Hernández González Jorge E, Eberle Raphael J, Willbold Dieter, Coronado Mônika A
Multiuser Center for Biomolecular Innovation, IBILCE, Universidade Estadual Paulista (UNESP), São Jose do Rio Preto, Brazil.
Laboratory for Molecular Modeling and Dynamics, Instituto de Biofísica Carlos Chagas Filho, Universidade Federal do Rio de Janeiro, Cidade Universitária Ilha do Fundão, Rio de Janeiro, Brazil.
Front Mol Biosci. 2022 Jan 24;8:816166. doi: 10.3389/fmolb.2021.816166. eCollection 2021.
The SARS-CoV-2 main protease, also known as 3-chymotrypsin-like protease (3CL), is a cysteine protease responsible for the cleavage of viral polyproteins pp1a and pp1ab, at least, at eleven conserved sites, which leads to the formation of mature nonstructural proteins essential for the replication of the virus. Due to its essential role, numerous studies have been conducted so far, which have confirmed 3CL as an attractive drug target to combat Covid-19 and have reported a vast number of inhibitors and their co-crystal structures. Despite all the ongoing efforts, D-peptides, which possess key advantages over L-peptides as therapeutic agents, have not been explored as potential drug candidates against 3CL. The current work fills this gap by reporting an approach for the discovery of D-peptides capable of inhibiting 3CL that involves structure-based virtual screening (SBVS) of an library of D-tripeptides and D-tetrapeptides into the protease active site and subsequent rescoring steps, including Molecular Mechanics Generalized-Born Surface Area (MM-GBSA) free energy calculations and molecular dynamics (MD) simulations. enzymatic assays conducted for the four top-scoring D-tetrapeptides at 20 μM showed that all of them caused 55-85% inhibition of 3CL activity, thus highlighting the suitability of the devised approach. Overall, our results present a promising computational strategy to identify D-peptides capable of inhibiting 3CL, with broader application in problems involving protein inhibition.
严重急性呼吸综合征冠状病毒2(SARS-CoV-2)主要蛋白酶,也称为3-糜蛋白酶样蛋白酶(3CL),是一种半胱氨酸蛋白酶,负责在至少11个保守位点切割病毒多聚蛋白pp1a和pp1ab,从而形成病毒复制所必需的成熟非结构蛋白。由于其关键作用,迄今为止已经进行了大量研究,这些研究证实3CL是对抗新型冠状病毒肺炎(Covid-19)的有吸引力的药物靶点,并报道了大量抑制剂及其共晶体结构。尽管一直在努力,但与L-肽相比具有关键优势的D-肽尚未被探索作为抗3CL的潜在药物候选物。当前的工作通过报告一种发现能够抑制3CL的D-肽的方法填补了这一空白,该方法包括将D-三肽和D-四肽库基于结构的虚拟筛选(SBVS)到蛋白酶活性位点以及随后的重新评分步骤,包括分子力学广义玻恩表面积(MM-GBSA)自由能计算和分子动力学(MD)模拟。对四种得分最高的D-四肽在20μM浓度下进行的酶活性测定表明,它们都导致3CL活性受到55-85%的抑制,从而突出了所设计方法的适用性。总体而言,我们的结果提出了一种有前景的计算策略来鉴定能够抑制3CL的D-肽,在涉及蛋白质抑制的问题中有更广泛的应用。
