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High-Content Phenotypic Screen of a Focused TCAMS Drug Library Identifies Novel Disruptors of the Malaria Parasite Calcium Dynamics

血凝蛋白 恶性疟原虫 青蒿素 生物 细胞毒性 氯喹 药效团 程序性细胞死亡 血红素 生物化学 疟疾 药理学 化学 细胞生物学 体外 细胞凋亡 免疫学 有机化学
作者
Wan-Ni Chia,Marı́a G. Gómez-Lorenzo,Isabel Castellote,Jie Xin Tong,Rajesh Chandramohanadas,Trang Thi Thu Chu,Wan Xiang Shen,Mei‐Lin Go,Cristina de Cózar,Benigno Crespo,María Jesús Almela,Fernando Neria,Virginia Franco,Francisco‐Javier Gamo,Kevin S. W. Tan
出处
期刊:ACS Chemical Biology [American Chemical Society]
卷期号:16 (11): 2348-2372 被引量:5
标识
DOI:10.1021/acschembio.1c00512
摘要

The search for new antimalarial drugs with unexplored mechanisms of action is currently one of the main objectives to combat the resistance already in the clinic. New drugs should target specific mechanisms that once initiated lead inevitably to the parasite's death and clearance and cause minimal toxicity to the host. One such new mode of action recently characterized is to target the parasite's calcium dynamics. Disruption of the calcium homeostasis is associated with compromised digestive vacuole membrane integrity and release of its contents, leading to programmed cell death-like features characterized by loss of mitochondrial membrane potential and DNA degradation. Intriguingly, chloroquine (CQ)-treated parasites were previously reported to exhibit such cellular features. Using a high-throughput phenotypic screen, we identified 158 physiological disruptors (hits) of parasite calcium distribution from a small subset of approximately 3000 compounds selected from the GSK TCAMS (Tres Cantos Anti-Malarial Set) compound library. These compounds were then extensively profiled for biological activity against various CQ- and artemisinin-resistant Plasmodium falciparum strains and stages. The hits were also examined for cytotoxicity, speed of antimalarial activity, and their possible inhibitory effects on heme crystallization. Overall, we identified three compounds, TCMDC-136230, -125431, and -125457, which were potent in inducing calcium redistribution but minimally inhibited heme crystallization. Molecular superimposition of the molecules by computational methods identified a common pharmacophore, with the best fit assigned to TCMDC-125457. There were low cytotoxicity or CQ cross-resistance issues for these three compounds. IC50 values of these three compounds were in the low micromolar range. In addition, TCMDC-125457 demonstrated high efficacy when pulsed in a single-dose combination with artesunate against tightly synchronized artemisinin-resistant ring-stage parasites. These results should add new drug options to the current armament of antimalarial drugs as well as provide promising starting points for development of drugs with non-classical modes of action.

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