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首页> 外文期刊>Tropical biomedicine. >Discovery of small molecule inhibitors against the NS3/4A serine protease of Hepatitis C virus genotype 3 via highthroughput virtual screening and in vitro evaluations
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Discovery of small molecule inhibitors against the NS3/4A serine protease of Hepatitis C virus genotype 3 via highthroughput virtual screening and in vitro evaluations

机译:通过高透视筛选和体外评估发现对丙型肝炎病毒基因型3的NS3 / 4A丝氨酸蛋白酶的小分子抑制剂的发现

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The hepatitis C virus (HCV) consists of eight genotypes and 90 subtypes, with genotype (GT) 3 being the second most common globally and is linked to higher incidences of steatosis and rapid development of fibrosis and cirrhosis. The NS3/4A serine protease, a heterodimer complex of two HCV non-structural proteins, is an effective target for pharmaceutical intervention due to its essential roles in processing HCV polyproteins and inhibiting innate immunity. This study combines structure-based virtual screening (SBVS) of predefined compound libraries, pharmacokinetic prediction (ADME/T) and in vitro evaluation to identify potential low molecular weight (500 Dalton) inhibitors of the NS3/4A serine protease (GT3). In silico screening of ZINC and PubChem libraries yielded five selected compounds as potential candidates. Dose-dependent inhibition of the NS3/4A serine protease and HCV replication in HuH-7.5 cells revealed that compound A (PubChem ID No. 16672637) exhibited inhibition towards HCV GT3 with an IC 50 of 106.7μM and EC 50 of 25.8μM, respectively. Thus, compound A may be developed as a potent, low molecular weight drug against the HCV NS3/4A serine protease of GT3.
机译:丙型肝炎病毒(HCV)由八种基因型和90个亚型组成,基因型(GT)3是全球第二次最常见的,并且与脂肪变性的较高发病率和纤维化和肝硬化的快速发展有关。 NS3 / 4A丝氨酸蛋白酶是两种HCV非结构蛋白的异二聚体复合物,是药物干预的有效靶标,这是加工HCV多蛋白的必要作用和抑制先天性免疫。该研究将基于结构的虚拟筛选(SBV)与预定义的复合文库,药代动力学预测(ADME / T)和体外评估结合,以鉴定NS3 / 4A丝氨酸蛋白酶(GT3)的潜在低分子量(<500Atalton)抑制剂。在锌和Pubchem文库的硅筛选中,将五种选定化合物作为潜在的候选物产生。 Huh-7.5细胞中的NS3 / 4A丝氨酸蛋白酶和HCV复制的剂量依赖性抑制表明,化合物A(PUBCHEM ID No.16672637)分别表现出对HCV GT3的抑制作用,IC 50分别为25.8μm的EC 50。 。因此,可以将化合物A作为富含HCV NS3 / 4A丝氨酸蛋白酶的效力低分子量药物。

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