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Review
. 2008 Jan:14 Suppl 1:53-62.
doi: 10.1111/j.1469-0691.2007.01849.x.

IRT and CMT beta-lactamases and inhibitor resistance

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Free article
Review

IRT and CMT beta-lactamases and inhibitor resistance

R Cantón et al. Clin Microbiol Infect. 2008 Jan.
Free article

Erratum in

  • Clin Microbiol Infect. 2008 Mar;14(3):293. Martín, O [removed]; de la Maza, S [corrected to de la Maza, O Martín S]
  • Clin Microbiol Infect. 2008 May;14 Suppl 5:21-4

Abstract

Acquired resistance to penicillin-beta-lactamase inhibitor combinations in Escherichia coli is due to: (i) penicillinase hyperproduction due to the presence of the bla(TEM-1) gene in small multicopy plasmids or strong promoters; (ii) overproduction of constitutive AmpC cephalosporinase; and (iii) OXA-type and inhibitor-resistant TEM (IRT) beta-lactamases. IRT enzymes emerge via mutational events from TEM-1 or TEM-2 beta-lactamases that affect substrate affinity for beta-lactamase inhibitors. They are mainly isolated in urinary infections from community patients. Prevalence is variable, depending on geographical area, detection methods and potential selection pressure. These enzymes may evolve into complex mutants (CMT enzymes), which also confer resistance to extended-spectrum cephalosporins. CTX-M enzymes with the IRT phenotype have not been detected to date. New studies of IRT enzymes, including population structure, association with virulence traits and plasmid dispersion, are needed.

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