School of Pharmacy, East China University of Science and Technology, 130 Mei Long Road, Shanghai 200237, China.
Bioorg Med Chem Lett. 2012 Jan 15;22(2):958-62. doi: 10.1016/j.bmcl.2011.12.011. Epub 2011 Dec 9.
Resistance of malaria parasites has quickly developed to almost all used antimalarial drugs. Accordingly, the discovery of new effective drugs to counter the spread of malaria parasites that are resistant to existing agents, especially acting on multi-targets, is an urgent need. The cysteine protease falcipain-2 (FP-2) and dihydrofolate reductase (DHFR) play crucial roles in the Plasmodium life cycle. In this study, a series of first-gereration small molecular dual inhibitor of FP-2 and DHFR have been designed and synthesized based on the lead compound 1, which was randomly identified by screening FP-2 inhibitors in our laboratory. Six compounds (2f-g, 2j, and 2m-o) showed improved dual inhibitory activities against FP-2 (IC(50)=2.7-13.2μM) and DHFR (IC(50)=1.8-19.8μM), and the inhibitory capability of compound 2o against FP-2 and DHFR were increased ∼8 and ∼6 times than that of compound 1, respectively. Moreover, compound 2o exhibited moderate in vivo antimalarial activity in a dose dependent fashion, its safety and survival rate were slightly better than that of positive drug. The preliminary SAR was obtained, meanwhile, molecular modeling result provided the key structural information to maintain the dual inhibitory activity, and was helpful for future dual inhibitors design.
疟原虫的抗药性已迅速发展到几乎所有已使用的抗疟药物。因此,迫切需要发现新的有效药物来对抗对现有药物具有抗药性的疟原虫的传播,特别是针对多靶点的药物。半胱氨酸蛋白酶 falcipain-2 (FP-2) 和二氢叶酸还原酶 (DHFR) 在疟原虫生命周期中发挥着至关重要的作用。在这项研究中,基于实验室随机筛选 FP-2 抑制剂而发现的先导化合物 1,我们设计并合成了一系列第一代小分子 FP-2 和 DHFR 的双重抑制剂。六种化合物(2f-g、2j 和 2m-o)表现出对 FP-2(IC50=2.7-13.2μM)和 DHFR(IC50=1.8-19.8μM)的双重抑制活性得到了改善,化合物 2o 对 FP-2 和 DHFR 的抑制能力分别比化合物 1 提高了约 8 倍和 6 倍。此外,化合物 2o 在体内具有剂量依赖性抗疟活性,其安全性和存活率略优于阳性药物。同时,获得了初步的 SAR,分子建模结果提供了维持双重抑制活性的关键结构信息,有助于未来的双重抑制剂设计。
