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通过使用一株经过特定缺失改造的、对抗生素敏感的淡紫链霉菌菌株来表征大环内酯-林可酰胺-链阳菌素B耐药表型。

The macrolide-lincosamide-streptogramin B resistance phenotypes characterized by using a specifically deleted, antibiotic-sensitive strain of Streptomyces lividans.

作者信息

Pernodet J L, Fish S, Blondelet-Rouault M H, Cundliffe E

机构信息

Laboratoire de Biologie et Génétique Moléculaire, Université Paris-Sud XI, Orsay, France.

出版信息

Antimicrob Agents Chemother. 1996 Mar;40(3):581-5. doi: 10.1128/AAC.40.3.581.

Abstract

Genes conferring resistance to macrolide, lincosamide, and streptogramin B (MLS) antibiotics via ribosomal modification are widespread in bacteria, including clinical isolates and MLS-producing actinomycetes. Such erm-type genes encode enzymes that mono- or dimethylate residue A-2058 of 23S rRNA. The different phenotypes resulting from monomethylation (MLS-I phenotype, conferred by erm type I genes) or dimethylation (MLS-II phenotype due to erm type II genes) have been characterized by introducing tlrD or ermE, respectively, into an MLS-sensitive derivative of Streptomyces lividans TK21. This strain (designated OS456) was generated by specific replacement of the endogenous resistance genes lrm and mgt. The MLS-I phenotype is characterized by high-level resistance to lincomycin with only marginal resistance to macrolides such as chalcomycin or tylosin, whereas the MLS-II phenotype involves high-level resistance to all MLS drugs. Mono- and dimethylated ribosomes were introduced into a cell-free protein-synthesizing system prepared from S. lividans and compared with unmodified particles in their response to antibiotics. There was no simple correlation between the relative potencies of MLS drugs at the level of the target site (i.e., the ribosome) and their antibacterial activities expressed as MICs.

摘要

通过核糖体修饰赋予对大环内酯类、林可酰胺类和链阳菌素B(MLS)抗生素抗性的基因在细菌中广泛存在,包括临床分离株和产生MLS的放线菌。此类erm型基因编码使23S rRNA的A-2058残基发生单甲基化或二甲基化的酶。分别将tlrD或ermE导入变铅青链霉菌TK21的MLS敏感衍生物中,已对单甲基化(由erm I型基因赋予的MLS-I表型)或二甲基化(由于erm II型基因导致的MLS-II表型)产生的不同表型进行了表征。该菌株(命名为OS456)是通过特异性替换内源性抗性基因lrm和mgt产生的。MLS-I表型的特征是对林可霉素具有高水平抗性,而对诸如加洛霉素或泰乐菌素等大环内酯类仅具有微弱抗性,而MLS-II表型则涉及对所有MLS药物的高水平抗性。将单甲基化和二甲基化的核糖体引入由变铅青链霉菌制备的无细胞蛋白质合成系统中,并将其对抗生素的反应与未修饰的颗粒进行比较。在靶位点(即核糖体)水平上MLS药物的相对效力与其以MIC表示的抗菌活性之间没有简单的相关性。

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