TB drug discovery: addressing issues of persistence and resistance - 22/08/11
Abstract |
Tuberculosis remains a leading cause of mortality worldwide into the 21st century. Among the main obstacles to the global control of the disease are emerging multi-drug resistant strains and the recalcitrance of persistent infections to treatment with conventional anti-TB drugs. Here we review recent developments in our understanding of some of the pathways involved in a persistent infection and pathogenesis of Mycobacterium tuberculosis, which reveal new targets for drug development. We describe the high-resolution crystal structures of enzymes of the glyoxylate shunt, isocitrate lyase and malate synthase, and of the cyclopropane synthases of mycolic acid biosynthesis. Structure-based drug design is now underway with the potential to lead to the development of new anti-tuberculars effective against persistent and resistant Mycobacterium tuberculosis infections.
Le texte complet de cet article est disponible en PDF.Keywords : Tuberculosis, Mycolic acid, Glyoxylate shunt, Isocitrate lyase, Malate synthase, Persistence, Resistance, Cyclopropane synthase, Potential drug target, Structure-based drug design
Plan
Vol 84 - N° 1-2
P. 45-55 - 2004 Retour au numéro
Article précédent
- M. tuberculosis persistence, latency, and drug tolerance
- James E Gomez, John D McKinney
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- Suriyati Mohamad, Pazilah Ibrahim, Amirin Sadikun
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