Drug Design and Synthesis Lab., Department of Chemistry, Jamia Millia Islamia, Jamia Nagar, New Delhi 110025, India.
International Centre for Genetic Engineering and Biotechnology (ICGEB), Aruna Asaf Ali Marg, New Delhi 110067, India.
Bioorg Chem. 2021 Mar;108:104514. doi: 10.1016/j.bioorg.2020.104514. Epub 2020 Nov 24.
Targeting Falcipain-2 (FP2) for the development of antimalarials is a promising and established concept in antimalarial drug discovery and development. FP2, a member of papain-family cysteine protease of the malaria parasite Plasmodium falciparum holds an important role in hemoglobin degradation pathway. A new series of quinoline carboxamide-based compounds was designed, synthesized and evaluated for antimalarial activity. We integrated molecular hybridization strategy with in-silico drug design to develop FP2 inhibitors. In-vitro results of FP2 inhibition by Qs17, Qs18, Qs20 and Qs21 were found to be in low micromolar range with IC 4.78, 7.37, 2.14 and 2.64 µM, respectively. Among the 25 synthesized compounds, four compounds showed significant antimalarial activities. These compounds also depicted morphological and food-vacuole abnormalities much better than that of E-64, an established FP2 inhibitor. Overall these aromatic substituted quinoline carboxamides can serve as promising leads for the development of novel antimalarial agents.
针对疟原虫裂殖体蛋白 2(FP2)开发抗疟药物是抗疟药物发现和开发中一个有前途且成熟的概念。FP2 是疟原虫恶性疟原虫木瓜蛋白酶家族半胱氨酸蛋白酶的成员,在血红蛋白降解途径中起着重要作用。设计、合成了一系列基于喹啉甲酰胺的化合物,并对其抗疟活性进行了评价。我们将分子杂交策略与计算机药物设计相结合,开发 FP2 抑制剂。Qs17、Qs18、Qs20 和 Qs21 对 FP2 的抑制作用的体外实验结果表明,其 IC 50 值分别为 4.78、7.37、2.14 和 2.64μM。在所合成的 25 种化合物中,有 4 种化合物表现出显著的抗疟活性。这些化合物在形态和食物液泡异常方面也比已建立的 FP2 抑制剂 E-64 表现得更好。总的来说,这些芳香取代的喹啉甲酰胺可以作为开发新型抗疟药物的有前途的先导化合物。
