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Adaptations of Vancomycin-Intermediate Sequence Type 72 Methicillin-Resistant Staphylococcus aureus for Daptomycin Nonsusceptibility

Authors
Lee, Gi YongKang, Kyung MiBack, Seung HyunBaek, Jin YangKim, So HyunPark, Jong-HwanYang, Soo-Jin
Issue Date
Dec-2018
Publisher
MARY ANN LIEBERT, INC
Keywords
ST72 vancomycin-intermediate MRSA; daptomycin; CA-MRSA
Citation
MICROBIAL DRUG RESISTANCE, v.24, no.10, pp 1489 - 1496
Pages
8
Journal Title
MICROBIAL DRUG RESISTANCE
Volume
24
Number
10
Start Page
1489
End Page
1496
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/18044
DOI
10.1089/mdr.2018.0112
ISSN
1076-6294
1931-8448
Abstract
In Korea, the major clonal type of community-associated methicillin-resistant Staphylococcus aureus (CA-MRSA) is sequence type 72 (ST72) with staphylococcal cassette chromosome mec (SCCmec) type IV (ST72-MRSA-IV). In this study, we used a previously well-characterized isogenic pair of ST72 vancomycin (VAN) susceptible-and VAN intermediate-MRSA strains (VSSA303 and VISA072) and several VSSA strains complemented with plasmids expressing single-point mutated genes (dprA(G196C), femA(F92C), vraR(E127K), and vraSR(E127K)) identified in the VISA strain. Using the strain set, we assessed the (1) susceptibilities to daptomycin (DAP) and cationic antimicrobial peptides (CAMPs), (2) alterations in cell envelope phenotypes, such as cell wall autolysis, surface positive charge, and membrane potential (), (3) transcriptional expression profiles of genes involved in surface charge regulation and changes of , and (4) cytokine stimulation profiles in murine macrophages. The vraR(E127K) mutation could enhance surface positive charge through mprF- and dltABCD-independent mechanisms with thickened cell wall. However, none of the single-point mutated genes increased DAP resistance. The DAP nonsusceptible (DAP-NS) phenotype observed in VISA072 strain likely resulted from the combined effects of low and increased positive surface charge. These results suggest that physicochemical alterations in cell envelope are involved in the survival response of DAP-NS VISA072 in sites of infections.
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