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对 16 株碳青霉烯酶产生临床株基因组中 40 个前噬菌体的基因组分析。

Genomic analysis of 40 prophages located in the genomes of 16 carbapenemase-producing clinical strains of .

机构信息

Microbiology Department, Research Institute Biomedical A Coruña (INIBIC), Hospital A Coruña (CHUAC), University of A Coruña (UDC), A Coruña, Spain.

Study Group on Mechanisms of Action and Resistance to Antimicrobials (GEMARA), Spanish Society of Infectious Diseases and Clinical Microbiology (SEIMC), Madrid.

出版信息

Microb Genom. 2020 May;6(5). doi: 10.1099/mgen.0.000369. Epub 2020 Apr 29.

Abstract

is the clinically most important species within the genus and, as a result of the continuous emergence of multi-drug resistant (MDR) strains, the cause of severe nosocomial infections. The decline in the effectiveness of antibiotic treatments for infections caused by MDR bacteria has generated particular interest in the study of bacteriophages. In this study, we characterized a total of 40 temperate bacteriophages (prophages) with a genome range of 11.454-84.199 kb, predicted from 16 carbapenemase-producing clinical strains of belonging to different sequence types, previously identified by multilocus sequence typing. These prophages were grouped into the three families in the order (27 prophages belonging to the family , 10 prophages belonging to the family and 3 prophages belonging to the family ). Genomic comparison of the 40 prophage genomes led to the identification of four prophages isolated from different strains and of genome sizes of around 33.3, 36.1, 39.6 and 42.6 kb. These prophages showed sequence similarities (query cover >90 %, identity >99.9 %) with international Microbe Versus Phage (MVP) (http://mvp.medgenius.info/home) clusters 4762, 4901, 3499 and 4280, respectively. Phylogenetic analysis revealed the evolutionary proximity among the members of the four groups of the most frequently identified prophages in the bacterial genomes studied (33.3, 36.1, 39.6 and 42.6 kb), with bootstrap values of 100 %. This allowed the prophages to be classified into three clusters: A, B and C. Interestingly, these temperate bacteriophages did not infect the highest number of strains as indicated by a host-range assay, these results could be explained by the development of superinfection exclusion mechanisms. In addition, bioinformatic analysis of the 40 identified prophages revealed the presence of 2363 proteins. In total, 59.7 % of the proteins identified had a predicted function, mainly involving viral structure, transcription, replication and regulation (lysogenic/lysis). Interestingly, some proteins had putative functions associated with bacterial virulence (toxin expression and efflux pump regulators), phage defence profiles such as toxin-antitoxin modules, an anti-CRISPR/Cas9 protein, TerB protein (from ter operon) and methyltransferase proteins.

摘要

是属中临床最重要的物种,由于多药耐药(MDR)菌株的不断出现,它是严重医院感染的原因。针对 MDR 细菌感染的抗生素治疗效果下降,促使人们对噬菌体产生了特别的兴趣。在这项研究中,我们对 16 株不同序列型的产碳青霉烯酶临床分离株进行了多基因序列分型,这些分离株来自不同的序列型,共鉴定出 40 个温和噬菌体(原噬菌体),其基因组范围为 11.454-84.199kb。这些原噬菌体分为三个科,分别为 科(27 个原噬菌体属于科,10 个原噬菌体属于科,3 个原噬菌体属于科)。对 40 个原噬菌体基因组的比较分析,鉴定出了来自不同菌株的 4 个原噬菌体,其基因组大小分别约为 33.3、36.1、39.6 和 42.6kb。这些原噬菌体与国际微生物与噬菌体(MVP)(http://mvp.medgenius.info/home)聚类 4762、4901、3499 和 4280 的序列相似性(查询覆盖率>90%,同一性>99.9%)。系统发育分析显示,在所研究的细菌基因组中,最常鉴定到的 4 组原噬菌体成员之间具有进化上的亲缘关系(33.3、36.1、39.6 和 42.6kb),其自举值为 100%。这使得这些温和噬菌体能够被分类为三个聚类:A、B 和 C。有趣的是,这些温和噬菌体的宿主范围试验表明,它们并没有感染最多数量的菌株,这些结果可以用超级感染排除机制来解释。此外,对鉴定出的 40 个原噬菌体的生物信息学分析表明,它们存在 2363 个蛋白。总的来说,鉴定到的蛋白中有 59.7%具有预测功能,主要涉及病毒结构、转录、复制和调控(溶原/裂解)。有趣的是,一些蛋白具有与细菌毒力相关的假定功能(毒素表达和外排泵调节剂)、噬菌体防御谱,如毒素-抗毒素模块、抗 CRISPR/Cas9 蛋白、TerB 蛋白(来自 ter 操纵子)和甲基转移酶蛋白。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/90db/7371120/be29110a551e/mgen-6-369-g001.jpg

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