Multitarget Drug Discovery for Tuberculosis and Other Infectious Diseases
Author(s) -
Kai Li,
Lici A. Schurig-Briccio,
Xinxin Feng,
Ashutosh Upadhyay,
Venugopal Pujari,
Benoît Lechartier,
Fabio L. Fontes,
Hongliang Yang,
Guodong Rao,
Wei Zhu,
Anmol Gulati,
Joo Hwan No,
Giovana Cintra,
Shan Bogue,
Yi-Liang Liu,
Katie J. Molohon,
Peter Orlean,
Douglas A. Mitchell,
Lúcio H. Freitas-Júnior,
Feifei Ren,
Hong Sun,
Tong Jiang,
Yujie Li,
ReyTing Guo,
Stewart T. Cole,
Robert B. Gennis,
Dean C. Crick,
Eric Oldfield
Publication year - 2014
Publication title -
journal of medicinal chemistry
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.01
H-Index - 261
eISSN - 1520-4804
pISSN - 0022-2623
DOI - 10.1021/jm500131s
Subject(s) - mycobacterium tuberculosis , bacteria , chemistry , drug discovery , tuberculosis , biosynthesis , transporter , enzyme , biochemistry , drug resistance , malaria , drug , microbiology and biotechnology , pharmacology , biology , gene , immunology , medicine , genetics , pathology
We report the discovery of a series of new drug leads that have potent activity against Mycobacterium tuberculosis as well as against other bacteria, fungi, and a malaria parasite. The compounds are analogues of the new tuberculosis (TB) drug SQ109 (1), which has been reported to act by inhibiting a transporter called MmpL3, involved in cell wall biosynthesis. We show that 1 and the new compounds also target enzymes involved in menaquinone biosynthesis and electron transport, inhibiting respiration and ATP biosynthesis, and are uncouplers, collapsing the pH gradient and membrane potential used to power transporters. The result of such multitarget inhibition is potent inhibition of TB cell growth, as well as very low rates of spontaneous drug resistance. Several targets are absent in humans but are present in other bacteria, as well as in malaria parasites, whose growth is also inhibited.
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