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粪肠球菌中poxtA扩增和23S rRNA突变导致对利奈唑胺的耐药性增强。

poxtA amplification and mutations in 23S rRNA confer enhanced linezolid resistance in Enterococcus faecalis.

作者信息

Shan Xinxin, Li Chenglong, Zhang Likuan, Zou Chenhui, Yu Runhao, Schwarz Stefan, Shang Yanhong, Li Dexi, Brenciani Andrea, Du Xiang-Dang

机构信息

Animal-Derived Food Safety Innovation Team, College of Animal Science and Technology, Anhui Agricultural University, Hefei 230036, China.

College of Veterinary Medicine, Henan Agricultural University, Zhengzhou 450046, China.

出版信息

J Antimicrob Chemother. 2024 Dec 2;79(12):3199-3203. doi: 10.1093/jac/dkae342.

Abstract

OBJECTIVES

This study aimed to explore the evolutionary patterns and resistance mechanisms of an Enterococcus faecalis strain harbouring poxtA under linezolid exposure.

METHODS

A poxtA-carrying E. faecalis electrotransformant DJH702 with a linezolid minimum inhibitory concentration of 4 mg/L was exposed to increasing concentrations of linezolid (8-64 mg/L). The derived strains growing at 8, 16, 32 and 64 mg/L, designed DJH702_8, DJH702_16, DJH702_32 and DJH702_64, were obtained. The amplification and overexpression of poxtA were measured using sequencing and RT-PCR, the fitness cost by competition assays and the stability of the repeat units by serial passage.

RESULTS

In all derived strains, high-level linezolid resistance develops through poxtA amplification. The relative copy numbers and transcription levels of poxtA were significantly increased. However, in the presence of higher linezolid concentrations, DJH702_32 and DJH702_64 showed reduced poxtA copy numbers and transcription levels compared with DJH702_8 and DJH702_16, but additional mutations in the 23S rRNA (G2505A). IS1216E-mediated formation of translocatable units with subsequent tandem amplification of these translocatable units supported the gain of poxtA segments. However, these amplicons were not stable and were lost frequently in the absence of a linezolid selection pressure. The amplification of the poxtA region did not result in a fitness cost, but mutations in 23S rRNA did.

CONCLUSIONS

poxtA-carrying E. faecalis electrotransformants used two distinct mechanisms to resist linezolid selection pressure: at lower concentrations, strains prioritized increasing poxtA expression levels, while at higher concentrations, a combination of increased poxtA expression and mutations in 23S rRNA was observed.

摘要

目的

本研究旨在探索携带poxtA的粪肠球菌菌株在利奈唑胺暴露下的进化模式和耐药机制。

方法

将利奈唑胺最低抑菌浓度为4 mg/L的携带poxtA的粪肠球菌电转化子DJH702暴露于浓度递增的利奈唑胺(8 - 64 mg/L)中。获得在8、16、32和64 mg/L下生长的衍生菌株,分别命名为DJH702_8、DJH702_16、DJH702_32和DJH702_64。采用测序和RT-PCR检测poxtA的扩增和过表达情况,通过竞争试验检测适应性代价,通过传代培养检测重复单元的稳定性。

结果

在所有衍生菌株中,高水平利奈唑胺耐药通过poxtA扩增产生。poxtA的相对拷贝数和转录水平显著增加。然而,在较高利奈唑胺浓度下,与DJH702_8和DJH702_16相比,DJH702_32和DJH702_64的poxtA拷贝数和转录水平降低,但23S rRNA发生了额外突变(G2505A)。IS1216E介导的可转移单元形成以及随后这些可转移单元的串联扩增支持了poxtA片段的获得。然而,这些扩增子不稳定,在没有利奈唑胺选择压力的情况下经常丢失。poxtA区域的扩增未导致适应性代价,但23S rRNA的突变导致了适应性代价。

结论

携带poxtA的粪肠球菌电转化子利用两种不同机制抵抗利奈唑胺选择压力:在较低浓度下,菌株优先增加poxtA表达水平,而在较高浓度下,观察到poxtA表达增加和23S rRNA突变的组合。

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