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多重耐药鲍曼不动杆菌在感染和治疗期间的基因组动态变化

Genome dynamics of multidrug-resistant Acinetobacter baumannii during infection and treatment.

作者信息

Wright Meredith S, Iovleva Alina, Jacobs Michael R, Bonomo Robert A, Adams Mark D

机构信息

The J. Craig Venter Institute, La Jolla, CA, USA.

Department of Medicine, University Hospitals Case Medical Center, Cleveland, OH, USA.

出版信息

Genome Med. 2016 Mar 3;8(1):26. doi: 10.1186/s13073-016-0279-y.

Abstract

BACKGROUND

Limited treatment options are available for patients infected with multidrug (MDR)- or pan-drug (PDR)-resistant bacterial pathogens, resulting in infections that can persist for weeks or months. In order to better understand transmission and evolutionary dynamics of MDR Acinetobacter baumannii (Ab) during long-term infection, we analyzed genomes from a series of isolates from individual patients at isolate-specific, patient-specific, and population levels.

METHODS

Whole genome analysis of longitudinal isolates (range 2-10 isolates per patient spanning 0-829 days) from 40 patients included detection of single-nucleotide variants (SNVs), insertion sequence (IS) mapping, and gene content changes.

RESULTS

Phylogenetic analysis revealed that a significant fraction of apparently persistent infections are in fact due to re-infection with new strains. SNVs primarily resulted in protein coding changes, and IS events primarily interrupted genes or were in an orientation such that the adjacent gene would be over-expressed. Mutations acquired during infection were over-represented in transcriptional regulators, notably pmrAB and adeRS, which can mediate resistance to the last line therapies colistin and tigecycline, respectively, as well as transporters, surface structures, and iron acquisition genes.

CONCLUSIONS

Most SNVs and IS events were isolate-specific indicating these mutations did not become fixed on the time scale investigated, yet over-representation of independent mutations in some genes or functional categories suggests that they are under selective pressure. Genome analysis at the population-level suggests that gene transfer including recombination also contributes to Ab evolutionary dynamics. These findings provide important insight into the transmission dynamics of Ab and the identification of patients with repeat infections has implications for infection control programs targeted to this pathogen.

摘要

背景

对于感染多重耐药(MDR)或泛耐药(PDR)细菌病原体的患者,可用的治疗选择有限,导致感染可能持续数周或数月。为了更好地了解长期感染期间MDR鲍曼不动杆菌(Ab)的传播和进化动态,我们在菌株特异性、患者特异性和群体水平上分析了来自个体患者的一系列菌株的基因组。

方法

对40名患者的纵向菌株(每位患者2 - 10株,时间跨度为0 - 829天)进行全基因组分析,包括单核苷酸变异(SNV)检测、插入序列(IS)定位和基因内容变化分析。

结果

系统发育分析表明,相当一部分看似持续的感染实际上是由于新菌株的再次感染。SNV主要导致蛋白质编码变化,而IS事件主要中断基因或处于使相邻基因过度表达的方向。感染期间获得的突变在转录调节因子中过度富集,特别是pmrAB和adeRS,它们分别可以介导对最后一线治疗药物黏菌素和替加环素的耐药性,以及转运蛋白、表面结构和铁摄取基因。

结论

大多数SNV和IS事件是菌株特异性的,表明这些突变在所研究的时间尺度上没有固定下来,但某些基因或功能类别中独立突变的过度富集表明它们处于选择压力之下。群体水平的基因组分析表明,包括重组在内的基因转移也有助于Ab的进化动态。这些发现为Ab的传播动态提供了重要见解,识别重复感染患者对针对该病原体的感染控制计划具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2c93/4776386/893a44a70678/13073_2016_279_Fig1_HTML.jpg

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