Expression of Mycobacterium smegmatis Pyrazinamidase in Mycobacterium tuberculosis Confers Hypersensitivity to Pyrazinamide and Related Amides

doi:10.1128/JB.182.19.5479-5485.2000

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Journal of Bacteriology, October 2000, p. 5479-5485, Vol. 182, No. 19
0021-9193/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Expression of Mycobacterium smegmatis Pyrazinamidase in Mycobacterium tuberculosis Confers Hypersensitivity to Pyrazinamide and Related Amides

Helena I. M. Boshoff and Valerie Mizrahi^*

MRC/SAIMR/WITS Molecular Mycobacteriology Research Unit, South African Institute for Medical Research, and Department of Molecular Medicine and Haematology, University of the Witwatersrand Medical School, Johannesburg, South Africa

Received 1 March 2000/Accepted 5 July 2000

A pyrazinamidase (PZase)-deficient pncA mutant of Mycobacterium tuberculosis, constructed by allelic exchange, was used toinvestigate the effects of heterologous amidase gene expressionon the susceptibility of this organism to pyrazinamide (PZA) andrelated amides. The mutant was highly resistant to PZA (MIC, >2,000µg/ml), in accordance with the well-established role of pncA inthe PZA susceptibility of M. tuberculosis (A. Scorpio and Y. Zhang,Nat. Med. 2:662-667, 1996). Integration of the pzaA gene encodingthe major PZase/nicotinamidase from Mycobacterium smegmatis (H.I. M. Boshoff and V. Mizrahi, J. Bacteriol. 180:5809-5814, 1998)or the M. tuberculosis pncA gene into the pncA mutant complementedits PZase/nicotinamidase defect. In both pzaA- and pncA-complementedmutant strains, the PZase activity was detected exclusively inthe cytoplasm, suggesting an intracellular localization for PzaAand PncA. The pzaA-complemented strain was hypersensitive to PZA(MIC, $<=$ 10 µg/ml) and nicotinamide (MIC, $>=$ 20 µg/ml) and was alsosensitive to benzamide (MIC, 20 µg/ml), unlike the wild-type andpncA-complemented mutant strains, which were highly resistantto this amide (MIC, >500 µg/ml). This finding was consistent withthe observation that benzamide is hydrolyzed by PzaA but not byPncA. Overexpression of PzaA also conferred sensitivity to PZA,nicotinamide, and benzamide on M. smegmatis (MIC, 150 µg/ml inall cases) and rendered Escherichia coli hypersensitive for growthat lowpH.

^* Corresponding author. Mailing address: MRC/SAIMR/WITS Molecular Mycobacteriology Research Unit, SAIMR, P.O. Box 1038, Johannesburg2000, South Africa. Phone: 2711-4899370. Fax: 2711-4899001. E-mail:075val{at}chiron.wits.ac.za.

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