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Pyrazinoic Acid Inhibits the Bifunctional Enzyme (Rv2783) in Mycobacterium tuberculosis by Competing with tmRNA.


ABSTRACT: Pyrazinamide (PZA) is a key drug for tuberculosis treatment. The active form of PZA, pyrazinoic acid (POA), appears to inhibit multiple targets in M. tuberculosis. Recently, the bifunctional enzyme Rv2783 was reported as a new target of POA. However, the mechanism by which POA inhibits Rv2783 is not yet clear. Here, we report how a new A2104C substitution in Rv2783c, identified in PZA-resistant clinical isolates, conferred resistance to PZA in M. tuberculosis. Expression of the mutant allele recapitulated the PZA resistance. All catalytic activities of Rv2783, but not the mutant, were inhibited by POA. Additionally, POA competed with transfer-messenger RNA (tmRNA) for binding to Rv2783, other than the mutant. These results provide new insight into the molecular mechanism of the antitubercular activity of PZA.

SUBMITTER: He L 

PROVIDER: S-EPMC6963974 | biostudies-literature | 2019 Nov

REPOSITORIES: biostudies-literature

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Pyrazinoic Acid Inhibits the Bifunctional Enzyme (Rv2783) in <i>Mycobacterium tuberculosis</i> by Competing with tmRNA.

He Lei L   Cui Peng P   Shi Wanliang W   Li Qiong Q   Zhang Wenhong W   Li Min M   Zhang Ying Y  

Pathogens (Basel, Switzerland) 20191112 4


Pyrazinamide (PZA) is a key drug for tuberculosis treatment. The active form of PZA, pyrazinoic acid (POA), appears to inhibit multiple targets in <i>M. tuberculosis.</i> Recently, the bifunctional enzyme Rv2783 was reported as a new target of POA. However, the mechanism by which POA inhibits Rv2783 is not yet clear. Here, we report how a new A2104C substitution in <i>Rv2783c</i>, identified in PZA-resistant clinical isolates, conferred resistance to PZA in <i>M. tuberculosis</i>. Expression of  ...[more]

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