Literature DB >> 15955819

Interdomain communication in hepatitis C virus polymerase abolished by small molecule inhibitors bound to a novel allosteric site.

Stefania Di Marco1, Cinzia Volpari, Licia Tomei, Sergio Altamura, Steven Harper, Frank Narjes, Uwe Koch, Michael Rowley, Raffaele De Francesco, Giovanni Migliaccio, Andrea Carfí.   

Abstract

The hepatitis C virus (HCV) polymerase is required for replication of the viral genome and is a key target for therapeutic intervention against HCV. We have determined the crystal structures of the HCV polymerase complexed with two indole-based allosteric inhibitors at 2.3- and 2.4-Angstroms resolution. The structures show that these inhibitors bind to a site on the surface of the thumb domain. A cyclohexyl and phenyl ring substituents, bridged by an indole moiety, fill two closely spaced pockets, whereas a carboxylate substituent forms a salt bridge with an exposed arginine side chain. Interestingly, in the apoenzyme, the inhibitor binding site is occupied by a small alpha-helix at the tip of the N-terminal loop that connects the fingers and thumb domains. Thus, these molecules inhibit the enzyme by preventing formation of intramolecular contacts between these two domains and consequently precluding their coordinated movements during RNA synthesis. Our structures identify a novel mechanism by which a new class of allosteric inhibitors inhibits the HCV polymerase and open the way to the development of novel antiviral agents against this clinically relevant human pathogen.

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Year:  2005        PMID: 15955819     DOI: 10.1074/jbc.M505423200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  52 in total

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Journal:  J Mol Biol       Date:  2006-12-01       Impact factor: 5.469

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3.  Comparative study of the genetic barriers and pathways towards resistance of selective inhibitors of hepatitis C virus replication.

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Review 4.  Apolipoprotein E4: a causative factor and therapeutic target in neuropathology, including Alzheimer's disease.

Authors:  Robert W Mahley; Karl H Weisgraber; Yadong Huang
Journal:  Proc Natl Acad Sci U S A       Date:  2006-03-27       Impact factor: 11.205

5.  Dynamics on multiple timescales in the RNA-directed RNA polymerase from the cystovirus phi6.

Authors:  Zhen Ren; Hsin Wang; Ranajeet Ghose
Journal:  Nucleic Acids Res       Date:  2010-04-12       Impact factor: 16.971

6.  Binding-site identification and genotypic profiling of hepatitis C virus polymerase inhibitors.

Authors:  Frederik Pauwels; Wendy Mostmans; Ludo M M Quirynen; Liesbet van der Helm; Carlo W Boutton; Anne-Stéphanie Rueff; Erna Cleiren; Pierre Raboisson; Dominique Surleraux; Origène Nyanguile; Kenneth A Simmen
Journal:  J Virol       Date:  2007-04-25       Impact factor: 5.103

7.  A locking mechanism regulates RNA synthesis and host protein interaction by the hepatitis C virus polymerase.

Authors:  Sreedhar Chinnaswamy; Ian Yarbrough; Satheesh Palaninathan; C T Ranjith Kumar; Vinodhini Vijayaraghavan; Borries Demeler; Stanley M Lemon; James C Sacchettini; C Cheng Kao
Journal:  J Biol Chem       Date:  2008-04-28       Impact factor: 5.157

8.  Computational predictions suggest that structural similarity in viral polymerases may lead to comparable allosteric binding sites.

Authors:  Jodian A Brown; Marie V Espiritu; Joel Abraham; Ian F Thorpe
Journal:  Virus Res       Date:  2016-06-01       Impact factor: 3.303

9.  Affinity labeling of hepatitis C virus replicase with a nucleotide analogue: identification of binding site.

Authors:  Dinesh Manvar; Kamlendra Singh; Virendra N Pandey
Journal:  Biochemistry       Date:  2013-01-04       Impact factor: 3.162

10.  Novel antiviral agent DTriP-22 targets RNA-dependent RNA polymerase of enterovirus 71.

Authors:  Tzu-Chun Chen; Hwan-You Chang; Pei-Fen Lin; Jyh-Haur Chern; John Tsu-An Hsu; Chu-Yi Chang; Shin-Ru Shih
Journal:  Antimicrob Agents Chemother       Date:  2009-05-04       Impact factor: 5.191

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