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葡萄球菌中的耐甲氧西林特性:分子与生化基础及临床意义

Methicillin resistance in staphylococci: molecular and biochemical basis and clinical implications.

作者信息

Chambers H F

机构信息

Medical Service, San Francisco General Hospital 94143, USA.

出版信息

Clin Microbiol Rev. 1997 Oct;10(4):781-91. doi: 10.1128/CMR.10.4.781.

Abstract

Methicillin resistance in staphylococci is determined by mec, composed of 50 kb or more of DNA found only in methicillin-resistant strains. mec contains mecA, the gene for penicillin-binding protein 2a (PBP 2a); mecI and mecR1, regulatory genes controlling mecA expression; and numerous other elements and resistance determinants. A distinctive feature of methicillin resistance is its heterogeneous expression. Borderline resistance, a low-level type of resistance to methicillin exhibited by strains lacking mecA, is associated with modifications in native PBPs, beta-lactamase hyperproduction, or possibly a methicillinase. The resistance phenotype is influenced by numerous factors, including mec and beta-lactamase (bla) regulatory elements, fem factors, and yet to be identified chromosomal loci. The heterogeneous nature of methicillin resistance confounds susceptibility testing. Methodologies based on the detection of mecA are the most accurate. Vancomycin is the drug of choice for treatment of infection caused by methicillin-resistant strains. PBP 2a confers cross-resistance to most currently available beta-lactam antibiotics. Investigational agents that bind PBP 2a at low concentrations appear promising but have not been tested in humans. Alternatives to vancomycin are few due to the multiple drug resistances typical of methicillin-resistant staphylococci.

摘要

葡萄球菌对甲氧西林的耐药性由mec决定,mec由50 kb或更多的DNA组成,仅在耐甲氧西林菌株中发现。mec包含mecA,即青霉素结合蛋白2a(PBP 2a)的基因;mecI和mecR1,控制mecA表达的调控基因;以及许多其他元件和耐药决定因素。甲氧西林耐药性的一个显著特征是其异质性表达。临界耐药性是缺乏mecA的菌株对甲氧西林表现出的一种低水平耐药类型,与天然PBP的修饰、β-内酰胺酶的过度产生或可能的一种甲氧西林酶有关。耐药表型受多种因素影响,包括mec和β-内酰胺酶(bla)调控元件、fem因子以及尚未确定的染色体位点。甲氧西林耐药性的异质性使药敏试验变得复杂。基于检测mecA的方法是最准确的。万古霉素是治疗由耐甲氧西林菌株引起的感染的首选药物。PBP 2a赋予对大多数目前可用的β-内酰胺类抗生素的交叉耐药性。低浓度结合PBP 2a的研究性药物似乎很有前景,但尚未在人体中进行测试。由于耐甲氧西林葡萄球菌典型的多重耐药性,万古霉素的替代药物很少。

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