Department of Biology, School of Arts and Sciences, The Catholic University of America, Washington, Washington DC, United States of America.
Department of Molecular Medicine, Morsani College of Medicine, University of South Florida, Tampa, Florida, United States of America.
PLoS Pathog. 2023 Aug 31;19(8):e1011592. doi: 10.1371/journal.ppat.1011592. eCollection 2023 Aug.
The SARS-CoV-2 main protease (Mpro) is a major therapeutic target. The Mpro inhibitor, nirmatrelvir, is the antiviral component of Paxlovid, an orally available treatment for COVID-19. As Mpro inhibitor use increases, drug resistant mutations will likely emerge. We have established a non-pathogenic system, in which yeast growth serves as an approximation for Mpro activity, enabling rapid identification of mutants with altered enzymatic activity and drug sensitivity. The E166 residue is known to be a potential hot spot for drug resistance and yeast assays identified substitutions which conferred strong nirmatrelvir resistance and others that compromised activity. On the other hand, N142A and the P132H mutation, carried by the Omicron variant, caused little to no change in drug response and activity. Standard enzymatic assays confirmed the yeast results. In turn, we solved the structures of Mpro E166R, and Mpro E166N, providing insights into how arginine may drive drug resistance while asparagine leads to reduced activity. The work presented here will help characterize novel resistant variants of Mpro that may arise as Mpro antivirals become more widely used.
严重急性呼吸综合征冠状病毒 2 主蛋白酶 (Mpro) 是主要的治疗靶点。Mpro 抑制剂奈玛特韦是帕罗韦德的抗病毒成分,帕罗韦德是一种用于治疗 COVID-19 的口服药物。随着 Mpro 抑制剂的使用增加,可能会出现耐药突变。我们建立了一个非致病性系统,其中酵母生长可作为 Mpro 活性的近似值,从而能够快速识别具有改变的酶活性和药物敏感性的突变体。众所周知,E166 残基是潜在的耐药热点,酵母测定鉴定出赋予奈玛特韦强耐药性的取代以及其他降低活性的取代。另一方面,奥密克戎变异株携带的 N142A 和 P132H 突变对药物反应和活性几乎没有影响。标准酶促测定证实了酵母的结果。反过来,我们解决了 Mpro E166R 和 Mpro E166N 的结构,深入了解了精氨酸如何导致耐药性,而天冬酰胺导致活性降低。这里介绍的工作将有助于表征 Mpro 可能出现的新型耐药变异体,因为 Mpro 抗病毒药物的使用越来越广泛。
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