2giq

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Revision as of 12:06, 21 November 2007 by OCA (talk | contribs) (New page: left|200px<br /><applet load="2giq" size="450" color="white" frame="true" align="right" spinBox="true" caption="2giq, resolution 1.65Å" /> '''Hepatitis C virus RN...)
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File:2giq.jpg


2giq, resolution 1.65Å

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Hepatitis C virus RNA-dependent RNA polymerase NS5B with NNI-2 inhibitor

OverviewOverview

Multiple nonnucleoside inhibitor binding sites have been identified within, the hepatitis C virus (HCV) polymerase, including in the palm and thumb, domains. After a single treatment with a thumb site inhibitor, (thiophene-2-carboxylic acid NNI-1), resistant HCV replicon variants, emerged that contained mutations at residues Leu419, Met423, and Ile482 in, the polymerase thumb domain. Binding studies using wild-type (WT) and, mutant enzymes and structure-based modeling showed that the mechanism of, resistance is through the reduced binding of the inhibitor to the mutant, enzymes. Combined treatment with a thumb- and a palm-binding polymerase, inhibitor had a dramatic impact on the number of replicon colonies able to, replicate in the presence of both inhibitors. A more exact, characterization through molecular cloning showed that 97.7% of replicons, contained amino acid substitutions that conferred resistance to either of, the inhibitors. Of those, 65% contained simultaneously multiple amino acid, substitutions that conferred resistance to both inhibitors. Double-mutant, replicons Met414Leu and Met423Thr were predominantly selected, which, showed reduced replication capacity compared to the WT replicon. These, findings demonstrate the selection of replicon variants dually resistant, to two NS5B polymerase inhibitors binding to different sites of the, enzyme. Additionally, these findings provide initial insights into the in, vitro mutational threshold of the HCV NS5B polymerase and the potential, impact of viral fitness on the selection of multiple-resistant mutants.

About this StructureAbout this Structure

2GIQ is a Single protein structure of sequence from Viruses with NN2 as ligand. Active as RNA-directed RNA polymerase, with EC number 2.7.7.48 Full crystallographic information is available from OCA.

ReferenceReference

Selection and characterization of replicon variants dually resistant to thumb- and palm-binding nonnucleoside polymerase inhibitors of the hepatitis C virus., Le Pogam S, Kang H, Harris SF, Leveque V, Giannetti AM, Ali S, Jiang WR, Rajyaguru S, Tavares G, Oshiro C, Hendricks T, Klumpp K, Symons J, Browner MF, Cammack N, Najera I, J Virol. 2006 Jun;80(12):6146-54. PMID:16731953

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