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金黄色葡萄球菌临床分离株中耐甲氧西林的多种机制及改进的检测方法

Multiple mechanisms of methicillin resistance and improved methods for detection in clinical isolates of Staphylococcus aureus.

作者信息

de Lencastre H, Sá Figueiredo A M, Urban C, Rahal J, Tomasz A

机构信息

Rockefeller University, New York, New York 10021-6399.

出版信息

Antimicrob Agents Chemother. 1991 Apr;35(4):632-9. doi: 10.1128/AAC.35.4.632.

Abstract

The mec gene of a number of clinical methicillin-resistant Staphylococcus aureus isolates exhibiting a variety of heterogeneous expression modes was selectively inactivated by allelic replacement mutagenesis. While the resistance level of each of the transformants was reduced, the methicillin MIC for these transformants was well above the MIC for susceptible laboratory strains of S. aureus and was similar to the methicillin MIC for many contemporary clinical isolates which did not react with the mec-specific DNA probe but which showed a low or borderline level of resistance to methicillin. A number of those strains had no detectable beta-lactamase, and for about half of the isolates that did carry plasmid-borne beta-lactamase, elimination of the plasmid caused only partial reduction of the methicillin MIC or no reduction at all. The findings suggest that many contemporary strains of staphylococci harbor a combination of at least three distinct beta-lactam resistance mechanisms: (i) the mechanism related to the acquisition of the foreign mec gene and (ii) a beta-lactamase-dependent and (iii) a beta-lactamase-independent mechanism, each one of which can provide a certain degree of resistance against penicillinase-resistant beta-lactam antibiotics.

摘要

通过等位基因置换诱变,选择性地使一些表现出多种异质表达模式的临床耐甲氧西林金黄色葡萄球菌分离株的mec基因失活。虽然每个转化体的耐药水平都有所降低,但这些转化体的甲氧西林最低抑菌浓度(MIC)远高于金黄色葡萄球菌敏感实验室菌株的MIC,并且与许多当代临床分离株的甲氧西林MIC相似,这些临床分离株不与mec特异性DNA探针反应,但对甲氧西林表现出低水平或临界水平的耐药性。其中一些菌株检测不到β-内酰胺酶,对于约一半携带质粒介导β-内酰胺酶的分离株,去除质粒仅导致甲氧西林MIC部分降低或根本没有降低。这些发现表明,许多当代葡萄球菌菌株至少具有三种不同的β-内酰胺耐药机制:(i)与获得外来mec基因相关的机制,(ii)β-内酰胺酶依赖性机制,以及(iii)β-内酰胺酶非依赖性机制,每一种机制都可以提供一定程度的抗耐青霉素酶β-内酰胺抗生素的能力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/819a/245071/2a871d53f24a/aac00049-0056-a.jpg

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