HCV RdRp,索非布韦及其他。

Q3 Biochemistry, Genetics and Molecular Biology
Enzymes Pub Date : 2021-01-01 Epub Date: 2021-09-24 DOI:10.1016/bs.enz.2021.06.003
Joy Y Feng, Adrian S Ray
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引用次数: 5

摘要

利用核苷酸类似物靶向治疗丙型肝炎病毒(HCV)的非结构蛋白5B (NS5B) RNA依赖RNA聚合酶(RdRp),使人们对该酶的结构、功能和底物特异性有了深入的了解。与先前研究的DNA聚合酶(包括人类免疫缺陷病毒的逆转录酶)不同,HCV RdRp的生化检测的发展具有挑战性,因为全长蛋白的溶解度低,外源引物/模板的接受效率低。尽管明显的特异性活性较差,但研究发现HCV RdRp一旦在体外开始延伸,就能支持快速和持续的转录,这与HCV RdRp在患者肝脏中的高水平病毒复制一致。对HCV RdRp底物特异性的了解导致索非布韦活性三磷酸作为病毒RNA转录物的非专性链终止物的发现。HCV RdRp的三联晶体结构、引物/模板和进入的核苷酸显示了核苷酸类似物与2'-羟基结合袋之间的相互作用,以及丝氨酸282向苏氨酸的不合适突变如何通过与尿嘧啶碱基和类似物2'-位置的修饰相互作用而导致耐药性。宿主聚合酶介导核苷酸类似物的脱靶毒性,索非布韦的活性代谢物被发现不能被宿主聚合酶包括线粒体RNA聚合酶(POLRMT)有效地掺入。研究HCV RdRp抑制剂所获得的知识有助于促进其他新出现的RNA病毒的抗病毒药物发现,包括发现瑞德西韦可作为引起COVID-19的严重急性呼吸综合征冠状病毒2 (SARS-CoV2)的抑制剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
HCV RdRp, sofosbuvir and beyond.

The therapeutic targeting of the nonstructural protein 5B (NS5B) RNA-dependent RNA polymerase (RdRp) of the Hepatitis C Virus (HCV) with nucleotide analogs led to a deep understanding of this enzymes structure, function and substrate specificity. Unlike previously studied DNA polymerases including the reverse transcriptase of Human Immunodeficiency Virus, development of biochemical assays for HCV RdRp proved challenging due to low solubility of the full-length protein and inefficient acceptance of exogenous primer/templates. Despite the poor apparent specific activity, HCV RdRp was found to support rapid and processive transcription once elongation is initiated in vitro consistent with its high level of viral replication in the livers of patients. Understanding of the substrate specificity of HCV RdRp led to the discovery of the active triphosphate of sofosbuvir as a nonobligate chain-terminator of viral RNA transcripts. The ternary crystal structure of HCV RdRp, primer/template, and incoming nucleotide showed the interaction between the nucleotide analog and the 2'-hydroxyl binding pocket and how an unfit mutation of serine 282 to threonine results in resistance by interacting with the uracil base and modified 2'-position of the analog. Host polymerases mediate off-target toxicity of nucleotide analogs and the active metabolite of sofosbuvir was found to not be efficiently incorporated by host polymerases including the mitochondrial RNA polymerase (POLRMT). Knowledge from studying inhibitors of HCV RdRp serves to advance antiviral drug discovery for other emerging RNA viruses including the discovery of remdesivir as an inhibitor of severe acute respiratory syndrome coronavirus 2 (SARS-CoV2), the virus that causes COVID-19.

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来源期刊
Enzymes
Enzymes Biochemistry, Genetics and Molecular Biology-Biotechnology
CiteScore
4.30
自引率
0.00%
发文量
10
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