SARS-CoV-2主要蛋白酶抑制剂:基于结构的抗病毒临床前GC376增强鼓励进一步开发

IF 2 4区化学 Q3 CHEMISTRY, MULTIDISCIPLINARY

Journal of Computational Biophysics and Chemistry Pub Date : 2022-12-07 DOI:10.1142/s273741652350014x

Elliot Perry, Simon Chapman, Yaozhong Xu

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引用次数: 0

摘要

严重急性呼吸系统综合征冠状病毒2型主要蛋白酶（Mpro）在病毒复制和转录中起关键作用。Mpro介导复制酶基因ORF1a和ORF1ab的翻译产物的蛋白水解。对临床前试验Mpro抑制剂的调查表明，某些部分的疗效可能会增强。与有前景的体外和计算机数据相一致，选择蛋白酶抑制剂GC376作为先导。GC376类似物的修饰产生了一系列有前景的Mpro抑制剂。设计优化确定化合物G59i为先导候选物，显示出复合物的结合能为-10.54kcal/mol。G59i和Mpro之间的交互性很强。具有值得称赞的ADMET特性和增强的效力，进一步的G59i分析可能是有利的；此外，已鉴定的关键Mpro残基有助于设计新型抑制剂。[来自作者]

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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SARS-CoV-2 main protease inhibitors: Structure-based enhancement to anti-viral pre-clinical GC376 encourages further development

SARS-CoV-2 Main protease (Mpro) is pivotal in viral replication and transcription. Mpro mediates proteolysis of translated products of replicase genes ORF1a and ORF1ab. Surveying pre-clinical trial Mpro inhibitors suggests potential enhanced efficacy for some moieties. Concordant with promising in vitro and in silico data, the protease inhibitor GC376 was chosen as a lead. Modification of GC376 analogues yielded a series of promising Mpro inhibitors. Design optimization identified compound G59i as lead candidate, displaying a binding energy of −10.54kcal/mol for the complex. Robust interactivity was noted between G59i and Mpro. With commendable ADMET characteristics and enhanced potency, further G59i analysis may be advantageous;moreover, identified key Mpro residues could contribute to the design of neotenic inhibitors. [ FROM AUTHOR]

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来源期刊

Journal of Computational Biophysics and Chemistry CHEMISTRY, MULTIDISCIPLINARY-

CiteScore

3.60

自引率

9.10%

发文量