate providing 52 which can in turn be reacted with ammonium acetate under thermal or microwave conditions to provide 50.
  • Imidazole 50 can be protected with an alkoxylmethyl group by treatment with the appropriate alkoxymethyl halide such as 2-(trimethylsilyl)ethoxymethyl chloride after first being deprotonated with a strong base such as sodium hydride.
  • Substituted Phenylglycine derivatives can be prepared by a number of methods shown below.
  • Phenylglycine t-butyl ester can be reductively alkylated (pathyway A) with an appropriate aldehyde and a reductant such as sodium cyanoborohydride in acidic medium.
  • Hydrolysis of the t-butyl ester can be accomplished with strong acid such as HCl or trifluoroacetic acid.
  • phenylglycine can be alkylated with an alkyl halide such as ethyl iodide and a base such as sodium bicarbonate or potassium carbonate (pathway B).
  • Pathway C illustrates reductive alkylation of phenylglycine as in pathway A followed by a second reductive alkylation with an alternate aldehyde such as formaldehyde in the presence of a reducing agent and acid.
  • Pathway D illustrates the synthesis of substituted phenylglycines via the corresponding mandelic acid analogs. Conversion of the secondary alcohol to a competent leaving group can be accomplished with p- toluensulfonyl chloride. Displacement of the tosylate group with an appropriate amine followed by reductive removal of the benzyl ester can provide substituted phenylglycine derivatives.
  • pathway E a racemic substituted phenylglycine derivative is resolved by esterification with an enantiomerically pure chiral auxiliary such as but not limited to (+)-l-phenylethanol, (-)- 1 -phenylethanol, an Evan's oxazolidinone, or enantiomerically pure pantolactone. Separation of the diastereomers is accomplished via chromatography (silica gel, HPLC, crystallization, etc) followed by removal of the chiral auxiliary providing enantiomerically pure phenylglycine derivatives.
  • Pathway H illustrates a synthetic sequence which intersects with pathway E wherein the aforementioned chiral auxiliary is installed prior to amine addition.
  • an ester of an arylacetic acid can be brominated with a source of bromonium ion such as bromine, N-bromosuccinimide, or CBr 4 .
  • the resultant benzylic bromide can be displaced with a variety of mono- or disubstituted amines in the presence of a tertiary amine base such as triethylamine or Hunig's base.
  • Hydrolysis of the methyl ester via treatment with lithium hydroxide at low temperature or 6N HCl at elevated temperature provides the substituted phenylglycine derivatives. Another method is shown in pathway G.
  • Glycine analogs can be derivatized with a variety of aryl halides in the presence of a source of palladium (0) such as palladium bis(tributylphosphine) and base such as potassium phosphate. The resultant ester can then be hydrolyzed by treatment with base or acid. It should be understood that other well known methods to prepare phenylglycine derivatives exist in the art and can be amended to provide the desired compounds in this description. It should also be understood that the final phenylglycine derivatives can be purified to enantiomeric purity greater than 98%ee via preparative HPLC.
  • acylated phenylglycine derivatives may be prepared as illustrated below.
  • Phenylglycine derivatives wherein the carboxylic acid is protected as an easily removed ester may be acylated with an acid chloride in the presence of a base such as triethylamine to provide the corresponding amides (pathway A).
  • Pathway B illustrates the acylation of the starting phenylglycine derivative with an appropriate chloroformate
  • pathway C shows reaction with an appropriate isocyanate or carbamoyl chloride.
  • Each of the three intermediates shown in pathways A - C may be deprotected by methods known by those skilled in the art (ie; treatment of the t-butyl ester with strong base such as HCl or trifluoroacetic acid).
  • Amino-substituted phenylacetic acids may be prepared by treatment of a chloromethylphenylacetic acid with an excess of an amine.
  • Solvent A 95% H 2 O: 5% CH 3 CN, 10 mm Ammonium acetate
  • TFA salt oi Cap-6 was synthesized from (R)-2-phenylglycine and 1- bromo-2-(2-bromoethoxy)ethane by using the method of preparation of Cap-5. 1 H
  • the enantiomeric separation of the intermediate benzyl 2-(A- hydroxypiperidin-l-yl)-2 -phenyl acetate was effected by employing the following conditions: the compound (500 mg) was dissolved in ethanol/heptane (5 mL/45 mL). The resulting solution was injected (5 mL/injection) on a chiral HPLC column (Chiracel OJ, 2 cm ID x 25 cm L, 10 ⁇ m) eluting with 80:20 heptane/ethanol at 10 mL/min, monitored at 220 nm, to provide 186.3 mg of enantiomer- 1 and 209.1 mg of enantiomer-2 as light-yellow viscous oils.
  • the diastereomeric separation of the intermediate benzyl 2-((S)-3- fluoropyrrolidin-l-yl)-2-phenylacetate was effected by employing the following conditions: the ester (220 mg) was separated on a chiral HPLC column (Chiracel OJ- H, 0.46 cm ID x 25 cm L, 5 ⁇ m) eluting with 95% CO 2 / 5% methanol with 0.1% TFA, at 10 bar pressure, 70 mL/min flow rate, and a temperature of 35 0 C.
  • Step 1 A mixture of (R)-(-)-D-phenylglycine tert-butyl ester (3.00 g, 12.3 mmol), NaBH 3 CN (0.773 g, 12.3 mmol), KOH (0.690 g, 12.3 mmol) and acetic acid (0.352 mL, 6.15 mmol) were stirred in methanol at 0 0 C. To this mixture was added glutaric dialdehyde (2.23 mL, 12.3 mmol) dropwise over 5 minutes. The reaction mixture was stirred as it was allowed to warm to ambient temperature and stirring was continued at the same temperature for 16 hours.
  • Step 2 To a stirred solution of the intermediate ester (1.12g, 2.88mmol) in dichloromethane (10 mL) was added TFA (3 mL). The reaction mixture was stirred at ambient temperature for 4 hours and then it was concentrated to dryness to give a light yellow oil. The oil was purified using reverse-phase preparative HPLC (Primesphere C- 18, 30 x 100mm; CH 3 CN-H 2 O-0.1% TFA). The appropriate fractions were combined and concentrated to dryness in vacuo. The residue was then dissolved in a minimum amount of methanol and applied to applied to MCX LP extraction cartridges (2 x 6 g).
  • Step 1; (S)-l-Phenylethyl 2-bromo-2-phenylacetate To a mixture of ⁇ - bromophenylacetic acid (10.75 g, 0.050 mol), (S)-(-)- 1 -phenylethanol (7.94 g, 0.065 mol) and DMAP (0.61 g, 5.0 mmol) in dry dichloromethane (100 mL) was added solid EDCI (12.46 g, 0.065 mol) all at once.
  • Step 2 (S)- 1 -Phenylethyl (R)-2-(4-hydroxy-4-methylpiperidin- 1 -yl)- 2- phenylacetate: To a solution of (S)-I -phenylethyl 2-bromo-2-phenylacetate (0.464 g, 1.45 mmol) in THF (8 mL) was added triethylamine (0.61 mL, 4.35 mmol), followed by tetrabutylammonium iodide (0.215 g, 0.58 mmol).
  • reaction mixture was stirred at room temperature for 5 minutes and then a solution of 4-methyl-4- hydroxypiperidine (0.251 g, 2.18 mmol) in THF (2 mL) was added. The mixture was stirred for 1 hour at room temperature and then it was heated at 55-60 0 C (oil bath temperature) for 4 hours. The cooled reaction mixture was then diluted with ethyl acetate (30 mL), washed (H 2 O x2, brine), dried (MgSO 4 ), filtered and concentrated.
  • Step 2 (R)-((S)-1-Phenylethyl) 2-(2-fluorophenyl)-2-(piperidin-l-yl)acetate: To a solution of (S)-I -phenylethyl 2-(2-fluorophenyl)acetate (5.00 g, 19.4 mmol) in THF (1200 mL) at 0 0 C was added DBU (6.19 g, 40.7 mmol) and the solution was allowed to warm to room temperature while stirring for 30 minutes.
  • Wavelength 220
  • Solvent A 10% methanol - 90% H 2 O - 0.1% TFA
  • Solvent B 90% methanol - 10% H 2 O - 0.1% TFA
  • Wavelength 220
  • Solvent A 10% methanol - 90% H 2 O - 0.1% TFA
  • Solvent B 90% methanol - 10% H 2 O - 0.1% TFA
  • Step 1; (R,S)-Ethyl 2-(4-pyridyl)-2-bromoacetate To a solution of ethyl 4- pyridylacetate (1.00 g, 6.05 mmol) in dry THF (150 mL) at 0 0 C under argon was added DBU (0.99 mL, 6.66 mmol). The reaction mixture was allowed to warm to room temperature over 30 minutes and then it was cooled to -78 0 C. To this mixture was added CBr 4 (2.21 g, 6.66 mmol) and stirring was continued at -78 0 C for 2 hours. The reaction mixture was then quenched with sat. aq. NH 4 Cl and the phases were separated.
  • Step 2 (R,S)-Ethyl 2-(4-pyridyl)-2-(N,N-dimethylamino)acetate: To a solution of (R,S)-ethyl 2-(4-pyridyl)-2-bromoacetate (1.40 g, 8.48 mmol) in DMF (10 mL) at room temperature was added dimethylamine (2M in THF, 8.5 mL, 17.0 mmol).
  • Step 2; (R)-2-(dimethylamino)-2-(2-fluorophenyl)acetic acid A mixture of (RH(S)- 1-phenylethyl) 2-(dimethylamino)-2-(2-fluorophenyl)acetate TFA salt (1.25 g, 3.01 mmol) and 20% Pd(OH) 2 /C (0.125 g) in ethanol (30 mL) was hydrogenated at room temperature and atmospheric pressure (H 2 balloon) for 4 hours. The solution was then purged with Ar, filtered through diatomaceous earth (Celite ® ), and concentrated in vacuo. This gave the title compound as a colorless solid (0.503 g, 98%).
  • the S-isomer could be obtained from (S)-((S)- 1-phenylethyl) 2- (dimethylamino)-2-(2-fluorophenyl)acetate TFA salt in similar fashion.
  • HMDS (1.85 mL, 8.77 mmol) was added to a suspension of (R)-2-amino-2- phenylacetic acid p-toluenesulfonate (2.83 g, 8.77 mmol) in CH2CI2 (10 mL) and the mixture was stirred at room temperature for 30 minutes. Methyl isocyanate (0.5 g, 8.77 mmol) was added in one portion stirring continued for 30 minutes. The reaction was quenched by addition of H 2 O (5 mL) and the resulting precipitate was filtered, washed with H 2 O and n-hexanes, and dried under vacuum.
  • Step 1; (R)-tert-butyl 2-(3,3-dimethylureido)-2-phenylacetate To a stirred solution of (R)-tert-butyl-2-amino-2-phenylacetate (1.0 g, 4.10 mmol) and Hunig's base (1.79 mL, 10.25 mmol) in DMF (40 mL) was added dimethylcarbamoyl chloride (0.38 mL, 4.18 mmol) dropwise over 10 minutes. After stirring at room temperature for 3 hours, the reaction was concentrated under reduced pressure and the resulting residue was dissolved in ethyl acetate. The organic layer was washed with H 2 O, IN aq.
  • Step 2 (R)-2-(3,3-dimethylureido)-2-phenylacetic acid: To a stirred solution of ((R)-tert-butyl 2-(3,3-dimethylureido)-2-phenylacetate ( 0.86 g, 3.10 mmol) in CH 2 Cl 2 (250 mL) was added TFA (15 mL) dropwise and the resulting solution was stirred at rt for 3 h. The desired compound was then precipitated out of solution with a mixture of EtOAC:Hexanes (5:20), filtered off and dried under reduced pressure.
  • Step 1; (R)-tert-butyl 2-(3-cyclopentylureido)-2-phenylacetate To a stirred solution of (R)-2-amino-2-phenylacetic acid hydrochloride (1.0 g, 4.10 mmol) and Hunig's base (1.0 mL, 6.15 mmol) in DMF (15 mL) was added cyclopentyl isocyanate (0.46 mL, 4.10 mmol) dropwise and over 10 minutes. After stirring at room temperature for 3 hours, the reaction was concentrated under reduced pressure and the resulting residue was traken up in ethyl acetate.
  • C ⁇ p-52 was synthesized from L-alanine according to the procedure described for the synthesis of C ⁇ p-51.
  • a portion of the crude material was purified by a reverse phase HPLC (H 2 O/MeOH/TFA) to afford C ⁇ p-52 as a colorless viscous oil.
  • Cap-53 to -64 were prepared from appropriate starting materials according to the procedure described for the synthesis of Cap-51 , with noted modifications if any.
  • Methyl chloroformate (0.65 mL, 8.39 mmol) was added dropwise over 5 min to a cooled (ice-water) mixture OfNa 2 CO 3 (0.449 g, 4.23 mmol), NaOH (8.2 mL of 1M/H 2 O, 8.2 mmol) and (5 * )-3-hydroxy-2-(methoxycarbonylamino)-3- methylbutanoic acid (1.04 g, 7.81 mmol).
  • the reaction mixture was stirred for 45 min, and then the cooling bath was removed and stirring was continued for an additional 3.75 hr.
  • Methyl chloroformate (0.38 ml, 4.9 mmol) was added drop-wise to a mixture of IN NaOH (aq) (9.0 ml, 9.0 mmol), IM NaHCO 3 (aq) (9.0 ml, 9.0 mol), L-aspartic acid ⁇ -benzyl ester (1.0 g, 4.5 mmol) and Dioxane (9 ml).
  • the reaction mixture was stirred at ambient conditions for 3 hr, and then washed with Ethyl acetate (50 ml, 3x).
  • the aqueous layer was acidified with 12N HCl to a pH ⁇ 1-2, and extracted with ethyl acetate (3 x 50 ml).
  • Cap-69a and -69b Cap-69a: (R)-enantiomer
  • Cap-69b (S)-enantiomer
  • NaCNBH 3 (2.416 g, 36.5 mmol) was added in batches to a chilled (-15 "C) water (17 mL)/MeOH (10 mL) solution of alanine (1.338 g, 15.0 mmol). A few minutes later acetaldehyde (4.0 mL, 71.3 mmol) was added drop-wise over 4 min, the cooling bath was removed, and the reaction mixture was stirred at ambient condition for 6 hr. An additional acetaldehyde (4.0 mL) was added and the reaction was stirred for 2 hr. Concentrated HCl was added slowly to the reaction mixture until the pH reached ⁇ 1.5, and the resulting mixture was heated for 1 hr at 40 °C.
  • Cap-70 to -74x were prepared according to the procedure described for the synthesis of Cap-69 by employing appropriate starting materials.
  • Cap-75
  • Methyl chloroformate (0.36 mL, 4.65 mmol) was added drop-wise over 11 min to a cooled (ice-water) mixture OfNa 2 CO 3 (0.243 g, 2.29 mmol), NaOH (4.6 mL of 1 MTH 2 O, 4.6 mmol) and the above product (802.4 mg).
  • the reaction mixture was stirred for 55 min, and then the cooling bath was removed and stirring was continued for an additional 5.25 hr.
  • the reaction mixture was diluted with equal volume of water and washed with CH 2 Cl 2 (30 mL, 2x), and the aqueous phase was cooled with ice-water bath and acidified with concentrated HCl to a pH region of 2.
  • CapSOa S/S-diastereomer
  • Cap-80b S/R-diastereomer
  • LiHMDS (9.2 mL of 1.0 M/THF, 9.2 mmol) was added drop-wise over 10 min to a cooled (-78 "C) THF (50 mL) solution of (S)-I -benzyl 4-methyl 2-(9- phenyl-9H-fluoren-9-ylamino)succinate (3.907 g, 8.18 mmol) and stirred for ⁇ 1 hr.
  • MeI (0.57 mL, 9.2 mmol) was added drop-wise over 8 min to the mixture, and stirring was continued for 16.5 hr while allowing the cooling bath to thaw to room temperature.
  • reaction mixture was removed from the cooling bath and rapidly poured into ⁇ 1M H3PO4/H2O (250 mL) with stirring, and the mixture was extracted with ether (100 mL, 2x). The combined organic phase was washed with brine, dried (MgSO 4 ), filtered and concentrated in vacuo.
  • a balloon of hydrogen was attached to a mixture of (2S,3S)-benzyl 4-(tert- butyldimethylsilyloxy)-3-methyl-2-(9-phenyl-9H-fluoren-9-ylamino)butanoate (836 mg, 1.447 mmol) and 10% Pd/C (213 mg) in EtOAc (16 mL) and the mixture was stirred at room temperature for ⁇ 21 hr, where the balloon was recharged with H 2 as necessary.
  • reaction mixture was diluted with CH 2 Cl 2 and filtered through a pad of diatomaceous earth (Celite-545 R ), and the pad was washed with EtOAc (200 mL), EtOAc/MeOH (1 : 1 mixture, 200 mL) and MeOH (750 mL).
  • EtOAc 200 mL
  • EtOAc/MeOH 1 : 1 mixture, 200 mL
  • MeOH 750 mL
  • the combined organic phase was concentrated, and a silica gel mesh was prepared from the resulting crude material and submitted to a flash chromatography (8:2: 1 mixture of EtOAc/i- PrOH/H 2 O) to afford (2S,3S)-2-amino-4-(tert-butyldimethylsilyloxy)-3- methylbutanoic acid as a white fluffy solid (325 mg).
  • (2S,3R)-benzyl 4-(tert- butyldimethylsilyloxy)-3 -methyl-2-(9-phenyl-9H-fluoren-9-ylamino)butanoate was similarly elaborated to (2S,3R)-2-amino-4-(tert-butyldimethylsilyloxy)-3- methylbutanoic acid.
  • Cap-%2 to Cap-85 were synthesized from appropriate starting materials according to the procedure described for Cap-51.
  • the samples exhibited similar spectral profiles as that of their enantiomers (i.e., Cap-4, Cap- 13, Cap-51 and Cap- 52, respectively)
  • the slurry was allowed to stand for 20 min and loaded onto a pad of cation exchange resin (Strata) (ca. 25g).
  • the pad was washed with H 2 O (200 mL), MeOH (200 mL), and then NH 3 (3 M in MeOH, 2X200 mL).
  • the appropriate fractions was concentrated in vacuo and the residue (ca. 1.1 g) was dissolved in H 2 O, frozen and lyophyllized.
  • the title compound was obtained as a foam (1.02 g, 62%).
  • Cap-90 was prepared according to the method described for the preparation of Cap-l. The crude material was used as is in subsequent steps. LCMS: Anal. Calcd. for C H H I5 NO 2 : 193; found: 192 (M-H) " .
  • caps Cap-I ll to Cap-123 the Boc amino acids were commercially available and were deprotected by treatment with 25% TFA in CH 2 Cl 2 . After complete reaction as judged by LCMS the solvents were removed in vacuo and the corresponding TFA salt of the amino acid was carbamoylated with methyl chloro formate according to the procedure for Cap-51.
  • Cap- 125 was prepared according to the procedure for the preparation of C ⁇ p-l. The crude product was used as is in subsequent reactions.
  • Cap- 127 was prepared according to the method for Cap- 126 above starting from (S)- 2-amino-3 -(I -methyl- lH-imidazol-4-yl)propanoic acid (1.11 g, 6.56 mmol), NaHCO 3 (1.21 g, 14.4 mmol) and ClCO 2 Me (0.56 mL, 7.28 mmol). The title compound was obtained as its HCl salt (1.79 g, >100%) contaminated with inorganic salts. LCMS and 1 H NMR showed the presence of ca. 5% of the methyl ester. The crude mixture was used as is without further purification.
  • cap-129 (S)-2-(benzyloxycarbonylamino)-3-(lH-pyrazol-l-yl)propanoic acid (0.20 g, 0.70 mmol) was hydrogenated in the presence of Pd-C (45 mg) in MeOH (5 mL) at atmospheric pressure for 2h. The product appeared to be insoluble in MeOH, therefore the rxn mixture was diluted with 5mL H 2 O and a few drops of 6N HCl.
  • Cap- 130 was prepared by acylation of commercially available (R)-phenylglycine analgous to the procedure given in: Calmes, M.; Daunis, J.; Jacquier, R.; Verducci, J. Tetrahedron, 1987, 43(10), 2285.
  • Solution percentages express a weight to volume relationship, and solution ratios express a volume to volume relationship, unless stated otherwise.
  • Nuclear magnetic resonance (NMR) spectra were recorded either on a Bruker 300, 400, or 500 MHz spectrometer; the chemical shifts ( ⁇ ) are reported in parts per million. Flash chromatography was carried out on silica gel (Si ⁇ 2 ) according to Still's flash chromatography technique (J. Org. Chem. 1978, 43, 2923).
  • Solvent A 0.1% TFA in 10% methanol/90%H 2 O
  • Solvent B 0.1% TFA in 90% methanol/10% H 2 O
  • Solvent A 0.1% TFA in 10% methanol/90%H 2 O
  • Solvent B 0.1% TFA in 90% methanol/10% H 2 O
  • Solvent A 0.1% TFA in 10% methanol/90%H 2 O
  • Solvent B 0.1% TFA in 90% methanol/10% H 2 O
  • N,N-Diisopropylethylamine (18 mL, 103.3 mmol) was added dropwise, over 15 minutes, to a heterogeneous mixture ofN-Boc-L-proline (7.139 g, 33.17 mmol), HATU (13.324 g, 35.04 mmol), the HCl salt of 2-amino-l-(4-bromophenyl)ethanone (8.127 g, 32.44 mmol), and DMF (105 mL), and stirred at ambient condition for 55 minutes. Most of the volatile component was removed in vacuo, and the resulting residue was partitioned between ethyl acetate (300 mL) and water (200 mL).
  • Analogous compounds such as intermediate 1-la to 1-5 a can be prepared by incorporating the appropriately substituted amino acid and aryl bromide isomer.
  • ketoamide Ia (12.8 g, 31.12 mmol) and NH 4 OAc (12.0 g, 155.7 mmol) in xylenes (155 mL) was heated in a sealed tube at 140 0 C for 2 hours.
  • the volatile component was removed in vacuo, and the residue was partitioned carefully between ethyl acetate and water, whereby enough saturated NaHCO 3 solution was added so as to make the pH of the aqueous phase slightly basic after the shaking of the biphasic system.
  • the layers were separated, and the aqueous layer was extracted with an additional ethyl acetate.
  • the combined organic phase was washed with brine, dried (MgSO 4 ), filtered, and concentrated in vacuo.
  • Analogous compounds such as intermediates 1-lb to l-4b can be prepared by incorporating the appropriate ketoamide.
  • Pd(Pli3P) 4 (469 mg, 0.406 mmol) was added to a pressure tube containing a mixture of bromide Ib (4.008 g, 10.22 mmol), bis(pinacolato)diboron (5.422 g, 21.35 mmol), potassium acetate (2.573g, 26.21 mmol) and 1,4-dioxane (80 mL).
  • the reaction flask was purged with nitrogen, capped and heated with an oil bath at 80 0 C for 16.5 hours.
  • the reaction mixture was filtered and the filtrate was concentrated in vacuo.
  • Analogous compounds such as intermediates 1-lc to l-4c can be prepared by incorporating the appropriate aryl bromide.
  • Example 1 (IR, 1 'R)-2, 2 '-(4,4'-biphenyldiylbis(lH-imidazole-5, 2-diyl(2S)-2, 1- pyrrolidinediyl))bis(N,N-dimethyl-2-oxo-l-phenylethanamine) HATU (44.6 mg, 0.117 mmol) was added to a mixture of pyrrolidine Ie (22.9 mg, 0.054 mmol), diisopropylethylamine (45 ⁇ L, 0.259 mmol) and Cap-l (28.1 mg, 0.13 mmol) in DMF (1.5 mL), and the resulting mixture was stirred at ambient for 90 minutes.
  • the volatile component was removed in vacuo, and the residue was purified first by MCX ( methanol wash; 2.0 M NHymethanol elution) and then by a reverse phase HPLC system (H 2 ⁇ /methanol/TFA) to provide the TFA salt of Example 1 as an off-white foam (44.1 mg).
  • Example 28 methyl ((lR)-2-oxo-l-phenyl-2-((2S)-2-(5-(4'-(2-((2S)-l-(phenylacetyl)-2- pyrrolidinyl)-lH-imidazol-5-yl)-4-biphenylyl)-lH-imidazol-2-yl)-l- pyrrolidinyl) ethyl) carbamate
  • HATU (19.868g, 52.25 mmol) was added to a heterogeneous mixture of N- Cbz-L- proline (12.436 g, 49.89 mmol) and the HCl salt of 2-amino-l-(4- bromophenyl) ethanone (12.157 g, 48.53 mmol) in DMF (156 mL).
  • the mixture was lowered in an ice-water bath, and immediately afterward NN-diisopropylethylamine (27 mL, 155 mmol) was added dropwise to it over 13 minutes. After the addition of the base was completed, the cooling bath was removed and the reaction mixture was stirred for an additional 50 minutes.
  • ketoamide 28a was a white solid (20.68 g).
  • Ketoamide 28a (10.723g, 24.08 mmol) was converted to 28b according to the procedure described for the synthesis of carbamate Ib, with the exception that the crude material was purified by flash chromatography (sample was loaded with eluting solvent; 50% ethyl acetate/hexanes). Bromide 28b was retrieved as an off- white foam (7.622 g).
  • 1 H NMR (DMSO-d 6 , ⁇ 2.5 ppm, 400 MHz): ⁇ 12.23/12.04/1 1.97 (m, IH), 7.73-6.96 (m, 10H), 5.1 1-4.85 (m, 3H), 3.61 (m, IH), 3.45 (m, IH), 2.33-184(m, 4H).
  • K 2 CO 3 (187.8 mg, 1.36 mmol) was added to a mixture of catalyst (10% Pd/C; 205.3 mg), carbamate 28c (1.018 g, ⁇ 1.5 mmol), methanol (20 mL) and 3 pipet- drops of water. A balloon Of H 2 was attached and the mixture was stirred for 6 hours. Then, additional catalyst (10% Pd/C, 100.8 mg) and K 2 CO 3 (101.8 mg, 0.738 mmol) were added and stirring continued for 3.5 hours. During the hydrogenation process, the balloon Of H 2 was changed at intervals three times. The reaction mixture was filtered through a pad of diatomaceous earth (Celite ® 521), and the filterate was removed in vacuo.
  • Example 28 step e tert-butyl (2S)-2-(5-(4'-(2-((2S)-l-((2R)-2-((methoxycarbonyl)amino)-2- phenylacetyl)-2-pyrrolidinyl)-lH-imidazol-5-yl)-4-biphenylyl)-lH-imidazol-2-yl)-l- pyrrolidinecarboxylate
  • Example 28 step/ methyl ((lR)-2-oxo-l-phenyl-2-((2S)-2-(5-(4'-(2-((2S)-2-pyrrolidinyl)-lH-imidazol-5- yl)-4-biphenylyl)-lH-imidazol-2-yl)-l-pyrrolidinyl)ethyl)carbamate
  • Step e HATU (316.6 mg, 0.833 mmol) was added to a DMF (7.0 mL) solution of pyrrolidine 28d (427 mg, 0.813 mmol), Cap-4 (177.6 mg, 0.849 mmol) and diisopropylethylamine (0.32 mL, 1.84 mmol), and the reaction mixture was stirred for 45 minutes. The volatile component was removed in vacuo, and the residue was partitioned between CH 2 Cl 2 (50 mL) and an aqueous medium (20 mL H 2 O + 1 mL saturated NaHCO 3 solution).
  • Step f Carbamate 28e was elaborated to amine 28f by employing the procedure described in the conversion of Id to Ie.
  • LC (Cond. 1): RT 1.49min; >98% homogeneity index.
  • Example 28 methyl ((lR)-2-oxo-l-phenyl-2-((2S)-2-(5-(4'-(2-((2S)-l-(phenylacetyl)-2- pyrrolidinyl)-lH-imidazol-5-yl)-4-biphenylyl)-lH-imidazol-2-yl)-l- pyrrolidinyl) ethyl) carbamate
  • keto-esters can be prepared in analogous fashion.
  • ketoester 121b (11.445 g, 3.39 mmol) and NH 4 OAc (2.93 g, 38.0 mmol) in xylenes (18 mL) was heated with a microwave at 140 0 C for 80 minutes. The volatile component was removed in vacuo, and the residue was carefully partitioned between CH 2 Cl 2 and water, where enough saturated NaHC ⁇ 3 solution was added to neutralize the aqueous medium. The aqueous phase was extracted with CH 2 Cl 2 , and the combined organic phase was dried (MgSO 4 ), filtered, and concentrated in vacuo.
  • PdCl 2 dppf-CH 2 Cl 2 (50.1 mg, 0.061 mmol) was added to a pressure tube containing a mixture of bromide 121c (538.3 mg, 1.325 mmol), bis(pinacolato)diboron (666.6 mg, 2.625 mmol), potassium acetate (365.8 mg, 3.727 mmol) and DMF (10 mL).
  • the reaction mixture was flushed with N 2 and heated at 80 0 C for 24.5 hours.
  • the volatile component was removed in vacuo and the residue was partitioned between CH 2 Cl 2 and water, where enough saturated NaHC ⁇ 3 solution was added to make the pH of the aqueous medium neutral.
  • the aqueous phase was extracted with CH 2 Cl 2 , and the combined organic phase was dried
  • Example 121 Step e and Example 121, Step/
  • Example 126-128 were prepared starting from bromide 28b and boronate
  • N-Bromosuccinimide (838.4 mg, 4.71 mmol) was added in batches, over 15 minutes, to a cooled (ice/water) CH 2 Cl 2 (20 mL) solution of imidazole 130a (1.0689 g, 4.504 mmol), and stirred at similar temperature for 75 minutes. The volatile component was removed in vacuo.
  • the crude material was purified by a reverse phase HPLC system (H 2 O/methanol/TFA) to separate bromide 130b from its dibromo-analog and the non-consumed starting material. The HPLC elute was neutralized with excess NH 3 /methanol and the volatile component was removed in vacuo.
  • Example 130 (TFA salt) was prepared from 130e and Cap-l according to the
  • Examples 131.1-1 through 131.1-2 were prepared in similar fashion to example 28 via the intermediacy of intermediate l-6e after appending Cap-4.
  • Cap-l was appended after the CBz carbamate was removed from l-6e with Pd/C/H 2 .
  • Example 131.1-2 methyl ((lR)-2-(methyl((lS)-l-(5-(4'-(2-((2S)-l-((2R)-2-phenyl-2-(l- piperidinyl)acetyl)-2-pyrrolidinyl)-lH-imidazol-5-yl)-4-biphenylyl)-lH-imidazol-2- yl)ethyl)amino)-2-oxo-l-phenylethyl)carbamate
  • Cap- 14 was appended after the CBz carbamate was removed from l-6e with Pd/C/H 2 .
  • Example 131.2 was prepared in similar fashion to example 131.1-1 and example 131.1-2 via the intermediacy of intermediate 1 -6e after appending Cap- 1.
  • Cap- 14 was appended after the CBz carbamate was removed with PdAZVH 2 .
  • t R 1.28 min
  • LRMS Anal. Calcd. for C 48 H 54 N 8 O 2 775.44; found: 775.45 (M+H) + .
  • Boc-L-proline (9.70 g, 45.06 mmol) was added in one batch to a heterogeneous mixture of crude 132a (15.4 g) and CH3CN (150 mL), and immediately afterward Et 3 N (13.0 mL, 93.2 mmol) was added drop-wise over 6 min. The reaction mixture was stirred for 50 min, the volatile component was removed in vacuo and the residue was partitioned between CH 2 Cl 2 and water.
  • ketoester 132b (1.318 g, 3.19 mmol) and NH 4 OAc (2.729 g, 35.4 mmol) in xylenes (18 mL) was heated with a microwave at 140 0 C for 90 min. The volatile component was removed in vacuo and the residue was partitioned between CH2CI2 and water, where enough saturated NaHCO 3 solution was added to neutralize the aqueous medium. The aqueous phase was extracted with CH 2 CI 2 , and the combined organic phase was dried (MgSO 4 ), filtered, and concentrated in vacuo. The resulting crude material was purified by a Biotage system (silica gel; 50%
  • Example 132 (H 2 O/MeOH/TFA) to afford the TFA salt of Example 132 as a yellow foam (39.2 mg).
  • Example 133-135 were prepared as TFA salts from 132e by using the same method of preparations as Example 132 and appropriate reagents.
  • PdCl 2 (Ph 3 P) 2 (257 mg, 0.367 mmol) was added to a dioxane (45 mL) solution of l-bromo-4-iodo-2-methylbenzene (3.01 g, 10.13 mmol) and tri-w-butyl(l- ethoxyvinyl)stannane (3.826 g, 10.59 mmol) and heated at 80 0 C for -17 hr.
  • the reaction mixture was treated with water (15 mL), cooled to ⁇ 0 0 C (ice/water), and then NBS (1.839 g, 10.3 mmol) was added in batches over 7 min.
  • ketoester 136b (11.445 g, 3.39 mmol) and NH 4 OAc (2.93 g, 38.0 mmol) in xylenes (18 mL) was heated with a microwave at 140 0 C for 80 min. The volatile component was removed in vacuo, and the residue was carefully partitioned between CH 2 Cl 2 and water, where enough saturated NaHC ⁇ 3 solution was added to neutralize the aqueous medium. The aqueous phase was extracted with CH 2 Cl 2 , and the combined organic phase was dried (MgSO 4 ), filtered, and concentrated in vacuo.
  • PdCl 2 dppf.CH 2 Cl 2 (50.1 mg, 0.061 mmol) was added to a pressure tube containing a mixture of bromide 136c (538.3 mg, 1.325 mmol), bis(pinacolato)diboron (666.6 mg, 2.625 mmol), KOAc (365.8 mg, 3.727 mmol) and DMF (10 mL).
  • the reaction mixture was flushed with N 2 and heated at 80 0 C for 24.5 hr.
  • the volatile component was removed in vacuo and the residue was partitioned between CH 2 Cl 2 and water, where enough saturated NaHC ⁇ 3 solution was added to make the pH of the aqueous medium neutral.
  • Biaryl 136e was prepared from bromide 132c and boronate 136d according to the coupling condition described for the preparation of biaryl 132d.
  • LC (Cond. Ia): RT 1.32 min; >90% homogeneity index
  • the deprotection of biaryl 136e was done according to the preparation of pyrrolidine 132e to afford 136f as a light yellow foam.
  • Example 136 (TFA salt) was synthesized from 136f according to the preparation of Example 132 from 132e. 1.05 min (Cond.1); >98%
  • Example 138 methyl ((lR)-2-((2S)-2-(5-(6-(4-(2-((2S)-l-((2R)-2-((methoxycarbonyl)amino)-2- phenylacetyl)-2-pyrrolidinyl)-lH-imidazol-5-yl)-2-methylphenyl)-3-pyridinyl)-lH- imidazol-2-yl)-l-pyrrolidinyl)-2-oxo-l-phenylethyl)carbamate
  • Example 138 was prepared similarly from pyrrolidine 136f and Cap-4. 1.60 min (Cond. 1); >98%
  • HATU 99.8 mg, 0.262 mmol
  • 132e 54.1 mg, 0.127 mmol
  • (R)-2-(?-butoxycarbonylamino)-2-phenylacetic acid 98.5 mg, 0.392 mmol
  • z ' -P ⁇ EtN 100 ⁇ L, 0.574 mol
  • the volatile component was removed in vacuo, and the residue was purified by a reverse phase HPLC (H 2 O/MeOH/TFA), where the HPLC elute was treated with excess 2.0 N NH 3 /MeOH before the removal of the volatile component in vacuo.
  • Example 140 methyl ((lR)-2-((2S)-2-(5-(4-(5-(2-((2S)-l-((2R)-2-(dimethylamino)-2-phenylacetyl)-
  • HATU (19.868g, 52.25 mmol) was added to a heterogeneous mixture of N-Cbz-L- proline (12.436 g, 49.89 mmol) and the HCl salt of 2-amino-l-(4-bromophenyl) ethanone (12.157 g, 48.53 mmol) in DMF (156 mL).
  • the mixture was lowered in an ice-water bath, and immediately afterward N,N-diisopropylethylamine (27 mL, 155 mmol) was added drop wise to it over 13 min. After the addition of the base was completed, the cooling bath was removed and the reaction mixture was stirred for an additional 50 min.
  • ketoamide 140a was a white solid (20.68 g).
  • Ketoamide 140a (10.723g, 24.08 mmol) was converted to 140b according to the procedure described for the synthesis of carbamate 132c, with the exception that the crude material was purified by flash chromatography (silica gel; 50%
  • Pd(Ph 3 P) 4 (208 mg, 0.180 mmol) was added to a pressure tube containing a mixture of bromide 140b (1.80 g, 4.22 mmol), bis(pinacolato)diboron (2.146 g, 8.45 mmol), KOAc (1.8 g, 11.0 mmol) and 1,4-dioxane (34 mL).
  • the reaction flask was purged with nitrogen, capped and heated with an oil bath at 80 0 C for 23 hr. The volatile component was removed in vacuo, and the residue was partitioned carefully between CH 2 CI 2 (70 mL) and an aqueous medium (22 mL water + 5 mL saturated NaHCO 3 solution).
  • Arylbromide 132c was coupled with boronate 140c to afford 14Od by using the same procedure described for the synthesis of biaryl 132d.
  • the sample contains the desbromo version of 132c as an impurity. Proceeded to the next step without further purification.
  • LC (Cond. 1): RT 1.72 min; -85% homogeneity index
  • LC/MS Anal. Calcd.
  • Pyrrolidine 14Og was prepared from 14Oe and Cap-4, via the intermediacy of carbamate 14Of, by sequentially employing the amide forming and Boc-deprotection protocols used in the synthesis of Example 132.
  • LC (Cond. 1): RT 1.09 min; -94% homogeneity index
  • Example 140 methyl ((lR)-2-((2S)-2-(5-(4-(5-(2-((2S)-l-((2R)-2-(dimethylamino)-2-phenylacetyl)- 2-pyrrolidinyl)-lH-imidazol-5-yl)-2-pyridinyl)phenyl)-lH-imidazol-2-yl)-l- pyrrolidinyl)-2-oxo-l-phenylethyl)carbamate
  • Example 140 The TFA salt of Example 140 was synthesized from pyrrolidine 14Og and Cap ⁇ by using the procedure described for the preparation of Example 132 from intermediate 132e.
  • Example 141-143 The TFA salt of Example 141-143 were synthesized from intermediate 14Og and appropriate reagents in a similar manner.
  • Pd(Ph 3 P) 4 (9.6 mg, 0.008 mmol) and LiCl (28 mg, 0.67 mmol) were added to a mixture of arylbromide 132c (98.7 mg, 0.251 mmol) and hexamethylditin (51.6 mg, 0.158 mmol), and heated at 80 0 C for ⁇ 3 days.
  • the volatile component was removed in vacuo and the resultant crude material was purified by flash chromatography (silica gel; 0-10% MeOH/EtOAc) followed by a reverse phase HPLC (H 2 O/MeOH/TFA). The HPLC elute was neutralized with excess 2.0 N NH 3 MeOH, and the volatile component was removed in vacuo.
  • Example 145 (TFA salt) was synthesized from 145b according to the preparation of Example 132 from 132e.
  • LC (Cond. 1): RT 1.63 min; 98% homogeneity index
  • LC/MS Anal. Calcd. for [M+H] + C 44 H 45 Ni 0 O 6 : 809.35; found 809.40
  • HBr salt 48% HBr (1.0 mL) was added drop-wise to a dioxane (5.0 mL) solution of carbamate 146a (840 mg, 2.66 mmol) over 3 min, and the reaction mixture was stirred at ambient temperature for 17.5 hr. The precipitate was filtered and washed with dioxane, and dried in vacuo to afford amine the HBr salt of 146b as an off- white solid (672.4 mg; the exact mole equivalent of the HBr salt was not determined).
  • aqueous layer was extracted with CH 2 Cl 2 , and the combined organic phase was dried (MgSO 4 ), filtered, and concentrated in vacuo.
  • the crude material was purified by a flash chromatography (silica gel; 20% EtOAc/hexanes) to afford 146e as a colorless viscous oil (87.5 mg). The exact regiochemistry of 146e was not determined.
  • Example 146 (TFA salt) was synthesized from pyrrolidine 146g according to the preparation of Example 132 from intermediate 132e.
  • LC/MS Anal. Calcd. for [M+H] + C 45 H 50 N 9 O 2 : 748.41; found 748.57
  • HRMS Anal. Calcd. for [M+H] + C 45 H 50 N 9 O 2 : 748.4087; found 748.4100
  • Example 147 methyl ((lR)-2-((2S)-2-(5-(5-(4-(2-((2S)-l-((2R)-2-((methoxycarbonyl)amino)-2- phenylacetyl)-2-pyrrolidinyl)-lH-imidazol-5-yl)phenyl)-2-pyridinyl)-lH-imidazol-2- yl)-l-pyrrolidinyl)-2-oxo-l-phenylethyl)carbamate
  • Example 147 The TFA salt of Example 147 was prepared similarly from intermediate 146g by using Cap-4.
  • LC (Cond. 1): RT 1.66 min; 95% homogenity index
  • Example 148 Step a A solution of bromine (1.3mL, 25.0mmol) in 15mL glacial acetic acid was added drop-wise to a solution of 4-4'-diacetylbiphenyl (3.Og, 12.5mmol) in 4OmL acetic acid at 50 0 C. Upon completion of addition the mixture was stirred at room temperature overnight. The precipitated product was filtered off and re-crystallized from chloroform to give l,l '-(biphenyl-4,4'-diyl)bis(2-bromoethanone) (3.84g, 77.5%) as a white solid.

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Cited By (136)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2008144380A1 (en) * 2007-05-17 2008-11-27 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
WO2009020825A1 (en) * 2007-08-08 2009-02-12 Bristol-Myers Squibb Company Process for synthesizing compounds useful for treating hepatitis c
WO2009102318A1 (en) * 2008-02-12 2009-08-20 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
WO2009102325A1 (en) * 2008-02-13 2009-08-20 Bristol-Myers Squibb Company Imidazolyl biphenyl imidazoles as hepatitis c virus inhibitors
US7704992B2 (en) 2008-02-13 2010-04-27 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US7745636B2 (en) 2006-08-11 2010-06-29 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2010033977A3 (en) * 2008-09-22 2010-07-01 Cayman Chemical Company Multiheteroaryl compounds as inhibitors of h-pgds and their use for treating prostaglandin d2 mediated diseases
WO2010075376A2 (en) 2008-12-23 2010-07-01 Abbott Laboratories Anti-viral compounds
US7759495B2 (en) 2006-08-11 2010-07-20 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2010099527A1 (en) 2009-02-27 2010-09-02 Enanta Pharmaceuticals, Inc. Hepatitis c virus inhibitors
WO2010107739A2 (en) 2009-03-18 2010-09-23 The Board Of Trustees Of The Leland Stanford Junior University Methods and compositions of treating a flaviviridae family viral infection
WO2010117635A1 (en) * 2009-03-30 2010-10-14 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
WO2010132601A1 (en) * 2009-05-13 2010-11-18 Gilead Sciences, Inc. Antiviral compounds
WO2010138791A1 (en) * 2009-05-29 2010-12-02 Schering Corporation Antiviral compounds composed of three linked aryl moieties to treat diseases such as hepatitis c
WO2010138488A1 (en) * 2009-05-29 2010-12-02 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
WO2011004276A1 (en) * 2009-07-06 2011-01-13 Pfizer Limited Hepatitis c virus inhibitors
WO2011015657A1 (en) 2009-08-07 2011-02-10 Tibotec Pharmaceuticals Phenyl ethynyl derivatives as hepatitis c virus inhibitors
WO2011015658A1 (en) 2009-08-07 2011-02-10 Tibotec Pharmaceuticals Bis-benzimidazole derivatives as hepatitis c virus inhibitors
WO2011026920A1 (en) 2009-09-03 2011-03-10 Tibotec Pharmaceuticals Bis-benzimidazole derivatives
US7906655B2 (en) 2008-08-07 2011-03-15 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2011054834A1 (en) 2009-11-04 2011-05-12 Tibotec Pharmaceuticals Benzimidazole-imidazole derivatives
WO2011059850A1 (en) 2009-11-11 2011-05-19 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
WO2011059887A1 (en) 2009-11-11 2011-05-19 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
WO2011068941A2 (en) 2009-12-04 2011-06-09 National Health Research Institutes Proline derivatives
WO2011075607A1 (en) * 2009-12-18 2011-06-23 Intermune, Inc. Novel inhibitors of hepatitis c virus replication
WO2011072370A1 (en) 2009-12-18 2011-06-23 Boehringer Ingelheim International Gmbh Hcv combination therapy
WO2011075615A1 (en) * 2009-12-18 2011-06-23 Idenix Pharmaceuticals, Inc. 5,5-fused arylene or heteroarylene hepatitis c virus inhibitors
WO2011079327A1 (en) * 2009-12-24 2011-06-30 Vertex Pharmaceuticals Incorporated Analogues for the treatment or prevention of flavivirus infections
WO2011081918A1 (en) 2009-12-14 2011-07-07 Enanta Pharmaceuticals, Inc Hepatitis c virus inhibitors
WO2011091532A1 (en) * 2010-01-28 2011-08-04 Boehringer Ingelheim International Gmbh Hepatitis c inhibitor compounds
WO2011119858A1 (en) * 2010-03-24 2011-09-29 Vertex Pharmaceuticals Incorporated Analogues for the treatment or prevention of flavivirus infections
US8093243B2 (en) 2008-02-12 2012-01-10 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2012006060A1 (en) 2010-06-28 2012-01-12 Vertex Pharmaceuticals Incorporated Compounds and methods for the treatment or prevention of flavivirus infections
WO2012006055A2 (en) 2010-06-28 2012-01-12 Vertex Pharmaceuticals Incorporated Compounds and methods for the treatment or prevention of flavivirus infections
US8101643B2 (en) 2009-02-27 2012-01-24 Enanta Pharmaceuticals, Inc. Benzimidazole derivatives
WO2012013643A1 (en) 2010-07-26 2012-02-02 Tibotec Pharmaceuticals Hetero-bicyclic derivatives as hcv inhibitors
WO2012021591A1 (en) * 2010-08-12 2012-02-16 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
WO2012024363A2 (en) 2010-08-17 2012-02-23 Vertex Pharmaceuticals Incorporated Compounds and methods for the treatment or prevention of flaviviridae viral infections
US8138215B2 (en) 2009-05-29 2012-03-20 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8143414B2 (en) 2009-04-13 2012-03-27 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8143301B2 (en) 2009-04-09 2012-03-27 Bristol Myers Squibb Company Hepatitis C virus inhibitors
CN102395579A (zh) * 2009-02-17 2012-03-28 百时美施贵宝公司 丙型肝炎病毒抑制剂
US8147818B2 (en) 2008-02-13 2012-04-03 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
JP2012510525A (ja) * 2008-12-03 2012-05-10 プレシディオ ファーマシューティカルズ インコーポレイテッド Hcvns5aの阻害剤
US8178531B2 (en) 2010-02-23 2012-05-15 Enanta Pharmaceuticals, Inc. Antiviral agents
US8188132B2 (en) 2009-02-17 2012-05-29 Enanta Pharmaceuticals, Inc. Linked dibenzimidazole derivatives
WO2012027712A3 (en) * 2010-08-26 2012-06-21 Rfs Pharma, Llc Potent and selective inhibitors of hepatitis c virus
US8221737B2 (en) 2009-06-16 2012-07-17 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8242156B2 (en) 2009-02-17 2012-08-14 Enanta Pharmaceuticals, Inc. Linked dibenzimidazole derivatives
EP2494991A1 (en) 2007-05-04 2012-09-05 Vertex Pharmaceuticals Incorporated Combination therapy for the treatment of HCV infection
WO2012074437A3 (ru) * 2010-11-30 2012-09-13 Алла Хем, Ллс Замещенные азолы, противовирусный активный компонент, фармацевтическая композиция, способ получения и применения
JP2012526834A (ja) * 2009-05-12 2012-11-01 シェーリング コーポレイション ウイルス疾患治療に有用な縮合型三環式アリール化合物
US8303944B2 (en) 2006-08-11 2012-11-06 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
JP2012529534A (ja) * 2009-06-11 2012-11-22 アボット・ラボラトリーズ Hcv感染を治療するための抗ウィルス化合物
EP2398474A4 (en) * 2009-02-23 2012-12-05 Presidio Pharmaceuticals Inc HCV NS5A SHEMMER
US8329159B2 (en) 2006-08-11 2012-12-11 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8344155B2 (en) 2009-09-04 2013-01-01 Glaxosmith Kline Llc Chemical compounds
WO2012068234A3 (en) * 2010-11-17 2013-01-17 12Gilead Sciences, Inc. Antiviral compounds
US8362020B2 (en) 2009-12-30 2013-01-29 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2013016501A1 (en) 2011-07-26 2013-01-31 Vertex Pharmaceuticals Incorporated Formulations of thiophene compounds
WO2013016499A1 (en) 2011-07-26 2013-01-31 Vertex Pharmaceuticals Incorporated Methods for preparation of thiophene compounds
US8377980B2 (en) 2009-12-16 2013-02-19 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8383094B2 (en) 2008-10-01 2013-02-26 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2013030750A1 (en) 2011-09-01 2013-03-07 Lupin Limited Antiviral compounds
US8394968B2 (en) 2009-02-17 2013-03-12 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
JP2013510857A (ja) * 2009-11-12 2013-03-28 ブリストル−マイヤーズ スクイブ カンパニー C型肝炎ウイルス阻害剤
US8420686B2 (en) 2009-02-17 2013-04-16 Enanta Pharmaceuticals, Inc. Linked diimidazole antivirals
US8426458B2 (en) 2009-02-27 2013-04-23 Enanta Pharmaceuticals, Inc. Hepatitis C Virus inhibitors
JP2013515068A (ja) * 2009-12-22 2013-05-02 メルク・シャープ・アンド・ドーム・コーポレーション ウイルス性疾患の治療のための縮合三環式化合物およびその使用方法
RU2486181C2 (ru) * 2007-07-05 2013-06-27 Эррэй Биофарма Инк. Пиримидилциклопентаны как ингибиторы акт-протеинкиназ
WO2013098313A1 (en) 2011-12-28 2013-07-04 Janssen R&D Ireland Hetero-bicyclic derivatives as hcv inhibitors
WO2013098320A1 (en) 2011-12-28 2013-07-04 Janssen R&D Ireland Quinazolinone derivatives as hcv inhibitors
EP2528436A4 (en) * 2010-01-25 2013-07-10 Enanta Pharm Inc INHIBITORS OF HEPATITIS C VIRUS
US8507522B2 (en) 2009-03-06 2013-08-13 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
WO2013118097A1 (en) 2012-02-10 2013-08-15 Lupin Limited Antiviral compounds with a dibenzooxaheterocycle moiety
US8546405B2 (en) 2008-12-23 2013-10-01 Abbott Laboratories Anti-viral compounds
US8552047B2 (en) 2011-02-07 2013-10-08 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8575135B2 (en) 2011-11-16 2013-11-05 Gilead Sciences, Inc. Antiviral compounds
US8609648B2 (en) 2009-07-02 2013-12-17 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8623814B2 (en) 2010-02-23 2014-01-07 Enanta Pharmaceuticals, Inc. Antiviral agents
EP2682393A1 (en) * 2008-12-03 2014-01-08 Presidio Pharmaceuticals, Inc. Inhibitors of HCV NS5A comprising a bicyclic core.
US8629171B2 (en) 2007-08-08 2014-01-14 Bristol-Myers Squibb Company Crystalline form of methyl ((1S)-1-((25)-2-(5-(4'-(2-((25)-1((2S)-2-((methoxycarbonyl)amino)-3-methylbutanoyl)-2-pyrrolidinyl)-1H-imidazol-2-yl)-1-pyrrolidinyl)carbonyl)-2-methylpropyl)carbamate dihydrochloride salt
US8637561B2 (en) 2009-02-17 2014-01-28 Enanta Pharmaceuticals, Inc. Linked diimidazole derivatives
WO2014019344A1 (en) * 2012-08-03 2014-02-06 Sunshine Lake Pharma Co., Ltd. Bridged ring compounds as hepatitis c virus (hcv) inhibitors and pharmaceutical applications thereof
RU2507201C1 (ru) * 2013-02-07 2014-02-20 Александр Васильевич Иващенко Алкил [(s)-1-((s)-2-{5-[4-(4-{2-[(s)-1-((s)-2-метоксикарбониламино-3-метил-бутирил)-пирролидин-2-ил]-3н-имидазол-4-ил}-бута-1,3-диинил)-фенил]-1н-имидазол-2-ил}-пирролидин-1-карбонил)-2-метил-пропил]-карбамат нафталин-1,5-дисульфонат, фармацевтическая композиция, лекарственное средство, способ лечения вирусных заболеваний
US8673954B2 (en) 2009-02-27 2014-03-18 Enanta Pharmaceuticals, Inc. Benzimidazole derivatives
EP2621932A4 (en) * 2010-09-29 2014-03-26 Merck Sharp & Dohme TETRACYCLIC HETEROCYCLUS COMPOUNDS FOR THE TREATMENT OF HEPATITIS C VIRUS INFECTIONS
US8686026B2 (en) 2010-06-10 2014-04-01 Abbvie Inc. Solid compositions
US8697704B2 (en) 2010-08-12 2014-04-15 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8703938B2 (en) 2009-09-11 2014-04-22 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8709999B2 (en) 2009-03-27 2014-04-29 Presidio Pharmaceuticals, Inc. Substituted bicyclic HCV inhibitors
US8716454B2 (en) 2009-06-11 2014-05-06 Abbvie Inc. Solid compositions
EP2651927A4 (en) * 2010-12-15 2014-06-04 Abbvie Inc ANTIVIRAL CONNECTIONS
EP2651928A4 (en) * 2010-12-15 2014-06-18 Abbvie Inc ANTI-VIRAL COMPOUNDS
US8759332B2 (en) 2009-09-11 2014-06-24 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8765731B2 (en) 2009-07-16 2014-07-01 Vertex Pharmaceuticals Incorporated Benzimidazole analogues for the treatment or prevention of flavivirus infections
US8779156B2 (en) 2010-03-24 2014-07-15 Vertex Pharmaceuticals Incorporated Analogues for the treatment or prevention of flavivirus infections
US8778938B2 (en) 2010-06-04 2014-07-15 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8815928B2 (en) 2009-09-11 2014-08-26 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8822520B2 (en) 2010-09-22 2014-09-02 Presidio Pharmaceuticals, Inc. Substituted bicyclic HCV inhibitors
US8822700B2 (en) 2009-09-11 2014-09-02 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
WO2014134251A1 (en) 2013-02-28 2014-09-04 Vertex Pharmaceuticals Incorporated Pharmaceutical compositions
US8927739B2 (en) 2011-05-18 2015-01-06 Enanta Pharmaceuticals, Inc. Processes for the preparation of 5-azaspiro[2.4]heptane-6-carboxylic acid and its derivatives
US8927709B2 (en) 2009-09-11 2015-01-06 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8933110B2 (en) 2010-01-25 2015-01-13 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8937150B2 (en) 2009-06-11 2015-01-20 Abbvie Inc. Anti-viral compounds
US8999967B2 (en) 2010-09-29 2015-04-07 Presidio Pharmaceuticals, Inc. Tricyclic fused ring inhibitors of hepatitis C
US9034832B2 (en) 2011-12-29 2015-05-19 Abbvie Inc. Solid compositions
US9060971B2 (en) 2010-03-04 2015-06-23 Enanta Pharmaceuticals, Inc. Combination pharmaceutical agents as inhibitors of HCV replication
US9127021B2 (en) 2010-04-09 2015-09-08 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US9156818B2 (en) 2009-09-11 2015-10-13 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US9241942B2 (en) 2007-06-08 2016-01-26 Mannkind Corporation IRE-1α inhibitors
US9278922B2 (en) 2009-04-15 2016-03-08 Abbvie Inc. Anti-viral compounds
WO2016040225A1 (en) * 2014-09-09 2016-03-17 Bristol-Myers Squibb Company Phenyl-(aza)cycloalkyl carboxylic acid gpr120 modulators
US9326973B2 (en) 2012-01-13 2016-05-03 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9333204B2 (en) 2014-01-03 2016-05-10 Abbvie Inc. Solid antiviral dosage forms
US9364484B2 (en) 2011-12-06 2016-06-14 The Board Of Trustees Of The Leland Stanford Junior University Methods and compositions for treating viral diseases
US9394279B2 (en) 2009-06-11 2016-07-19 Abbvie Inc. Anti-viral compounds
US9546160B2 (en) 2011-05-12 2017-01-17 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9717712B2 (en) 2013-07-02 2017-08-01 Bristol-Myers Squibb Company Combinations comprising tricyclohexadecahexaene derivatives for use in the treatment of hepatitis C virus
US9765087B2 (en) 2009-02-27 2017-09-19 Enanta Pharmaceuticals, Inc. Benzimidazole derivatives
US9770439B2 (en) 2013-07-02 2017-09-26 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9775831B2 (en) 2013-07-17 2017-10-03 Bristol-Myers Squibb Company Combinations comprising biphenyl derivatives for use in the treatment of HCV
GB2552919A (en) * 2015-11-18 2018-02-21 Azad Pharmaceutical Ingredients Ag Stable amorphous form of daclatasvir
US10039779B2 (en) 2013-01-31 2018-08-07 Gilead Pharmasset Llc Combination formulation of two antiviral compounds
WO2018160090A1 (ru) 2017-02-28 2018-09-07 Александр Васильевич ИВАЩЕНКО Противовирусная композиция и способ ее применения
US10086011B2 (en) 2013-08-27 2018-10-02 Gilead Pharmasset Llc Combination formulation of two antiviral compounds
US10201584B1 (en) 2011-05-17 2019-02-12 Abbvie Inc. Compositions and methods for treating HCV
US10456414B2 (en) 2011-09-16 2019-10-29 Gilead Pharmasset Llc Methods for treating HCV
US10617675B2 (en) 2015-08-06 2020-04-14 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2020117849A1 (en) 2018-12-04 2020-06-11 Bristol-Myers Squibb Company Methods of analysis using in-sample calibration curve by multiple isotopologue reaction monitoring
US10800789B2 (en) 2012-05-16 2020-10-13 Gilead Pharmasset Llc Antiviral compounds
US11203599B2 (en) 2014-06-11 2021-12-21 Gilead Pharmasset Llc Solid forms of an antiviral compound
US11484534B2 (en) 2013-03-14 2022-11-01 Abbvie Inc. Methods for treating HCV
US12037340B2 (en) 2021-05-21 2024-07-16 Gilead Sciences, Inc. Pentacyclic derivatives as Zika virus inhibitors
US12497408B2 (en) 2022-05-19 2025-12-16 Gilead Sciences, Inc. Tetracyclic compounds and methods for the treatment of Zika virus infection

Families Citing this family (31)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US8729077B2 (en) * 2008-11-28 2014-05-20 Glaxosmithkline Llc Anti-viral compounds, compositions, and methods of use
US10752611B2 (en) 2009-02-27 2020-08-25 Enanta Pharmaceuticals, Inc. Benzimidazole derivatives
AU2010229795A1 (en) * 2009-03-27 2011-10-13 Presidio Pharmaceuticals, Inc. Fused ring inhibitors of hepatitis C
TWI476190B (zh) * 2009-03-30 2015-03-11 必治妥美雅史谷比公司 C型肝炎病毒抑制劑
AU2010253790A1 (en) 2009-05-29 2011-12-15 Merck Sharp & Dohme Corp. Antiviral compounds composed of three aligned aryl moieties to treat diseases such as Hepatitis C
WO2011031934A1 (en) * 2009-09-11 2011-03-17 Enanta Pharmaceuticals, Inc. Hepatitis c virus inhibitors
US20120276047A1 (en) 2009-11-25 2012-11-01 Rosenblum Stuart B Fused tricyclic compounds and derivatives thereof useful for the treatment of viral diseases
US20110137633A1 (en) * 2009-12-03 2011-06-09 Abbott Laboratories Anti-viral compounds and methods of identifying the same
BR112012022125A2 (pt) 2010-03-09 2016-11-01 Merck Sharp & Dhme Corp composto, sal de dicloridrato, composição farmacêutica, uso do composto, e, método para tratar um paciente
JP2013541499A (ja) 2010-07-26 2013-11-14 メルク・シャープ・エンド・ドーム・コーポレイション 置換されたビフェニレン化合物およびウイルス性疾患の治療のためのその使用方法
AU2011314168A1 (en) 2010-09-29 2013-04-04 Merck Sharp & Dohme Corp. Fused tetracycle derivatives and methods of use thereof for the treatment of viral diseases
JP5731004B2 (ja) 2010-10-26 2015-06-10 プレシディオ ファーマシューティカルズ インコーポレイテッド C型肝炎ウイルスの阻害剤
WO2012061552A1 (en) 2010-11-04 2012-05-10 Theravance, Inc. Novel inhibitors of hepatitis c virus
EP2655334B1 (en) 2010-12-22 2018-10-03 Eutropics Pharmaceuticals, Inc. Compositions and methods useful for treating diseases
EP2655362A1 (en) 2010-12-22 2013-10-30 Abbvie Inc. Hepatitis c inhibitors and uses thereof
WO2012122716A1 (en) * 2011-03-17 2012-09-20 Merck Sharp & Dohme Corp. Tetracyclic xanthene derivatives and methods of use thereof for treatment of viral diseases
FR2981071B1 (fr) * 2011-10-10 2014-02-07 Centre Nat Rech Scient Synthese versatile et stereospecifique d'acides amines gamma,delta-insatures par la reaction de wittig
EP2755981A4 (en) 2011-09-14 2015-03-25 Merck Sharp & Dohme SILICULAR HETEROCYCLIC DERIVATIVES AND METHOD FOR THEIR USE FOR THE TREATMENT OF VIRUS DISEASES
US8957048B2 (en) 2011-10-06 2015-02-17 Allergan, Inc. Compositions for the treatment of dry eye
BR112014010401A8 (pt) 2011-11-03 2017-12-19 Theravance Inc Inibidores do vírus da hepatite c rod-like que contêm o fragmento {2-[4-(bifenil-4-il)-1h-imidazo-2-il] pirrolidina-1-carbonilmetil}amina
US9907826B2 (en) 2011-12-07 2018-03-06 Allergan, Inc. Efficient lipid delivery to human tear film using a salt-sensitive emulsion system
HK1203356A1 (en) 2012-03-22 2015-10-30 艾丽奥斯生物制药有限公司 Pharmaceutical combinations comprising a thionucleotide analog
JP6069492B2 (ja) 2012-04-25 2017-02-01 セラヴァンス バイオファーマ アール&ディー アイピー, エルエルシー C型肝炎ウイルス阻害剤
WO2013163262A1 (en) 2012-04-25 2013-10-31 Theravance, Inc. Piperazine-piperidine compounds as hepatitis c virus inhibitors
CA2878621C (en) * 2012-07-10 2020-09-15 Ares Trading S.A. Pyrimidine pyrazolyl derivatives
CN103848818B (zh) 2012-11-29 2017-03-15 广东东阳光药业有限公司 作为丙型肝炎抑制剂的并环化合物、药物组合物及它们在药物中的应用
WO2014082379A1 (en) 2012-11-29 2014-06-05 Sunshine Lake Pharma Co.,Ltd. Spiro ring compound as hepatitis c virus (hcv) inhibitor and uses thereof field of the invention
US10167298B2 (en) 2013-10-30 2019-01-01 Merck Sharp & Dohme Corp. Pseudopolymorphs of an HCV NS5A inhibitor and uses thereof
WO2015089810A1 (en) 2013-12-20 2015-06-25 Merck Sharp & Dohme Corp. Fused tetracyclic heterocyclic compounds and methods of use thereof for the treatment of viral diseases
WO2015110048A1 (en) 2014-01-23 2015-07-30 Sunshine Lake Pharma Co., Ltd. Bridged ring compounds as hepatitis c virus inhibitors, pharmaceutical compositions and uses thereof
CN109456375B (zh) * 2018-12-11 2019-10-22 枣庄学院 一种抑制丙肝病毒的含单糖基杂环类化合物及制备方法

Family Cites Families (22)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5654451B1 (en) 1993-01-14 2000-02-22 Magainin Pharma Amino acids and peptides having modified c-terminals and modified n-terminals
EP0679153A4 (en) 1993-01-14 1996-05-15 Magainin Pharma FINALLY MODIFIED AMINO ACIDS AND PEPTIDES.
WO1998027108A2 (en) * 1996-12-16 1998-06-25 Fujisawa Pharmaceutical Co., Ltd. New amide compounds and their use as nitric oxide synthase inhibitors
US7244721B2 (en) * 2000-07-21 2007-07-17 Schering Corporation Peptides as NS3-serine protease inhibitors of hepatitis C virus
MXPA05000256A (es) 2002-07-01 2005-07-15 Upjohn Co Inhibidores de polimerasa ns5b del vhc.
EP1532118A2 (en) * 2002-07-05 2005-05-25 Axxima Pharmaceuticals Aktiengesellschaft Imidazole compounds for the treatment of hepatitis c virus infections
US7220745B2 (en) 2003-05-15 2007-05-22 Rigel Pharmaceuticals Heterocyclic compounds useful to treat HCV
US20050119318A1 (en) 2003-10-31 2005-06-02 Hudyma Thomas W. Inhibitors of HCV replication
GB0326168D0 (en) 2003-11-10 2003-12-17 Arrow Therapeutics Ltd Chemical compounds
KR20070011501A (ko) 2004-04-28 2007-01-24 애로우 쎄라퓨틱스 리미티드 항바이러스제로서 유용한 모르폴리닐아닐리노퀴나졸린유도체
WO2006022442A1 (ja) 2004-08-24 2006-03-02 Santen Pharmaceutical Co., Ltd. ジヒドロオロテートデヒドロゲナーゼ阻害活性を有する新規複素環アミド誘導体
WO2006093867A1 (en) 2005-02-28 2006-09-08 The Rockefeller University Structure of the hepatitits c virus ns5a protein
US8143288B2 (en) 2005-06-06 2012-03-27 Bristol-Myers Squibb Company Inhibitors of HCV replication
DK1940786T3 (da) 2005-09-16 2010-11-08 Arrow Therapeutics Ltd Biphenylderivater og deres anvendelse ved behandling af hepatitis C
WO2007058384A1 (en) 2005-11-17 2007-05-24 Osaka University Method of suppressing replication of hepatitis c virus, inhibitor of replication of the virus and method of screening for the same
EP1971611B1 (en) 2005-12-21 2012-10-10 Abbott Laboratories Anti-viral compounds
SG133452A1 (en) 2005-12-30 2007-07-30 Novartis Ag Peptide deformylase inhibitors for treatment of mycobacterial and other parasitic diseases
ATE508125T1 (de) 2006-01-11 2011-05-15 Arrow Therapeutics Ltd Triazoloanilinopyrimidinderivate zur verwendung als antivirale mittel
WO2007082554A1 (en) 2006-01-23 2007-07-26 Istituto Di Ricerche Di Biologia Molecolare P Angeletti Spa Modulators of hcv replication
CA2653924A1 (en) 2006-05-30 2007-12-06 Arrow Therapeutics Limited Biphenyl derivatives and their use in treating hepatitis c
US8329159B2 (en) 2006-08-11 2012-12-11 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US7759495B2 (en) 2006-08-11 2010-07-20 Bristol-Myers Squibb Company Hepatitis C virus inhibitors

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
None

Cited By (274)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US9758487B2 (en) 2006-08-11 2017-09-12 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8846023B2 (en) 2006-08-11 2014-09-30 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8329159B2 (en) 2006-08-11 2012-12-11 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9421192B2 (en) 2006-08-11 2016-08-23 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9018390B2 (en) 2006-08-11 2015-04-28 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8900566B2 (en) 2006-08-11 2014-12-02 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8642025B2 (en) 2006-08-11 2014-02-04 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US7745636B2 (en) 2006-08-11 2010-06-29 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8303944B2 (en) 2006-08-11 2012-11-06 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8288562B2 (en) 2006-08-11 2012-10-16 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US7759495B2 (en) 2006-08-11 2010-07-20 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9227961B2 (en) 2006-08-11 2016-01-05 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US10047056B2 (en) 2006-08-11 2018-08-14 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8492553B2 (en) 2006-08-11 2013-07-23 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
EP2494991A1 (en) 2007-05-04 2012-09-05 Vertex Pharmaceuticals Incorporated Combination therapy for the treatment of HCV infection
WO2008144380A1 (en) * 2007-05-17 2008-11-27 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
US7741347B2 (en) 2007-05-17 2010-06-22 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9981901B2 (en) 2007-06-08 2018-05-29 Fosun Orinove Pharmatech, Inc. IRE-1α inhibitors
US9546149B2 (en) 2007-06-08 2017-01-17 Mannkind Corporation IRE-1α inhibitors
US9241942B2 (en) 2007-06-08 2016-01-26 Mannkind Corporation IRE-1α inhibitors
RU2486181C2 (ru) * 2007-07-05 2013-06-27 Эррэй Биофарма Инк. Пиримидилциклопентаны как ингибиторы акт-протеинкиназ
WO2009020825A1 (en) * 2007-08-08 2009-02-12 Bristol-Myers Squibb Company Process for synthesizing compounds useful for treating hepatitis c
JP2013231072A (ja) * 2007-08-08 2013-11-14 Bristol Myers Squibb Co C型肝炎の治療に有用な化合物の合成方法
EA017173B1 (ru) * 2007-08-08 2012-10-30 Бристол-Маерс Сквибб Компани Способ синтеза соединений, пригодных для лечения гепатита с
US8629171B2 (en) 2007-08-08 2014-01-14 Bristol-Myers Squibb Company Crystalline form of methyl ((1S)-1-((25)-2-(5-(4'-(2-((25)-1((2S)-2-((methoxycarbonyl)amino)-3-methylbutanoyl)-2-pyrrolidinyl)-1H-imidazol-2-yl)-1-pyrrolidinyl)carbonyl)-2-methylpropyl)carbamate dihydrochloride salt
CN101778841B (zh) * 2007-08-08 2015-07-22 百时美-施贵宝爱尔兰控股公司 用于合成用于治疗丙型肝炎的化合物的方法
US7728027B2 (en) 2007-08-08 2010-06-01 Bristol-Myers Squibb Company Process for synthesizing compounds useful for treating hepatitis C
WO2009102318A1 (en) * 2008-02-12 2009-08-20 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
EA018782B1 (ru) * 2008-02-12 2013-10-30 Бристол-Маерс Сквибб Компани Ингибиторы вируса гепатита с
US8093243B2 (en) 2008-02-12 2012-01-10 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
EA018088B1 (ru) * 2008-02-13 2013-05-30 Бристол-Маерс Сквибб Компани Имидазолилбифенильные имидазолы в качестве ингибиторов вируса гепатита с
US7704992B2 (en) 2008-02-13 2010-04-27 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2009102325A1 (en) * 2008-02-13 2009-08-20 Bristol-Myers Squibb Company Imidazolyl biphenyl imidazoles as hepatitis c virus inhibitors
US8147818B2 (en) 2008-02-13 2012-04-03 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US7906655B2 (en) 2008-08-07 2011-03-15 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2010033977A3 (en) * 2008-09-22 2010-07-01 Cayman Chemical Company Multiheteroaryl compounds as inhibitors of h-pgds and their use for treating prostaglandin d2 mediated diseases
US8536185B2 (en) 2008-09-22 2013-09-17 Cayman Chemical Company, Incorporated Multiheteroaryl compounds as inhibitors of H-PGDS and their use for treating prostaglandin D2 mediated diseases
US9126973B2 (en) 2008-09-22 2015-09-08 Cayman Chemical Company, Incorporated Multiheteroaryl compounds as inhibitors of H-PGDS and their use for treating prostaglandin D2 mediated diseases
US8383094B2 (en) 2008-10-01 2013-02-26 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
EP2774927A1 (en) * 2008-12-03 2014-09-10 Presidio Pharmaceuticals, Inc. Inhibitors of HCV NS5A
US9120779B2 (en) 2008-12-03 2015-09-01 Presidio Pharmaceuticals, Inc. Inhibitors of HCV NS5A
KR101784830B1 (ko) * 2008-12-03 2017-10-16 프레시디오 파마슈티칼스, 인코포레이티드 Hcv ns5a의 억제제
EP2682393A1 (en) * 2008-12-03 2014-01-08 Presidio Pharmaceuticals, Inc. Inhibitors of HCV NS5A comprising a bicyclic core.
JP2012510525A (ja) * 2008-12-03 2012-05-10 プレシディオ ファーマシューティカルズ インコーポレイテッド Hcvns5aの阻害剤
US9249138B2 (en) 2008-12-23 2016-02-02 Abbvie Inc. Anti-viral compounds
US9163017B2 (en) 2008-12-23 2015-10-20 Abbvie Inc. Anti-viral compounds
US8541424B2 (en) 2008-12-23 2013-09-24 Abbott Laboratories Anti-viral compounds
US8546405B2 (en) 2008-12-23 2013-10-01 Abbott Laboratories Anti-viral compounds
WO2010075376A2 (en) 2008-12-23 2010-07-01 Abbott Laboratories Anti-viral compounds
US8242156B2 (en) 2009-02-17 2012-08-14 Enanta Pharmaceuticals, Inc. Linked dibenzimidazole derivatives
US8420686B2 (en) 2009-02-17 2013-04-16 Enanta Pharmaceuticals, Inc. Linked diimidazole antivirals
US8394968B2 (en) 2009-02-17 2013-03-12 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8809548B2 (en) 2009-02-17 2014-08-19 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
JP2012518000A (ja) * 2009-02-17 2012-08-09 ブリストル−マイヤーズ スクイブ カンパニー C型肝炎ウイルス阻害剤
US8188132B2 (en) 2009-02-17 2012-05-29 Enanta Pharmaceuticals, Inc. Linked dibenzimidazole derivatives
US8637561B2 (en) 2009-02-17 2014-01-28 Enanta Pharmaceuticals, Inc. Linked diimidazole derivatives
CN102395579A (zh) * 2009-02-17 2012-03-28 百时美施贵宝公司 丙型肝炎病毒抑制剂
EP2398474A4 (en) * 2009-02-23 2012-12-05 Presidio Pharmaceuticals Inc HCV NS5A SHEMMER
JP2012519185A (ja) * 2009-02-27 2012-08-23 エナンタ ファーマシューティカルズ インコーポレイテッド C型肝炎ウイルスインヒビター
US8673954B2 (en) 2009-02-27 2014-03-18 Enanta Pharmaceuticals, Inc. Benzimidazole derivatives
US8426458B2 (en) 2009-02-27 2013-04-23 Enanta Pharmaceuticals, Inc. Hepatitis C Virus inhibitors
US8101643B2 (en) 2009-02-27 2012-01-24 Enanta Pharmaceuticals, Inc. Benzimidazole derivatives
US9765087B2 (en) 2009-02-27 2017-09-19 Enanta Pharmaceuticals, Inc. Benzimidazole derivatives
WO2010099527A1 (en) 2009-02-27 2010-09-02 Enanta Pharmaceuticals, Inc. Hepatitis c virus inhibitors
US8507522B2 (en) 2009-03-06 2013-08-13 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
WO2010107739A2 (en) 2009-03-18 2010-09-23 The Board Of Trustees Of The Leland Stanford Junior University Methods and compositions of treating a flaviviridae family viral infection
US8709999B2 (en) 2009-03-27 2014-04-29 Presidio Pharmaceuticals, Inc. Substituted bicyclic HCV inhibitors
CN102448956B (zh) * 2009-03-30 2015-05-06 百时美施贵宝公司 丙型肝炎病毒抑制剂
JP2012522053A (ja) * 2009-03-30 2012-09-20 ブリストル−マイヤーズ スクイブ カンパニー C型肝炎ウイルス阻害剤
WO2010117635A1 (en) * 2009-03-30 2010-10-14 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
CN102448956A (zh) * 2009-03-30 2012-05-09 百时美施贵宝公司 丙型肝炎病毒抑制剂
EA022384B1 (ru) * 2009-03-30 2015-12-30 Бристол-Маерс Сквибб Компани Ингибиторы вируса гепатита c
US8796466B2 (en) 2009-03-30 2014-08-05 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8143301B2 (en) 2009-04-09 2012-03-27 Bristol Myers Squibb Company Hepatitis C virus inhibitors
US8143414B2 (en) 2009-04-13 2012-03-27 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
JP2012523457A (ja) * 2009-04-13 2012-10-04 ブリストル−マイヤーズ スクイブ カンパニー C型肝炎ウイルス阻害剤
US9278922B2 (en) 2009-04-15 2016-03-08 Abbvie Inc. Anti-viral compounds
JP2012526834A (ja) * 2009-05-12 2012-11-01 シェーリング コーポレイション ウイルス疾患治療に有用な縮合型三環式アリール化合物
EP3002281A1 (en) * 2009-05-13 2016-04-06 Gilead Pharmasset LLC Antiviral compounds
US9981955B2 (en) 2009-05-13 2018-05-29 Gilead Pharmasset Llc Antiviral compounds
CN104211713A (zh) * 2009-05-13 2014-12-17 吉里德科学公司 抗病毒化合物
EA026536B1 (ru) * 2009-05-13 2017-04-28 Джилид Фармассет Ллс Противовирусные соединения
EA027493B1 (ru) * 2009-05-13 2017-07-31 Джилид Фармассет Ллс Промежуточные соединения для получения противовирусного соединения
US8841278B2 (en) 2009-05-13 2014-09-23 Gilead Pharmasset Llc Antiviral compounds
CN104211713B (zh) * 2009-05-13 2017-04-12 吉利德制药有限责任公司 抗病毒化合物
JP2014169331A (ja) * 2009-05-13 2014-09-18 Gilead Sciences Inc 抗ウイルス化合物
EA021974B1 (ru) * 2009-05-13 2015-10-30 Джилид Фармассет Ллс Противовирусное соединение
EP3309157A1 (en) * 2009-05-13 2018-04-18 Gilead Pharmasset LLC Antiviral compounds
US8822430B2 (en) 2009-05-13 2014-09-02 Gilead Pharmasset Llc Antiviral compounds
EP2873665A1 (en) * 2009-05-13 2015-05-20 Gilead Pharmasset LLC Antiviral compounds
US9511056B2 (en) 2009-05-13 2016-12-06 Gilead Pharmasset Llc Antiviral compounds
US8088368B2 (en) 2009-05-13 2012-01-03 Gilead Sciences, Inc. Antiviral compounds
KR101503752B1 (ko) 2009-05-13 2015-03-18 길리애드 파마셋 엘엘씨 항바이러스 화합물
JP2019104732A (ja) * 2009-05-13 2019-06-27 ギリアド ファーマセット エルエルシー 抗ウイルス化合物
WO2010132601A1 (en) * 2009-05-13 2010-11-18 Gilead Sciences, Inc. Antiviral compounds
CN109020961A (zh) * 2009-05-13 2018-12-18 吉利德制药有限责任公司 抗病毒化合物
AP3622A (en) * 2009-05-13 2016-03-02 Gilead Sciences Inc Antiviral compounds
US8669234B2 (en) 2009-05-13 2014-03-11 Gilead Sciences, Inc. Antiviral compounds
US8273341B2 (en) 2009-05-13 2012-09-25 Gilead Sciences, Inc. Antiviral compounds
EP3626716A1 (en) * 2009-05-13 2020-03-25 Gilead Pharmasset LLC Antiviral compounds
EP2857394A1 (en) * 2009-05-13 2015-04-08 Gilead Pharmasset LLC Antiviral compounds
JP2012528166A (ja) * 2009-05-29 2012-11-12 ブリストル−マイヤーズ スクイブ カンパニー C型肝炎ウイルス阻害剤
WO2010138488A1 (en) * 2009-05-29 2010-12-02 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
WO2010138791A1 (en) * 2009-05-29 2010-12-02 Schering Corporation Antiviral compounds composed of three linked aryl moieties to treat diseases such as hepatitis c
US8138215B2 (en) 2009-05-29 2012-03-20 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
CN102459250B (zh) * 2009-05-29 2015-05-06 百时美施贵宝公司 丙型肝炎病毒抑制剂
US8211928B2 (en) 2009-05-29 2012-07-03 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
CN102459250A (zh) * 2009-05-29 2012-05-16 百时美施贵宝公司 丙型肝炎病毒抑制剂
JP2012529534A (ja) * 2009-06-11 2012-11-22 アボット・ラボラトリーズ Hcv感染を治療するための抗ウィルス化合物
US8937150B2 (en) 2009-06-11 2015-01-20 Abbvie Inc. Anti-viral compounds
US10028937B2 (en) 2009-06-11 2018-07-24 Abbvie Inc. Anti-viral compounds
JP2014144973A (ja) * 2009-06-11 2014-08-14 Avvi Bahamas Ltd Hcv感染を治療するための抗ウィルス化合物
US8921514B2 (en) 2009-06-11 2014-12-30 Abbvie Inc. Anti-viral compounds
US8691938B2 (en) 2009-06-11 2014-04-08 Abbvie Inc. Anti-viral compounds
US8716454B2 (en) 2009-06-11 2014-05-06 Abbvie Inc. Solid compositions
US10039754B2 (en) 2009-06-11 2018-08-07 Abbvie Inc. Anti-viral compounds
US9586978B2 (en) 2009-06-11 2017-03-07 Abbvie Inc. Anti-viral compounds
US9394279B2 (en) 2009-06-11 2016-07-19 Abbvie Inc. Anti-viral compounds
US8221737B2 (en) 2009-06-16 2012-07-17 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8609648B2 (en) 2009-07-02 2013-12-17 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
WO2011004276A1 (en) * 2009-07-06 2011-01-13 Pfizer Limited Hepatitis c virus inhibitors
US8765731B2 (en) 2009-07-16 2014-07-01 Vertex Pharmaceuticals Incorporated Benzimidazole analogues for the treatment or prevention of flavivirus infections
US8623899B2 (en) 2009-08-07 2014-01-07 Janssen Research & Development Ireland Bis-benzimidazole derivatives as hepatitis C virus inhibitors
US9045463B2 (en) 2009-08-07 2015-06-02 Janssen R&D Ireland Phenyl ethynyl derivatives as hepatitis C virus inhibitors
WO2011015658A1 (en) 2009-08-07 2011-02-10 Tibotec Pharmaceuticals Bis-benzimidazole derivatives as hepatitis c virus inhibitors
WO2011015657A1 (en) 2009-08-07 2011-02-10 Tibotec Pharmaceuticals Phenyl ethynyl derivatives as hepatitis c virus inhibitors
WO2011026920A1 (en) 2009-09-03 2011-03-10 Tibotec Pharmaceuticals Bis-benzimidazole derivatives
US8344155B2 (en) 2009-09-04 2013-01-01 Glaxosmith Kline Llc Chemical compounds
US9814699B2 (en) 2009-09-04 2017-11-14 Janssen Pharmaceuticals, Inc. Chemical compounds
US8492554B2 (en) 2009-09-04 2013-07-23 Glaxosmithkline Llc Chemical compounds
US8853416B2 (en) 2009-09-04 2014-10-07 Janssen Pharmaceuticals, Inc. Chemical compounds
US9150587B2 (en) 2009-09-04 2015-10-06 Janssen Pharmaceuticals, Inc. Chemical compounds
US8822700B2 (en) 2009-09-11 2014-09-02 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US9156818B2 (en) 2009-09-11 2015-10-13 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8927709B2 (en) 2009-09-11 2015-01-06 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8759332B2 (en) 2009-09-11 2014-06-24 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8815928B2 (en) 2009-09-11 2014-08-26 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8703938B2 (en) 2009-09-11 2014-04-22 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
WO2011054834A1 (en) 2009-11-04 2011-05-12 Tibotec Pharmaceuticals Benzimidazole-imidazole derivatives
US9433609B2 (en) 2009-11-04 2016-09-06 Janssen Sciences Ireland Uc Benzimidazole-imidazole derivatives
US9427428B2 (en) 2009-11-04 2016-08-30 Janssen Sciences Ireland Uc Benzimidazole-imidazole derivatives
WO2011059850A1 (en) 2009-11-11 2011-05-19 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
WO2011059887A1 (en) 2009-11-11 2011-05-19 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
US9006455B2 (en) 2009-11-11 2015-04-14 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9776981B2 (en) 2009-11-11 2017-10-03 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8618153B2 (en) 2009-11-12 2013-12-31 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
JP2013510857A (ja) * 2009-11-12 2013-03-28 ブリストル−マイヤーズ スクイブ カンパニー C型肝炎ウイルス阻害剤
EP2507232B1 (en) * 2009-12-04 2019-03-20 National Health Research Institutes Proline derivatives
US8415482B2 (en) 2009-12-04 2013-04-09 National Health Research Institutes Proline derivatives
WO2011068941A2 (en) 2009-12-04 2011-06-09 National Health Research Institutes Proline derivatives
WO2011081918A1 (en) 2009-12-14 2011-07-07 Enanta Pharmaceuticals, Inc Hepatitis c virus inhibitors
US8653070B2 (en) 2009-12-14 2014-02-18 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8377980B2 (en) 2009-12-16 2013-02-19 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2011075607A1 (en) * 2009-12-18 2011-06-23 Intermune, Inc. Novel inhibitors of hepatitis c virus replication
US8362068B2 (en) 2009-12-18 2013-01-29 Idenix Pharmaceuticals, Inc. 5,5-fused arylene or heteroarylene hepatitis C virus inhibitors
CN102822175A (zh) * 2009-12-18 2012-12-12 埃迪尼克斯医药公司 5,5-稠合的亚芳基或亚杂芳基丙型肝炎病毒抑制剂
CN102791687A (zh) * 2009-12-18 2012-11-21 英特穆恩公司 C型肝炎病毒复制的新型抑制剂
US9187496B2 (en) 2009-12-18 2015-11-17 Idenix Pharmaceuticals Llc 5,5-fused arylene or heteroarylene hepatitis C virus inhibitors
JP2013514982A (ja) * 2009-12-18 2013-05-02 イデニク プハルマセウティカルス,インコーポレイテッド 5,5−縮合アリーレン又はヘテロアリーレンc型肝炎ウイルス阻害剤
WO2011072370A1 (en) 2009-12-18 2011-06-23 Boehringer Ingelheim International Gmbh Hcv combination therapy
WO2011075615A1 (en) * 2009-12-18 2011-06-23 Idenix Pharmaceuticals, Inc. 5,5-fused arylene or heteroarylene hepatitis c virus inhibitors
CN104530079A (zh) * 2009-12-18 2015-04-22 北京凯因科技股份有限公司 C型肝炎病毒复制的新型抑制剂
JP2017008058A (ja) * 2009-12-18 2017-01-12 イデニク プハルマセウティカルス,インコーポレイテッド 5,5−縮合アリーレン又はヘテロアリーレンc型肝炎ウイルス阻害剤
CN104341401A (zh) * 2009-12-18 2015-02-11 北京凯因科技股份有限公司 C型肝炎病毒复制的新型抑制剂
CN102791687B (zh) * 2009-12-18 2015-02-11 北京凯因科技股份有限公司 C型肝炎病毒复制的新型抑制剂
CN104341401B (zh) * 2009-12-18 2017-02-15 北京凯因科技股份有限公司 C型肝炎病毒复制的新型抑制剂
JP2013515068A (ja) * 2009-12-22 2013-05-02 メルク・シャープ・アンド・ドーム・コーポレーション ウイルス性疾患の治療のための縮合三環式化合物およびその使用方法
EP2515902A1 (en) * 2009-12-24 2012-10-31 Vertex Pharmaceuticals Incorporated Analogues for the treatment or prevention of flavivirus infections
JP2013515746A (ja) * 2009-12-24 2013-05-09 ヴァーテックス ファーマシューティカルズ、 インコーポレイテッド フラビウイルス感染症の治療又は予防のための類似体
WO2011079327A1 (en) * 2009-12-24 2011-06-30 Vertex Pharmaceuticals Incorporated Analogues for the treatment or prevention of flavivirus infections
CN102883718A (zh) * 2009-12-24 2013-01-16 顶点制药公司 用于治疗或预防黄病毒感染的类似物
US8735398B2 (en) 2009-12-30 2014-05-27 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8362020B2 (en) 2009-12-30 2013-01-29 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US8933110B2 (en) 2010-01-25 2015-01-13 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8785487B2 (en) 2010-01-25 2014-07-22 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
EP2528436A4 (en) * 2010-01-25 2013-07-10 Enanta Pharm Inc INHIBITORS OF HEPATITIS C VIRUS
WO2011091532A1 (en) * 2010-01-28 2011-08-04 Boehringer Ingelheim International Gmbh Hepatitis c inhibitor compounds
US8178531B2 (en) 2010-02-23 2012-05-15 Enanta Pharmaceuticals, Inc. Antiviral agents
US8623814B2 (en) 2010-02-23 2014-01-07 Enanta Pharmaceuticals, Inc. Antiviral agents
US9060971B2 (en) 2010-03-04 2015-06-23 Enanta Pharmaceuticals, Inc. Combination pharmaceutical agents as inhibitors of HCV replication
WO2011119858A1 (en) * 2010-03-24 2011-09-29 Vertex Pharmaceuticals Incorporated Analogues for the treatment or prevention of flavivirus infections
US8779156B2 (en) 2010-03-24 2014-07-15 Vertex Pharmaceuticals Incorporated Analogues for the treatment or prevention of flavivirus infections
US9127021B2 (en) 2010-04-09 2015-09-08 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8778938B2 (en) 2010-06-04 2014-07-15 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
US8686026B2 (en) 2010-06-10 2014-04-01 Abbvie Inc. Solid compositions
WO2012006060A1 (en) 2010-06-28 2012-01-12 Vertex Pharmaceuticals Incorporated Compounds and methods for the treatment or prevention of flavivirus infections
WO2012006055A2 (en) 2010-06-28 2012-01-12 Vertex Pharmaceuticals Incorporated Compounds and methods for the treatment or prevention of flavivirus infections
US8815849B2 (en) 2010-07-26 2014-08-26 Janssen R&D Ireland Hetero-bicyclic derivatives as HCV inhibitors
WO2012013643A1 (en) 2010-07-26 2012-02-02 Tibotec Pharmaceuticals Hetero-bicyclic derivatives as hcv inhibitors
WO2012021591A1 (en) * 2010-08-12 2012-02-16 Bristol-Myers Squibb Company Hepatitis c virus inhibitors
EA024171B1 (ru) * 2010-08-12 2016-08-31 Бристол-Майерс Сквибб Компани Ингибиторы вируса гепатита с
US8697704B2 (en) 2010-08-12 2014-04-15 Enanta Pharmaceuticals, Inc. Hepatitis C virus inhibitors
WO2012024363A2 (en) 2010-08-17 2012-02-23 Vertex Pharmaceuticals Incorporated Compounds and methods for the treatment or prevention of flaviviridae viral infections
EP2616461A4 (en) * 2010-08-26 2014-03-26 Rfs Pharma Llc POTENTIVE AND SELECTIVE INHIBITORS OF HEPATITIS C VIRUS
US9181227B2 (en) 2010-08-26 2015-11-10 Cocrystal Pharma, Inc. Potent and selective inhibitors of hepatitis C virus
US8859595B2 (en) 2010-08-26 2014-10-14 Rfs Pharma, Llc Potent and selective inhibitors of hepatitis C virus
US9932326B2 (en) 2010-08-26 2018-04-03 Cocrystal Pharma, LLC Potent and selective inhibitors of hepatitis C virus
WO2012027712A3 (en) * 2010-08-26 2012-06-21 Rfs Pharma, Llc Potent and selective inhibitors of hepatitis c virus
EP2963034A1 (en) * 2010-08-26 2016-01-06 RFS Pharma, LLC. Potent and selective inhibitors of hepatitis c virus
US8822520B2 (en) 2010-09-22 2014-09-02 Presidio Pharmaceuticals, Inc. Substituted bicyclic HCV inhibitors
EP2621932A4 (en) * 2010-09-29 2014-03-26 Merck Sharp & Dohme TETRACYCLIC HETEROCYCLUS COMPOUNDS FOR THE TREATMENT OF HEPATITIS C VIRUS INFECTIONS
US8999967B2 (en) 2010-09-29 2015-04-07 Presidio Pharmaceuticals, Inc. Tricyclic fused ring inhibitors of hepatitis C
AU2011328980B2 (en) * 2010-11-17 2015-07-30 Gilead Sciences, Inc. Antiviral compounds
EP3284741A1 (en) * 2010-11-17 2018-02-21 Gilead Pharmasset LLC Antiviral compounds
KR101835474B1 (ko) 2010-11-17 2018-03-08 길리애드 파마셋 엘엘씨 항바이러스 화합물
US9156823B2 (en) 2010-11-17 2015-10-13 Gilead Pharmasset Llc Antiviral compounds
WO2012068234A3 (en) * 2010-11-17 2013-01-17 12Gilead Sciences, Inc. Antiviral compounds
US10344019B2 (en) 2010-11-17 2019-07-09 Gilead Pharmasset Llc Antiviral compounds
EA020949B1 (ru) * 2010-11-30 2015-02-27 Александр Васильевич ИВАЩЕНКО Замещенные азолы, противовирусный активный компонент, фармацевтическая композиция, способ получения и применения
AU2011337290B2 (en) * 2010-11-30 2016-06-16 Alla Chem, Llc Substituted azoles, anti-viral active ingredient, pharmaceutical composition, method for the production and use thereof
WO2012074437A3 (ru) * 2010-11-30 2012-09-13 Алла Хем, Ллс Замещенные азолы, противовирусный активный компонент, фармацевтическая композиция, способ получения и применения
EP2651927A4 (en) * 2010-12-15 2014-06-04 Abbvie Inc ANTIVIRAL CONNECTIONS
EP2651928A4 (en) * 2010-12-15 2014-06-18 Abbvie Inc ANTI-VIRAL COMPOUNDS
US8552047B2 (en) 2011-02-07 2013-10-08 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9340520B2 (en) 2011-02-07 2016-05-17 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9546160B2 (en) 2011-05-12 2017-01-17 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US10201584B1 (en) 2011-05-17 2019-02-12 Abbvie Inc. Compositions and methods for treating HCV
US10201541B1 (en) 2011-05-17 2019-02-12 Abbvie Inc. Compositions and methods for treating HCV
US8927739B2 (en) 2011-05-18 2015-01-06 Enanta Pharmaceuticals, Inc. Processes for the preparation of 5-azaspiro[2.4]heptane-6-carboxylic acid and its derivatives
WO2013016491A1 (en) 2011-07-26 2013-01-31 Vertex Pharmaceuticals Incorporated Thiophene compounds
WO2013016492A1 (en) 2011-07-26 2013-01-31 Vertex Pharmaceuticals Incorporated Thiophene compounds
WO2013016499A1 (en) 2011-07-26 2013-01-31 Vertex Pharmaceuticals Incorporated Methods for preparation of thiophene compounds
WO2013016490A1 (en) 2011-07-26 2013-01-31 Vertex Pharmaceuticals Incorporated Thiophene compounds
WO2013016501A1 (en) 2011-07-26 2013-01-31 Vertex Pharmaceuticals Incorporated Formulations of thiophene compounds
WO2013030750A1 (en) 2011-09-01 2013-03-07 Lupin Limited Antiviral compounds
US10456414B2 (en) 2011-09-16 2019-10-29 Gilead Pharmasset Llc Methods for treating HCV
US8940718B2 (en) 2011-11-16 2015-01-27 Gilead Pharmasset Llc Antiviral compounds
US9809600B2 (en) 2011-11-16 2017-11-07 Gilead Pharmasset Llc Antiviral compounds
US8921341B2 (en) 2011-11-16 2014-12-30 Gilead Pharmasset Llc Antiviral compounds
US9221833B2 (en) 2011-11-16 2015-12-29 Gilead Pharmasset Llc Antiviral compounds
US10807990B2 (en) 2011-11-16 2020-10-20 Gilead Pharmasset Llc Antiviral compounds
US9868745B2 (en) 2011-11-16 2018-01-16 Gilead Pharmasset Llc Antiviral compounds
US8575135B2 (en) 2011-11-16 2013-11-05 Gilead Sciences, Inc. Antiviral compounds
US9051340B2 (en) 2011-11-16 2015-06-09 Gilead Pharmasset Llc Antiviral compounds
US9364484B2 (en) 2011-12-06 2016-06-14 The Board Of Trustees Of The Leland Stanford Junior University Methods and compositions for treating viral diseases
US10869873B2 (en) 2011-12-06 2020-12-22 The Board Of Trustees Of The Leland Stanford Junior University Methods and compositions for treating viral diseases
CN104169271B (zh) * 2011-12-28 2017-04-05 爱尔兰詹森科学公司 作为hcv抑制剂的喹唑啉酮衍生物
CN104203940A (zh) * 2011-12-28 2014-12-10 爱尔兰詹森研发公司 作为hcv抑制剂的杂双环衍生物
WO2013098320A1 (en) 2011-12-28 2013-07-04 Janssen R&D Ireland Quinazolinone derivatives as hcv inhibitors
JP2015503537A (ja) * 2011-12-28 2015-02-02 ヤンセン・アールアンドデイ・アイルランド Hcv阻害剤としてのキナゾリノン誘導体
US9382261B2 (en) 2011-12-28 2016-07-05 Janssen Sciences Ireland Uc Substituted quinazolinones as HCV inhibitors
CN104169271A (zh) * 2011-12-28 2014-11-26 爱尔兰詹森研发公司 作为hcv抑制剂的喹唑啉酮衍生物
US9126986B2 (en) 2011-12-28 2015-09-08 Janssen Sciences Ireland Uc Hetero-bicyclic derivatives as HCV inhibitors
WO2013098313A1 (en) 2011-12-28 2013-07-04 Janssen R&D Ireland Hetero-bicyclic derivatives as hcv inhibitors
US9034832B2 (en) 2011-12-29 2015-05-19 Abbvie Inc. Solid compositions
US9326973B2 (en) 2012-01-13 2016-05-03 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
WO2013118097A1 (en) 2012-02-10 2013-08-15 Lupin Limited Antiviral compounds with a dibenzooxaheterocycle moiety
US9073942B2 (en) 2012-02-10 2015-07-07 Lupin Limited Antiviral compounds with a heterotricycle moiety
US9073943B2 (en) 2012-02-10 2015-07-07 Lupin Limited Antiviral compounds with a dibenzooxaheterocycle moiety
WO2013118102A1 (en) 2012-02-10 2013-08-15 Lupin Limited Antiviral compounds with a heterotricycle moiety
US10800789B2 (en) 2012-05-16 2020-10-13 Gilead Pharmasset Llc Antiviral compounds
WO2014019344A1 (en) * 2012-08-03 2014-02-06 Sunshine Lake Pharma Co., Ltd. Bridged ring compounds as hepatitis c virus (hcv) inhibitors and pharmaceutical applications thereof
US10039779B2 (en) 2013-01-31 2018-08-07 Gilead Pharmasset Llc Combination formulation of two antiviral compounds
RU2507201C1 (ru) * 2013-02-07 2014-02-20 Александр Васильевич Иващенко Алкил [(s)-1-((s)-2-{5-[4-(4-{2-[(s)-1-((s)-2-метоксикарбониламино-3-метил-бутирил)-пирролидин-2-ил]-3н-имидазол-4-ил}-бута-1,3-диинил)-фенил]-1н-имидазол-2-ил}-пирролидин-1-карбонил)-2-метил-пропил]-карбамат нафталин-1,5-дисульфонат, фармацевтическая композиция, лекарственное средство, способ лечения вирусных заболеваний
WO2014134251A1 (en) 2013-02-28 2014-09-04 Vertex Pharmaceuticals Incorporated Pharmaceutical compositions
US11484534B2 (en) 2013-03-14 2022-11-01 Abbvie Inc. Methods for treating HCV
US9770439B2 (en) 2013-07-02 2017-09-26 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
US9717712B2 (en) 2013-07-02 2017-08-01 Bristol-Myers Squibb Company Combinations comprising tricyclohexadecahexaene derivatives for use in the treatment of hepatitis C virus
US9775831B2 (en) 2013-07-17 2017-10-03 Bristol-Myers Squibb Company Combinations comprising biphenyl derivatives for use in the treatment of HCV
US11707479B2 (en) 2013-08-27 2023-07-25 Gilead Sciences, Inc. Combination formulation of two antiviral compounds
US11116783B2 (en) 2013-08-27 2021-09-14 Gilead Pharmasset Llc Combination formulation of two antiviral compounds
US10086011B2 (en) 2013-08-27 2018-10-02 Gilead Pharmasset Llc Combination formulation of two antiviral compounds
US10105365B2 (en) 2014-01-03 2018-10-23 Abbvie Inc. Solid antiviral dosage forms
US9333204B2 (en) 2014-01-03 2016-05-10 Abbvie Inc. Solid antiviral dosage forms
US9744170B2 (en) 2014-01-03 2017-08-29 Abbvie Inc. Solid antiviral dosage forms
US11203599B2 (en) 2014-06-11 2021-12-21 Gilead Pharmasset Llc Solid forms of an antiviral compound
WO2016040225A1 (en) * 2014-09-09 2016-03-17 Bristol-Myers Squibb Company Phenyl-(aza)cycloalkyl carboxylic acid gpr120 modulators
US10336684B2 (en) 2014-09-09 2019-07-02 Bristol=Myers Squibb Company Phenyl-(aza)cycloalkyl carboxylic acid GPR120 modulators
US10617675B2 (en) 2015-08-06 2020-04-14 Bristol-Myers Squibb Company Hepatitis C virus inhibitors
GB2552919A (en) * 2015-11-18 2018-02-21 Azad Pharmaceutical Ingredients Ag Stable amorphous form of daclatasvir
WO2018160090A1 (ru) 2017-02-28 2018-09-07 Александр Васильевич ИВАЩЕНКО Противовирусная композиция и способ ее применения
WO2020117849A1 (en) 2018-12-04 2020-06-11 Bristol-Myers Squibb Company Methods of analysis using in-sample calibration curve by multiple isotopologue reaction monitoring
US12037340B2 (en) 2021-05-21 2024-07-16 Gilead Sciences, Inc. Pentacyclic derivatives as Zika virus inhibitors
US12497408B2 (en) 2022-05-19 2025-12-16 Gilead Sciences, Inc. Tetracyclic compounds and methods for the treatment of Zika virus infection

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