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  • Impact of vancomycin on sarA-mediated biofilm formation: role in persistent endovascular infections due to methicillin-resistant Staphylococcus aureus.

Impact of vancomycin on sarA-mediated biofilm formation: role in persistent endovascular infections due to methicillin-resistant Staphylococcus aureus.

The Journal of infectious diseases (2014-01-10)
Wessam Abdelhady, Arnold S Bayer, Kati Seidl, Derek E Moormeier, Kenneth W Bayles, Ambrose Cheung, Michael R Yeaman, Yan Q Xiong
要旨

Staphylococcus aureus is the most common cause of endovascular infections. The staphylococcal accessory regulator A locus (sarA) is a major virulence determinant that may potentially impact methicillin-resistant S. aureus (MRSA) persistence in such infections via its influence on biofilm formation. Two healthcare-associated MRSA isolates from patients with persistent bacteremia and 2 prototypical community-acquired MRSA strains, as well as their respective isogenic sarA mutants, were studied for in vitro biofilm formation, fibronectin-binding capacity, autolysis, and protease and nuclease activities. These assays were done in the presence or absence of sub-minimum inhibitory concentrations (MICs) of vancomycin. In addition, these strain pairs were compared for intrinsic virulence and responses to vancomycin therapy in experimental infective endocarditis, a prototypical biofilm model. All sarA mutants displayed significantly reduced biofilm formation and binding to fibronectin but increased protease production in vitro, compared with their respective parental strains. Interestingly, exposure to sub-MICs of vancomycin significantly promoted biofilm formation and fibronectin-binding in parental strains but not in sarA mutants. In addition, all sarA mutants became exquisitely susceptible to vancomycin therapy, compared with their respective parental strains, in the infective endocarditis model. These observations suggest that sarA activation is important in persistent MRSA endovascular infection, potentially in the setting of biofilm formation.

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製品内容

Sigma-Aldrich
バンコマイシン 塩酸塩 Streptomyces orientalis由来, ≥900 μg per mg (as vancomycin base)
Sigma-Aldrich
バンコマイシン 塩酸塩 Streptomyces orientalis由来, ≥85% (Vancomycin B)
Sigma-Aldrich
バンコマイシン 塩酸塩 Streptomyces orientalis由来, BioReagent, suitable for plant cell culture
Sigma-Aldrich
バンコマイシン 塩酸塩 Streptomyces orientalis由来, meets USP testing specifications
Millipore
バンコマイシン 塩酸塩, suitable for microbiology