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Development of Cell-Based Assays for In Vitro Characterization of Hepatitis C Virus NS3/4A Protease Inhibitors

机译:基于细胞的丙型肝炎病毒NS3 / 4A蛋白酶抑制剂体外鉴定方法的开发

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摘要

A recombinant vaccinia virus, expressing the NS3-to-NS5 region of the N clone of hepatitis C virus (HCV), was generated and utilized both in a gel-based assay and in an enzyme-linked immunosorbent assay (ELISA) to evaluate the pyrrolidine-5,5-trans-lactams, a series of inhibitors of the HCV NS3/4A protease. The absolute levels of processed, mature HCV nonstructural proteins in this system were found to decrease in the presence of the trans-lactams. Monitoring of this reduction enabled end points and 50% inhibitory concentrations to be calculated in order to rank the active compounds according to potency. These compounds had no effect on the transcription or translation of the NS3-5 polyprotein at concentrations shown to inhibit NS3/4A protease, and they were shown to be specific inhibitors of this protease. The ELISA, originally developed using the vaccinia virus expression system, was modified to utilize Huh-7 cells containing an HCV replicon. Results with this assay correlated well with those obtained with the recombinant vaccinia virus assays. These results demonstrate the utility of these assays for the characterization of NS3/4A protease inhibitors. In addition, inhibitors of other viral targets, such as polymerase and helicase, can be evaluated in the context of the replicon ELISA.
机译:产生了表达丙型肝炎病毒(HCV)N克隆的NS3-to-NS5区的重组牛痘病毒,并将其用于基于凝胶的测定和酶联免疫吸附测定(ELISA)中,以评估吡咯烷-5,5-反式内酰胺类,HCV NS3 / 4A蛋白酶的一系列抑制剂。发现在存在反式内酰胺的情况下,该系统中加工的,成熟的HCV非结构蛋白的绝对水平降低。监测这种减少使得能够计算出终点和50%抑制浓度,以便根据效力对活性化合物进行排名。这些化合物在显示抑制NS3 / 4A蛋白酶的浓度下对NS3-5多蛋白的转录或翻译没有影响,并且显示为该蛋白酶的特异性抑制剂。最初使用牛痘病毒表达系统开发的ELISA进行了修改,以利用含有HCV复制子的Huh-7细胞。该测定的结果与通过重组牛痘病毒测定获得的结果很好地相关。这些结果证明了这些测定法用于表征NS3 / 4A蛋白酶抑制剂的实用性。另外,可以在复制子ELISA的背景下评估其他病毒靶标的抑制剂,例如聚合酶和解旋酶。

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