恶性疟原虫
体外
酶
螯合作用
生物化学
化学
立体化学
生物
药理学
疟疾
免疫学
有机化学
作者
René Chofor,Martijn Risseeuw,Jenny Pouyez,Chinchu Johny,Johan Wouters,Cynthia S. Dowd,Robin D. Couch,Serge Van Calenbergh
出处
期刊:Molecules
[Multidisciplinary Digital Publishing Institute]
日期:2014-02-24
卷期号:19 (2): 2571-2587
被引量:18
标识
DOI:10.3390/molecules19022571
摘要
Fourteen new fosmidomycin analogues with altered metal chelating groups were prepared and evaluated for inhibition of E. coli Dxr, M. tuberculosis Dxr and the growth of P. falciparum K1 in human erythrocytes. None of the synthesized compounds showed activity against either enzyme or the Plasmodia. This study further underlines the importance of the hydroxamate functionality and illustrates that identifying effective alternative bidentate ligands for this target enzyme is challenging.
科研通智能强力驱动
Strongly Powered by AbleSci AI