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Hsp100/Clp protease complexes are molecular machines important for cellular protein homeostasis and are concurrently embedded in the control of various signal transduction networks by regulatory proteolysis. In Mycobacteria, the genes encoding the components of these Hsp100/Clp protease complexes are essential for growth and were identified as targets for antibiotics, with a new antimicrobial mechanism, that are active on slow growing or even dormant cells. Schmitz and Sauer (2014) report the biochemical characterization of mycobacterial Hsp100/Clp protease complexes actively degrading folded substrate proteins. Their results suggest an unusual activation mechanism for this protease complex and will set the stage for further mechanistic studies of antibiotics acting on this new cellular target. © 2014 John Wiley & Sons Ltd.

Citation

Noël Molière, Kürşad Turgay. The key to unlock the Hsp100/Clp protein degradation machines of Mycobacterium. Molecular microbiology. 2014 Aug;93(4):583-6

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PMID: 24979233

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