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抗金黄色葡萄球菌小菌落变异体的抗生素活性:体外、动物和临床数据的综述。

Antibiotic activity against small-colony variants of Staphylococcus aureus: review of in vitro, animal and clinical data.

机构信息

Pharmacologie cellulaire et moléculaire & Louvain Drug Research Institute, Université catholique de Louvain, Brussels, Belgium.

出版信息

J Antimicrob Chemother. 2013 Jul;68(7):1455-64. doi: 10.1093/jac/dkt072. Epub 2013 Mar 13.

Abstract

The pathogen Staphylococcus aureus uses various strategies for persisting in the host, among which switching to a small-colony variant (SCV) phenotype is of particular biological and therapeutic significance. Phenotypically, SCVs are characterized by a slow growth rate, atypical colony morphology and unusual biochemical features, constituting a real challenge for identification by the clinical microbiology laboratory. Their metabolic defects also alter their susceptibility to antibiotics, which, combined with the ability to survive intracellularly and, for some strains, to form biofilms, largely contributes to therapeutic failures. This paper reviews the available literature on antibiotic activity against SCVs of S. aureus in vitro, in animal models and in clinics. In vitro, aminoglycosides and antifolate agents show high MICs for electron-transport-defective and thymidine-dependent SCVs, respectively. The other antibiotic classes usually show MICs comparable to those measured for the parental strains, but they are less bactericidal. Intracellularly, auxotrophs for thymidine, haemin or menadione show contrasting behaviours with respect to their response to antibiotics, resulting from differences in their intracellular fate. In animal models, SCVs often persist in various locations, including metastatic ones, in spite of the administration of active antibiotics. In healthcare, several case reports mention the selection of SCVs after prolonged administration of not only aminoglycosides and antifolate agents, but also several other antibiotic classes. Apparent eradication requires several weeks or even months of aggressive polytherapy combined, whenever possible, with surgical intervention. Further research is thus warranted for optimizing the treatment of infections caused by SCVs.

摘要

金黄色葡萄球菌利用各种策略在宿主体内存活,其中转变为小菌落变异体(SCV)表型具有特殊的生物学和治疗意义。表型上,SCVs 的特征是生长缓慢、典型菌落形态和异常生化特征,这给临床微生物学实验室的鉴定带来了真正的挑战。它们的代谢缺陷也改变了它们对抗生素的敏感性,再加上能够在细胞内生存,以及某些菌株能够形成生物膜,这在很大程度上导致了治疗失败。本文综述了金黄色葡萄球菌 SCV 在体外、动物模型和临床中的抗生素活性的相关文献。在体外,氨基糖苷类和抗叶酸剂分别对电子传递缺陷和胸苷依赖性 SCV 表现出高 MIC。其他抗生素类别通常表现出与亲本菌株相当的 MIC,但杀菌活性较低。在细胞内,胸苷、血红素或亚甲蓝营养缺陷型对抗生素的反应表现出不同的行为,这是由于它们在细胞内命运的差异。在动物模型中,SCVs 经常在各种部位(包括转移性部位)存在,尽管给予了有效的抗生素。在医疗保健中,有几个病例报告提到,在长时间使用氨基糖苷类和抗叶酸剂以及其他几种抗生素类别后,会选择 SCVs。要明显清除 SCVs 需要数周甚至数月的强化联合治疗,如有可能,还需要结合手术干预。因此,需要进一步研究以优化 SCVs 引起的感染的治疗方法。

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