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首页> 外文期刊>Antimicrobial agents and chemotherapy. >PTC725, an NS4B-Targeting Compound, Inhibits a Hepatitis C Virus Genotype 3 Replicon, as Predicted by Genome Sequence Analysis and Determined Experimentally
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PTC725, an NS4B-Targeting Compound, Inhibits a Hepatitis C Virus Genotype 3 Replicon, as Predicted by Genome Sequence Analysis and Determined Experimentally

机译:PTC725,一种靶向NS4B的化合物,可抑制丙型肝炎病毒基因型3复制子,这是通过基因组序列分析预测并通过实验确定的

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摘要

PTC725 is a small molecule NS4B-targeting inhibitor of hepatitis C virus (HCV) genotype (gt) 1 RNA replication that lacks activity against HCV gt2. We analyzed the Los Alamos HCV sequence database to predict susceptible/resistant HCV gt's according to the prevalence of known resistance-conferring amino acids in the NS4B protein. Our analysis predicted that HCV gt3 would be highly susceptible to the activity of PTC725. Indeed, PTC725 was shown to be active against a gt3 subgenomic replicon with a 50% effective concentration of similar to 5 nM. De novo resistance selection identified mutations encoding amino acid substitutions mapping to the first predicted transmembrane region of NS4B, a finding consistent with results for PTC725 and other NS4Btargeting compounds against HCV gt1. This is the first report of the activity of an NS4B targeting compound against HCV gt3. In addition, we have identified previously unreported amino acid substitutions selected by PTC725 treatment which further demonstrate that these compounds target the NS4B first transmembrane region.
机译:PTC725是靶向小分子NS4B的丙型肝炎病毒(HCV)基因型(gt)1 RNA复制抑制剂,对HCV gt2没有活性。我们分析了洛斯阿拉莫斯(Los Alamos)HCV序列数据库,根据NS4B蛋白中已知的可赋予抗性氨基酸的流行程度来预测易感性/抗性HCV gt。我们的分析预测,HCV gt3对PTC725的活性高度敏感。实际上,已显示PTC725对gt3亚基因组复制子有活性,其有效浓度为50%,接近5 nM。从头抗性选择确定了编码映射到NS4B的第一个预测跨膜区域的氨基酸取代的突变,这一发现与PTC725和其他针对HCV gt1的NS4B靶向化合物的结果一致。这是NS4B靶向化合物抗HCV gt3活性的首次报道。另外,我们已经鉴定了通过PTC725处理选择的以前未报告的氨基酸取代,这进一步证明了这些化合物靶向NS4B第一跨膜区域。

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