Haste makes waste: A critical review of docking-based virtual screening in drug repurposing for SARS-CoV-2 main protease (M-pro) inhibition

IF 10.9 1区 医学 Q1 CHEMISTRY, MEDICINAL
Guillem Macip, Pol Garcia-Segura, Júlia Mestres-Truyol, Bryan Saldivar-Espinoza, María José Ojeda-Montes, Aleix Gimeno, Adrià Cereto-Massagué, Santiago Garcia-Vallvé, Gerard Pujadas
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引用次数: 30

Abstract

This review makes a critical evaluation of 61 peer-reviewed manuscripts that use a docking step in a virtual screening (VS) protocol to predict SARS-CoV-2 M-pro (M-pro) inhibitors in approved or investigational drugs. Various manuscripts predict different compounds, even when they use a similar initial dataset and methodology, and most of them do not validate their methodology or results. In addition, a set of known 150 SARS-CoV-2 M-pro inhibitors extracted from the literature and a second set of 81 M-pro inhibitors and 113 inactive compounds obtained from the COVID Moonshot project were used to evaluate the reliability of using docking scores as feasible predictors of the potency of a SARS-CoV-2 M-pro inhibitor. Using two SARS-CoV-2 M-pro structures and five protein-ligand docking programs, we proved that the correlation between the pIC50 and docking scores is not good. Neither was any correlation found between the pIC50 and the ∆G calculated with an MM-GBSA method. When a group of experimentally known inactive compounds was added, neither the docking scores or the ∆G were able to distinguish between compounds with or without M-pro experimental inhibitory activity. Performances improved when covalent and noncovalent inhibitors were treated separately, but were not good enough to fully support using a docking score as a cutoff value for selecting new putative M-pro inhibitors or predicting the relative bioactivity of a compound by comparison with a reference compound. The two sets of known SARS-CoV-2 M-pro inhibitors presented here could be used for validating future VS protocols which aim to predict M-pro inhibitors.

欲速不达:基于对接的虚拟筛选对SARS-CoV-2主蛋白酶(M-pro)抑制药物再利用的重要回顾
本综述对61篇同行评审的手稿进行了批判性评估,这些手稿使用虚拟筛选(VS)方案中的对接步骤来预测已批准或研究药物中的SARS-CoV-2 M-pro (M-pro)抑制剂。不同的手稿预测了不同的化合物,即使他们使用了相似的初始数据集和方法,而且大多数都没有验证他们的方法或结果。此外,利用从文献中提取的一组已知的150种SARS-CoV-2 M-pro抑制剂,以及从COVID Moonshot项目中获得的第二组81种M-pro抑制剂和113种非活性化合物,评估了将对接评分作为SARS-CoV-2 M-pro抑制剂效价预测指标的可靠性。利用2种SARS-CoV-2 M-pro结构和5种蛋白-配体对接方案,我们证明pIC50与对接评分相关性不佳。用MM-GBSA法计算的pIC50与∆G之间也没有相关性。当加入一组实验上已知的无活性化合物时,对接分数或∆G都无法区分具有或不具有M-pro实验抑制活性的化合物。当共价和非共价抑制剂分别处理时,性能得到改善,但不足以完全支持使用对接评分作为选择新的假定M-pro抑制剂或通过与参考化合物比较来预测化合物的相对生物活性的临界值。本文提出的两组已知的SARS-CoV-2 M-pro抑制剂可用于验证旨在预测M-pro抑制剂的未来VS方案。
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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来源期刊
CiteScore
29.30
自引率
0.00%
发文量
52
审稿时长
2 months
期刊介绍: Medicinal Research Reviews is dedicated to publishing timely and critical reviews, as well as opinion-based articles, covering a broad spectrum of topics related to medicinal research. These contributions are authored by individuals who have made significant advancements in the field. Encompassing a wide range of subjects, suitable topics include, but are not limited to, the underlying pathophysiology of crucial diseases and disease vectors, therapeutic approaches for diverse medical conditions, properties of molecular targets for therapeutic agents, innovative methodologies facilitating therapy discovery, genomics and proteomics, structure-activity correlations of drug series, development of new imaging and diagnostic tools, drug metabolism, drug delivery, and comprehensive examinations of the chemical, pharmacological, pharmacokinetic, pharmacodynamic, and clinical characteristics of significant drugs.
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