鲍曼不动杆菌中 trm 编码的 SAM 依赖型甲基转移酶突变导致替加环素敏感性降低。
Decreased susceptibility to tigecycline in Acinetobacter baumannii mediated by a mutation in trm encoding SAM-dependent methyltransferase.
机构信息
Department of Infectious Diseases, Sir Run Run Shaw Hospital, College of Medicine, Zhejiang University, Hangzhou, Zhejiang 310016, China.
出版信息
J Antimicrob Chemother. 2014 Jan;69(1):72-6. doi: 10.1093/jac/dkt319. Epub 2013 Aug 8.
OBJECTIVES
Acinetobacter baumannii is an important opportunistic pathogen and multidrug-resistant isolate. Although tigecycline is a potent antibiotic for treating infections with multidrug-resistant isolates, resistance is becoming a problem. This study aimed to explore the mechanism of tigecycline resistance in A. baumannii.
METHODS
A serial passage experiment was performed to collect isolates selected by tigecycline. The expression of efflux pumps was quantified in the final selected isolate, 19606-T8. The whole genome of 19606-T8 was sequenced and the putative mutations were confirmed using PCR and Sanger sequencing. A complementation experiment was performed to evaluate the contribution of the mutations to decreased susceptibility to tigecycline. The significance of a deletion mutation was further investigated in terms of growth rate and antibiotic susceptibilities.
RESULTS
We collected serial isolates by selective pressure of tigecycline, and designated them 19606-T1 to 19606-T8. The efflux pumps AdeABC, AdeFGH and AdeIJK were not overexpressed in 19606-T8, which had decreased susceptibility to tigecycline. Isolate 19606-T8 carried one deletion mutation in trm and three non-synonymous substitutions in msbA (A84V), lolA (P91L) and filC (N168K). The deletion mutation in trm (encoding S-adenosyl-L-methionine-dependent methyltransferase) resulted in decreased susceptibility to tigecycline as well as to minocycline and doxycycline. In complementation experiments, the MICs of tigecycline, minocycline and doxycycline in a tigecycline-resistant isolate were restored by complementation with wild-type trm.
CONCLUSIONS
Given that the deletion mutation in trm was associated with decreased susceptibility to tigecycline and that a wild-type trm plasmid could restore the susceptibility, trm is considered to play an important role in decreased susceptibility to tigecycline in A. baumannii.
目的
鲍曼不动杆菌是一种重要的机会致病菌和多药耐药分离株。虽然替加环素是治疗多药耐药分离株感染的有效抗生素,但耐药性已成为一个问题。本研究旨在探讨鲍曼不动杆菌对替加环素耐药的机制。
方法
通过替加环素的选择压力进行连续传代实验,收集分离株。在最终选择的分离株 19606-T8 中定量测定外排泵的表达。对 19606-T8 的全基因组进行测序,并通过 PCR 和 Sanger 测序确认假定的突变。进行互补实验以评估突变对降低替加环素敏感性的贡献。从生长速度和抗生素敏感性方面进一步研究缺失突变的意义。
结果
我们通过替加环素的选择压力收集了一系列连续分离株,并将其命名为 19606-T1 至 19606-T8。在对替加环素敏感性降低的 19606-T8 中,并没有过度表达 AdeABC、AdeFGH 和 AdeIJK 外排泵。19606-T8 携带 trm 中的一个缺失突变和 msbA(A84V)、lolA(P91L)和 filC(N168K)中的三个非同义取代。trm(编码 S-腺苷-L-甲硫氨酸依赖性甲基转移酶)中的缺失突变导致对替加环素以及米诺环素和强力霉素的敏感性降低。在互补实验中,通过用野生型 trm 互补,替加环素耐药分离株的替加环素、米诺环素和强力霉素的 MIC 值得以恢复。
结论
鉴于 trm 中的缺失突变与替加环素敏感性降低有关,并且野生型 trm 质粒可以恢复敏感性,因此 trm 被认为在鲍曼不动杆菌对替加环素的敏感性降低中起重要作用。
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