Shamsara Jamal
Pharmaceutical Research Center, Pharmaceutical Technology Institute, Mashhad University of Medical Sciences, Mashhad, Iran.
Drug Res (Stuttg). 2018 Sep;68(9):529-535. doi: 10.1055/a-0586-8308. Epub 2018 Apr 3.
MMP-2 belongs to a large family of proteases called matrix metalloproteinases (MMPs) that degrades type IV collagen, the main structural component of basement membranes and gelatin. The main pathologic role of MMP-2 overexpression is to contribute to the development of cancer through the progression of metastasis and angiogenesis. A structure-based virtual screening was employed to find new inhibitors with possible selectivity for MMP-2. The inhibitory activities of 3 inhibitors (one was not a suitable drug-like hit) among 19 purchased compounds were approved by enzyme inhibition assay. 5 hits were non-zinc-binding inhibitors of MMP-2. The results demonstrated that a computer-aided drug design could be successfully applied for discovering new MMP-2 inhibitors. We found inhibitors with new scaffolds for the inhibition of MMP-2 with some selectivity features that could be used for future lead optimization processes. According to the docked pose and MD simulation, compound 13 was expected to interact with the S1' specificity loop of MMP-2 and had 2 π-π interactions and a stable hydrogen bond with the MMP-2 active site. The key feature of compound 13 could be used to guide the design of new non-zinc-binding inhibitors of MMP-2.
基质金属蛋白酶-2(MMP-2)属于一个名为基质金属蛋白酶(MMPs)的蛋白酶大家族,该家族可降解IV型胶原蛋白,而IV型胶原蛋白是基底膜和明胶的主要结构成分。MMP-2过表达的主要病理作用是通过转移和血管生成的进展促进癌症的发展。采用基于结构的虚拟筛选来寻找对MMP-2具有可能选择性的新抑制剂。通过酶抑制试验验证了19种购买化合物中3种抑制剂(其中一种不是合适的类药物先导化合物)的抑制活性。5种先导化合物是MMP-2的非锌结合抑制剂。结果表明,计算机辅助药物设计可成功应用于发现新的MMP-2抑制剂。我们发现了具有新骨架的抑制剂来抑制MMP-2,其具有一些选择性特征,可用于未来的先导化合物优化过程。根据对接构象和分子动力学模拟,化合物13预计与MMP-2的S1'特异性环相互作用,并与MMP-2活性位点有2个π-π相互作用和一个稳定的氢键。化合物13的关键特征可用于指导新型MMP-2非锌结合抑制剂的设计。
