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一种与氟喹诺酮类药物耐药性相关的突变 gyrA 影响空肠弯曲菌的 DNA 超螺旋结构。

A fluoroquinolone resistance associated mutation in gyrA Affects DNA supercoiling in Campylobacter jejuni.

机构信息

Department of Veterinary Microbiology and Preventive Medicine, Iowa State University Ames, IA, USA.

出版信息

Front Cell Infect Microbiol. 2012 Mar 1;2:21. doi: 10.3389/fcimb.2012.00021. eCollection 2012.

Abstract

The prevalence of fluoroquinolone (FQ)-resistant Campylobacter has become a concern for public health. To facilitate the control of FQ-resistant (FQ(R)) Campylobacter, it is necessary to understand the impact of FQ(R) on the fitness of Campylobacter in its natural hosts as understanding fitness will help to determine and predict the persistence of FQ(R)Campylobacter. Previously it was shown that acquisition of resistance to FQ antimicrobials enhanced the in vivo fitness of FQ(R)Campylobacter. In this study, we confirmed the role of the Thr-86-Ile mutation in GyrA in modulating Campylobacter fitness by reverting the mutation to the wild-type (WT) allele, which resulted in the loss of the fitness advantage. Additionally, we determined if the resistance-conferring GyrA mutations alter the enzymatic function of the DNA gyrase. Recombinant WT gyrase and mutant gyrases with three different types of mutations (Thr-86-Ile, Thr-86-Lys, and Asp-90-Asn), which are associated with FQ(R) in Campylobacter, were generated in E. coli and compared for their supercoiling activities using an in vitro assay. The mutant gyrase with the Thr-86-Ile change showed a greatly reduced supercoiling activity compared with the WT gyrase, while other mutant gyrases did not show an altered supercoiling. Furthermore, we measured DNA supercoiling within Campylobacter cells using a reporter plasmid. Consistent with the results from the in vitro supercoiling assay, the FQ(R) mutant carrying the Thr-86-Ile change in GyrA showed much less DNA supercoiling than the WT strain and the mutant strains carrying other mutations. Together, these results indicate that the Thr-86-Ile mutation, which is predominant in clinical FQ(R)Campylobacter, modulates DNA supercoiling homeostasis in FQ(R)Campylobacter.

摘要

氟喹诺酮(FQ)耐药弯曲杆菌的流行引起了公众健康的关注。为了便于控制 FQ 耐药(FQ(R))弯曲杆菌,了解 FQ(R)对其天然宿主中弯曲杆菌适应性的影响是必要的,因为了解适应性有助于确定和预测 FQ(R)弯曲杆菌的持久性。先前已经表明,对 FQ 抗菌药物的耐药性获得增强了 FQ(R)弯曲杆菌的体内适应性。在这项研究中,我们通过将突变恢复为野生型(WT)等位基因来证实 GyrA 中 Thr-86-Ile 突变在调节弯曲杆菌适应性中的作用,这导致了适应性优势的丧失。此外,我们确定了耐药性赋予的 GyrA 突变是否改变了 DNA 回旋酶的酶促功能。在大肠杆菌中生成了重组 WT 回旋酶和具有三种不同类型突变(Thr-86-Ile、Thr-86-Lys 和 Asp-90-Asn)的突变回旋酶,这些突变与弯曲杆菌中的 FQ(R)相关联,并在体外测定中比较了它们的超螺旋活性。与 WT 回旋酶相比,带有 Thr-86-Ile 变化的突变回旋酶显示出大大降低的超螺旋活性,而其他突变回旋酶则没有显示出改变的超螺旋。此外,我们使用报告质粒测量了弯曲杆菌细胞内的 DNA 超螺旋。与体外超螺旋测定的结果一致,携带 GyrA 中 Thr-86-Ile 变化的 FQ(R)突变体显示出比 WT 菌株和携带其他突变的突变菌株更少的 DNA 超螺旋。总之,这些结果表明,在临床 FQ(R)弯曲杆菌中占主导地位的 Thr-86-Ile 突变调节了 FQ(R)弯曲杆菌中的 DNA 超螺旋动态平衡。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0986/3417464/15b2e10cdbdd/fcimb-02-00021-g001.jpg

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