Super Computing Applications and Innovation, Department HPC, CINECA, Casalecchio di Reno, Italy.
Laboratory of Bioinorganic Chemistry, Department of Pharmacy and Biotechnology, University of Bologna, Bologna, Italy.
Proteins. 2023 Sep;91(9):1288-1297. doi: 10.1002/prot.26548. Epub 2023 Jul 6.
Thanks to the considerable research which has been undertaken in the last few years to improve our understanding of the biology and mechanism of action of SARS-CoV-2, we know how the virus uses its surface spike protein to infect host cells. The transmembrane prosthesis, serine 2 (TMPRSS2) protein, located on the surface of human cells, recognizes the cleavage site in the spike protein, leading to the release of the fusion peptide and entry of the virus into the host cells. Because of its role, TMPRSS2 has been proposed as a drug target to prevent infection by the virus. In this study, we aim to increase our understanding of TMPRSS2 using long scale microsecond atomistic molecular dynamics simulations, focusing on the conformational changes over time. The comparison between simulations conducted on the protein in the native (apo) and inhibited form (holo), has shown that in the holo form the inhibitor stabilizes the catalytic site and induces rearrangements in the extracellular domain of the protein. In turn, it leads to the formation of a new cavity in the vicinity of the ligand binding pocket that is stable in the microsecond time scale. Given the low specificity of known protease inhibitors, these findings suggest a new potential drug target site that can be used to improve TMPRSS2 specific recognition by newly designed inhibitors.
由于在过去几年中进行了大量研究,我们对 SARS-CoV-2 的生物学和作用机制有了更深入的了解,我们知道病毒如何利用其表面刺突蛋白感染宿主细胞。位于人细胞表面的跨膜蛋白酶 2(TMPRSS2)蛋白识别刺突蛋白中的切割位点,导致融合肽的释放和病毒进入宿主细胞。由于其作用,TMPRSS2 已被提议作为一种药物靶点,以防止病毒感染。在这项研究中,我们旨在使用长尺度微秒原子分子动力学模拟来增加对 TMPRSS2 的理解,重点关注随时间的构象变化。对天然(apo)和抑制形式(holo)下的蛋白质进行模拟的比较表明,在 holo 形式下,抑制剂稳定了催化位点并诱导蛋白质外域的重排。反过来,它导致配体结合口袋附近形成一个在微秒时间尺度上稳定的新空腔。鉴于已知蛋白酶抑制剂的特异性低,这些发现表明了一个新的潜在药物靶点,可用于通过新设计的抑制剂提高 TMPRSS2 的特异性识别。
