Computational Biological Center, IBM Thomas J. Watson Research, New York, New York, USA.
Proteins. 2022 May;90(5):1081-1089. doi: 10.1002/prot.26260. Epub 2021 Oct 21.
Since the beginning of the COVID-19 pandemic, scientists across the globe are racing to find a cure for the highly contagious infectious disease caused by the SARS-CoV-2 virus. Despite many promising ongoing progress, there are currently no FDA approved drug to treat infected patients. Recently, the crowdsourcing of drug discovery for inhibiting the main protease (Mpro) of SARS-CoV-2 have yielded a plenty of drug fragments resolved inside the active site of Mpro via the crystallography method. Following the principle of fragment-based drug design (FBDD), we are motivated to design a potent drug candidate (named B19) by merging three fragments JFM, U0P, and HWH. Through extensive all-atom molecular dynamics simulation and molecular docking, we found that B19 among all designed ones is most stable inside the Mpro's active site and the binding free energy of B19 is comparable to or even a little better than that of a native protein ligand processed by Mpro. Our promising results suggest that B19 and its derivatives can potentially be efficacious drug candidates for COVID-19.
自 COVID-19 大流行开始以来,全球科学家一直在竞相寻找治疗由 SARS-CoV-2 病毒引起的高传染性传染病的方法。尽管目前有许多有前途的研究正在进行中,但还没有获得 FDA 批准的药物来治疗感染患者。最近,通过晶体学方法解析了大量抑制 SARS-CoV-2 主要蛋白酶(Mpro)的药物片段,从而进行了药物发现的众包。基于基于片段的药物设计(FBDD)的原理,我们通过融合三个片段 JFM、U0P 和 HWH 来设计一种有效的候选药物(命名为 B19)。通过广泛的全原子分子动力学模拟和分子对接,我们发现,在所设计的所有分子中,B19 是最稳定的,位于 Mpro 的活性部位内,B19 的结合自由能与 Mpro 处理的天然蛋白配体相当,甚至稍好一些。我们有希望的结果表明,B19 及其衍生物可能是治疗 COVID-19 的有效候选药物。
