Design, synthesis, molecular modelling, and in vitro evaluation of tricyclic coumarins against Trypanosoma cruzi

苯硝唑 克鲁兹锥虫 恰加斯病 三环 杀锥虫剂 药理学 硝呋替莫 化学 杀虫药 药品 亚氨基糖 生物化学 立体化学 生物 体外 布氏锥虫 病毒学 寄生虫寄主 万维网 计算机科学 基因
作者
Gleicekelly Silva Coelho,Josimara Souza Andrade,Viviane Flores Xavier,Policarpo Ademar Sales,Barbara Caroline Rodrigues de Araujo,Kátia da Silva Fonseca,Melissa Soares Caetano,Silvane Maria Fonseca Murta,Paula Melo de Abreu Vieira,Cláudia Martins Carneiro,Jason G. Taylor
出处
期刊:Chemical Biology & Drug Design [Wiley]
卷期号:93 (3): 337-350 被引量:15
标识
DOI:10.1111/cbdd.13420
摘要

Abstract Chagas disease is caused by infection with the parasite protozoan Trypanosoma cruzi and affects about 8 million people in 21 countries in Latin America. The main form of treatment of this disease is still based on the use of two drugs, benznidazole and nifurtimox, which both present low cure rates in the chronic phase and often have serious side‐effects. Herein, we describe the synthesis of tricyclic coumarins that were obtained via NHC organocatalysis and evaluation of their trypanocidal activity. Molecular docking studies against trypanosomal enzyme triosephosphate isomerase (TIM) were carried out, as well as a theoretical study of the physicochemical parameters. The tricyclic coumarins were tested in vitro against the intracellular forms of Trypanosoma cruzi . Among the 18 compounds tested, 10 were more active than the reference drug benznidazole. The trypanocidal activity of the lead compound was rationalized by molecular docking study which suggested the strong interaction with the enzyme TIM by T. cruzi and therefore indicating a possible mode of action. Furthermore, the selectivity index of eight tricyclic coumarins with high anti‐ T . cruzi activity was above 50 and thus showing that these lead compounds are viable candidates for further in vivo assays.

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