Dipartimento Biotecnologie, Chimica e Farmacia, Università degli Studi di Siena, Via A. De Gasperi 2, 53100 Siena, Italy.
ChemMedChem. 2013 Mar;8(3):475-83. doi: 10.1002/cmdc.201200584. Epub 2013 Feb 12.
Targeting protein-protein interactions, such as the HIV-1 gp120-CD4 interface, has become a cutting-edge approach in the current drug discovery scenario. Many small molecules have been developed so far as inhibitors of the interaction between CD4 and HIV-1 gp120. However, due to a variety of reasons such as solubility, drug toxicity and drug resistance, these inhibitors have failed to prove clinically useful. As such, the identification of novel compounds that bind to protein-protein interactions is still a research area of considerable interest. Here, a structure-based virtual screening approach was successfully applied with the aim of identifying novel HIV-1 entry inhibitors targeting the Phe43 pocket of HIV-1 gp120. Several compounds able to inhibit viral replication in cell culture were identified, with the best agent endowed with an EC(50) value of 0.9 μM. Inactivity of all the identified hits toward a mutant (Met475Ile) strain strongly suggests that they interact in the Phe43 cavity of gp120, as intended. Remarkably, all of these small molecules have a chemical scaffold unrelated to any known class of entry inhibitors reported thus far. Overall, our strategy led to the identification of four novel chemical scaffolds that inhibit HIV-1 replication through the destabilization of the HIV-1 gp120-CD4 interface.
针对蛋白质-蛋白质相互作用,如 HIV-1 gp120-CD4 界面,已经成为当前药物发现领域的一种前沿方法。迄今为止,已经开发出许多小分子作为 CD4 和 HIV-1 gp120 之间相互作用的抑制剂。然而,由于溶解度、药物毒性和耐药性等多种原因,这些抑制剂未能在临床上证明是有用的。因此,识别与蛋白质-蛋白质相互作用结合的新型化合物仍然是一个相当有兴趣的研究领域。在这里,成功地应用了一种基于结构的虚拟筛选方法,旨在鉴定针对 HIV-1 gp120 的 Phe43 口袋的新型 HIV-1 进入抑制剂。鉴定出了几种能够在细胞培养中抑制病毒复制的化合物,其中最好的化合物具有 0.9 μM 的 EC(50)值。所有鉴定出的化合物对突变体(Met475Ile)菌株均无活性,这强烈表明它们与 gp120 中的 Phe43 腔相互作用,如预期的那样。值得注意的是,所有这些小分子都具有与迄今为止报道的任何已知类别的进入抑制剂无关的化学支架。总体而言,我们的策略导致了四种新型化学支架的鉴定,这些支架通过 HIV-1 gp120-CD4 界面的失稳来抑制 HIV-1 的复制。
