Literature DB >> 22004792

Pyrazinoic acid efflux rate in Mycobacterium tuberculosis is a better proxy of pyrazinamide resistance.

Mirko Zimic1, Patricia Fuentes, Robert H Gilman, Andrés H Gutiérrez, Daniela Kirwan, Patricia Sheen.   

Abstract

Pyrazinamide is one of the most important drugs in the treatment of latent Mycobacterium tuberculosis infection. The emergence of strains resistant to pyrazinamide represents an important public health problem, as both first- and second-line treatment regimens include pyrazinamide. The accepted mechanism of action states that after the conversion of pyrazinamide into pyrazinoic acid by the bacterial pyrazinamidase enzyme, the drug is expelled from the bacteria by an efflux pump. The pyrazinoic acid is protonated in the extracellular environment and then re-enters the mycobacterium, releasing the proton and causing a lethal disruption of the membrane. Although it has been shown that mutations causing significant loss of pyrazinamidase activity significantly contribute to pyrazinamide resistance, the mechanism of resistance is not completely understood. The pyrazinoic acid efflux rate may depend on multiple factors, including pyrazinamidase activity, intracellular pyrazinamidase concentration, and the efficiency of the efflux pump. Whilst the importance of the pyrazinoic acid efflux rate to the susceptibility to pyrazinamide is recognized, its quantitative effect remains unknown. Thirty-four M. tuberculosis clinical isolates and a Mycobacterium smegmatis strain (naturally resistant to PZA) were selected based on their susceptibility to pyrazinamide, as measured by Bactec 460TB and the Wayne method. For each isolate, the initial velocity at which pyrazinoic acid is released from the bacteria and the initial velocity at which pyrazinamide enters the bacteria were estimated. The data indicated that pyrazinoic acid efflux rates for pyrazinamide-susceptible M. tuberculosis strains fell within a specific range, and M. tuberculosis strains with a pyrazinoic acid efflux rate below this range appeared to be resistant. This finding contrasts with the high pyrazinoic acid efflux rate for M. smegmatis, which is innately resistant to pyrazinamide: its pyrazinoic acid efflux rate was found to be 900 fold higher than the average efflux rate for M. tuberculosis strains. No significant variability was observed in the pyrazinamide flux rate. The pyrazinoic acid efflux rate explained 61% of the variability in Bactec pyrazinamide susceptibility, 24% of Wayne activity, and 51% of the Bactec 460TB growth index. In contrast, pyrazinamidase activity accounted for only 27% of the Bactec pyrazinamide susceptibility. This finding suggests that mechanisms other than pncA mutations (reduction of pyrazinamidase activity) are also implicated in pyrazinamide resistance, and that pyrazinoic acid efflux rate acts as a better proxy for pyrazinamide resistance than the presence of pncA mutations. This is relevant to the design of molecular diagnostics for pyrazinamide susceptibility, which currently rely on pncA gene mutation detection.
Copyright © 2011 Elsevier Ltd. All rights reserved.

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Year:  2011        PMID: 22004792      PMCID: PMC3269536          DOI: 10.1016/j.tube.2011.09.002

Source DB:  PubMed          Journal:  Tuberculosis (Edinb)        ISSN: 1472-9792            Impact factor:   3.131


  30 in total

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2.  Crystal structure and mechanism of catalysis of a pyrazinamidase from Pyrococcus horikoshii.

Authors:  X Du; W Wang; R Kim; H Yakota; H Nguyen; S H Kim
Journal:  Biochemistry       Date:  2001-11-27       Impact factor: 3.162

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Authors:  Yasuhiko Suzuki; Aya Suzuki; Aki Tamaru; Chihiro Katsukawa; Hajime Oda
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4.  pncA mutations as a major mechanism of pyrazinamide resistance in Mycobacterium tuberculosis: spread of a monoresistant strain in Quebec, Canada.

Authors:  S J Cheng; L Thibert; T Sanchez; L Heifets; Y Zhang
Journal:  Antimicrob Agents Chemother       Date:  2000-03       Impact factor: 5.191

Review 5.  The curious characteristics of pyrazinamide: a review.

Authors:  Y Zhang; D Mitchison
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7.  Detection by denaturing gradient gel electrophoresis of pncA mutations associated with pyrazinamide resistance in Mycobacterium tuberculosis isolates from the United States-Mexico border region.

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8.  Mode of action of pyrazinamide: disruption of Mycobacterium tuberculosis membrane transport and energetics by pyrazinoic acid.

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Review 9.  The growing burden of tuberculosis: global trends and interactions with the HIV epidemic.

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10.  Effect of pyrazinamidase activity on pyrazinamide resistance in Mycobacterium tuberculosis.

Authors:  Patricia Sheen; Patricia Ferrer; Robert H Gilman; Jon López-Llano; Patricia Fuentes; Eddy Valencia; Mirko J Zimic
Journal:  Tuberculosis (Edinb)       Date:  2009-02-26       Impact factor: 3.131

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2.  A new approach for pyrazinamide susceptibility testing in Mycobacterium tuberculosis.

Authors:  Mirko Zimic; Sebastian Loli; Robert H Gilman; Andrés Gutierrez; Patricia Fuentes; Milagros Cotrina; Daniela Kirwan; Patricia Sheen
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3.  Redefining multidrug-resistant tuberculosis based on clinical response to combination therapy.

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Journal:  Antimicrob Agents Chemother       Date:  2014-08-04       Impact factor: 5.191

Review 4.  Systematic review of mutations in pyrazinamidase associated with pyrazinamide resistance in Mycobacterium tuberculosis clinical isolates.

Authors:  Sarah M Ramirez-Busby; Faramarz Valafar
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5.  Ameliorative effects of pyrazinoic acid against oxidative and metabolic stress manifested in rats with dimethylhydrazine induced colonic carcinoma.

Authors:  Anil K Sahdev; Vinit Raj; Ashok K Singh; Amit Rai; Amit K Keshari; Arnab De; Amalesh Samanta; Umesh Kumar; Atul Rawat; Dinesh Kumar; Sneha Nath; Anand Prakash; Sudipta Saha
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6.  Clinical application of whole-genome sequencing to inform treatment for multidrug-resistant tuberculosis cases.

Authors:  Adam A Witney; Katherine A Gould; Amber Arnold; David Coleman; Rachel Delgado; Jasvir Dhillon; Marcus J Pond; Cassie F Pope; Tim D Planche; Neil G Stoker; Catherine A Cosgrove; Philip D Butcher; Thomas S Harrison; Jason Hinds
Journal:  J Clin Microbiol       Date:  2015-02-11       Impact factor: 5.948

7.  High Systemic Exposure of Pyrazinoic Acid Has Limited Antituberculosis Activity in Murine and Rabbit Models of Tuberculosis.

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8.  pncA gene expression and prediction factors on pyrazinamide resistance in Mycobacterium tuberculosis.

Authors:  Patricia Sheen; Katherine Lozano; Robert H Gilman; Hugo J Valencia; Sebastian Loli; Patricia Fuentes; Louis Grandjean; Mirko Zimic
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9.  The efflux pump inhibitor timcodar improves the potency of antimycobacterial agents.

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10.  Pyrazinamide susceptibility testing of Mycobacterium tuberculosis by high resolution melt analysis.

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