Influence of femB on methicillin resistance and peptidoglycan metabolism in Staphylococcus aureus.

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J Bacteriol. 1993 March; 175(6): 1612-1620

research-article

Influence of femB on methicillin resistance and peptidoglycan metabolism in Staphylococcus aureus.

U Henze, T Sidow, J Wecke, H Labischinski and B Berger-Bächi

Institute of Medical Microbiology, University of Zürich, Switzerland.

ABSTRACT

The inactivation of FemB by insertion of Tn551 in the centralpart of the femB open reading frame was shown to increase susceptibilityof methicillin-resistant Staphylococcus aureus strains towardbeta-lactam antibiotics to the same extent as did inactivationof femA. Strains carrying the methicillin resistance determinant(mec) and expressing PBP 2' were affected to the same extentas were strains selected for in vitro resistance, which didnot express PBP 2'. Both femA and femB, which form an operon,are involved in a yet unknown manner in the glycine interpeptidebridge formation of the S. aureus peptidoglycan. FemB inactivationwas shown to reduce the glycine content of peptidoglycan byapproximately 40%, depending on the S. aureus strain. The reductionof the interpeptide bridge glycine content led to significantreduction in peptidoglycan cross-linking, as measured by gelpermeation high-pressure liquid chromatography of muramidase-digestedcell walls. Maximum peptide chain length was reduced by approximately40%. It is shown that the complete pentaglycine interpeptidebridge is important for the sensitivity against beta-lactamantibiotics and for the undisturbed activity of the staphylococcalcell wall-synthesizing and hydrolyzing enzymes, as was alsoapparent from electron microscopic examinations, which revealedaberrant placement of cross walls and retarded cell separation,leading to a pseudomulticellular phenotype of the cells forboth femA and femB mutants.

J Bacteriol. 1993 March; 175(6): 1612-1620

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