Dipartimento di Scienze Farmaceutiche Pietro Pratesi, Università di Milano, Via Mangiagalli 25, 20133 Milano, Italy.
ChemMedChem. 2012 Sep;7(9):1594-600. doi: 10.1002/cmdc.201200274. Epub 2012 Jun 29.
Herein we report the synthesis of a set of constrained peptidomimetics endowed with an electrophilic vinyl ester warhead and structurally related to a previously identified lead compound, a potent and irreversible inhibitor of falcipain-2 (FP-2). FP-2 is the main hemoglobinase of the malaria parasite P. falciparum. The new compounds were evaluated for their inhibition against FP-2, and the results were rationalized on the basis of docking experiments. These studies underscore the pivotal role of both the ester function at the P1' site and the trifluoromethyl group of the P3 side chain in determining the correct orientation of the Michael acceptor warhead in the catalytic site, and as a consequence, the potency of the inhibitors as well as their reversible or irreversible mode of inhibition.
在此,我们报告了一组具有亲电乙烯酯弹头的约束性肽类似物的合成,这些类似物与先前鉴定的一种有效的、不可逆的疟原虫 falcipain-2(FP-2)抑制剂的先导化合物在结构上相关。FP-2 是疟原虫 P. falciparum 的主要血红蛋白酶。评估了新化合物对 FP-2 的抑制作用,并根据对接实验对结果进行了合理化。这些研究强调了 P1' 位的酯功能和 P3 侧链的三氟甲基在确定迈克尔受体弹头在催化部位的正确取向以及抑制剂的效力及其可逆或不可逆抑制模式方面的关键作用。
