Literature DB >> 20688819

ClgR regulation of chaperone and protease systems is essential for Mycobacterium tuberculosis parasitism of the macrophage.

Megan Estorninho1, Hilde Smith, Jelle Thole, Jose Harders-Westerveen, Andrzej Kierzek, Rachel E Butler, Olivier Neyrolles, Graham R Stewart.   

Abstract

Chaperone and protease systems play essential roles in cellular homeostasis and have vital functions in controlling the abundance of specific cellular proteins involved in processes such as transcription, replication, metabolism and virulence. Bacteria have evolved accurate regulatory systems to control the expression and function of chaperones and potentially destructive proteases. Here, we have used a combination of transcriptomics, proteomics and targeted mutagenesis to reveal that the clp gene regulator (ClgR) of Mycobacterium tuberculosis activates the transcription of at least ten genes, including four that encode protease systems (ClpP1/C, ClpP2/C, PtrB and HtrA-like protease Rv1043c) and three that encode chaperones (Acr2, ClpB and the chaperonin Rv3269). Thus, M. tuberculosis ClgR controls a larger network of protein homeostatic and regulatory systems than ClgR in any other bacterium studied to date. We demonstrate that ClgR-regulated transcriptional activation of these systems is essential for M. tuberculosis to replicate in macrophages. Furthermore, we observe that this defect is manifest early in infection, as M. tuberculosis lacking ClgR is deficient in the ability to control phagosome pH 1 h post-phagocytosis.

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Year:  2010        PMID: 20688819     DOI: 10.1099/mic.0.042275-0

Source DB:  PubMed          Journal:  Microbiology        ISSN: 1350-0872            Impact factor:   2.777


  32 in total

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6.  Protein aggregation in Ehrlichia chaffeensis during infection of mammalian cells.

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8.  Validation of the essential ClpP protease in Mycobacterium tuberculosis as a novel drug target.

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Journal:  J Bacteriol       Date:  2011-11-28       Impact factor: 3.490

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Journal:  J Bacteriol       Date:  2011-08-05       Impact factor: 3.490

Review 10.  On the design of broad based screening assays to identify potential pharmacological chaperones of protein misfolding diseases.

Authors:  Subhashchandra Naik; Na Zhang; Phillip Gao; Mark T Fisher
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