恰加斯病
克鲁兹锥虫
锥虫病
疾病
化学
药理学
病毒学
寄生虫寄主
生物
医学
内科学
计算机科学
万维网
作者
Justin R. Harrison,Sandipan Sarkar,Shahienaz E. Hampton,Jennifer Riley,Laste Stojanovski,Christer Sahlberg,Pia Appelqvist,Jessey Erath,Vinodhini Mathan,Ana Rodrı́guez,Marcel Kaiser,Dolores González Pacanowska,Kevin D. Read,Nils Gunnar Johansson,Ian H. Gilbert
标识
DOI:10.1021/acs.jmedchem.9b01852
摘要
Chagas disease is caused by the protozoan parasite Trypanosoma cruzi. It is endemic in South and Central America and recently has been found in other parts of the world, due to migration of chronically infected patients. The current treatment for Chagas disease is not satisfactory, and there is a need for new treatments. In this work, we describe the optimization of a hit compound resulting from the phenotypic screen of a library of compounds against T. cruzi. The compound series was optimized to the level where it had satisfactory pharmacokinetics to allow an efficacy study in a mouse model of Chagas disease. We were able to demonstrate efficacy in this model, although further work is required to improve the potency and selectivity of this series.
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