Sequential inactivation of rdxA (HP0954) and frxA (HP0642) nitroreductase genes causes moderate and high-level metronidazole resistance in Helicobacter pylori

Jeong, Jin-Yong ; Mukhopadhyay, Asish K. ; Dailidiene, Daiva ; Wang, Yipeng ; Velapatiño, Billie ; Gilman, Robert H. ; Parkinson, Alan J. ; Balakrish Nair, G. ; Wong, Benjamin C. Y. ; Lam, Shiu Kum ; Mistry, Rajesh ; Segal, Isidore ; Yuan, Yuan ; Gao, Hua ; Alarcon, Teresa ; Brea, MaNuel Lopez ; Ito, Yoshiyuki ; Kersulyte, Dangeruta ; Lee, Hae-Kyung ; Gong, Yan ; Goodwin, Avery ; Hoffman, Paul S. ; Berg, Douglas E. (2000) Sequential inactivation of rdxA (HP0954) and frxA (HP0642) nitroreductase genes causes moderate and high-level metronidazole resistance in Helicobacter pylori Jouranl of Bacteriology, 182 (18). pp. 5082-5090. ISSN 0021-9193

Full text not available from this repository.

Official URL: http://jb.asm.org/content/182/18/5082.short

Related URL: http://dx.doi.org/10.1128/JB.182.18.5082-5090.2000

Abstract

Helicobacter pylori is a human-pathogenic bacterial species that is subdivided geographically, with different genotypes predominating in different parts of the world. Here we test and extend an earlier conclusion that metronidazole (Mtz) resistance is due to mutation in rdxA (HP0954), which encodes a nitroreductase that converts Mtz from prodrug to bactericidal agent. We found that (i) rdxA genes PCR amplified from 50 representative Mtzr strains from previously unstudied populations in Asia, South Africa, Europe, and the Americas could, in each case, transform Mtzs H. pylori to Mtzr; (ii) Mtzr mutant derivatives of a cultured Mtzsstrain resulted from mutation in rdxA; and (iii) transformation of Mtzs strains with rdxA-null alleles usually resulted in moderate level Mtz resistance (16 µg/ml). However, resistance to higher Mtz levels was common among clinical isolates, a result that implicates at least one additional gene. Expression in Escherichia coli offrxA (HP0642; flavin oxidoreductase), anrdxA paralog, made this normally resistant species Mtzs, and frxA inactivation enhanced Mtz resistance in rdxA-deficient cells but had little effect on the Mtz susceptibility of rdxA+ cells. Strains carrying frxA-null and rdxA-null alleles could mutate to even higher resistance, a result implicating one or more additional genes in residual Mtz susceptibility and hyperresistance. We conclude that most Mtz resistance in H. pylori depends onrdxA inactivation, that mutations in frxA can enhance resistance, and that genes that confer Mtz resistance withoutrdxA inactivation are rare or nonexistent in H. pylori populations.

Item Type:Article
Source:Copyright of this article belongs to American Society for Microbiology.
ID Code:82035
Deposited On:09 Feb 2012 04:30
Last Modified:09 Feb 2012 04:30

Repository Staff Only: item control page