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大肠杆菌致病分离株特有的染色体区域具有系统发育聚类分布。

Chromosomal regions specific to pathogenic isolates of Escherichia coli have a phylogenetically clustered distribution.

作者信息

Boyd E F, Hartl D L

机构信息

Department of Organismic and Evolutionary Biology, Harvard University, Cambridge, Massachusetts 02138, USA.

出版信息

J Bacteriol. 1998 Mar;180(5):1159-65. doi: 10.1128/JB.180.5.1159-1165.1998.

Abstract

We studied the ancestry of virulence-associated genes in Escherichia coli by examining chromosomal regions specific to pathogenic isolates. The four virulence determinants examined were the alpha-hemolysin (hly) loci hlyI and hlyII, the type II capsule gene cluster kps, and the P (pap) and S (sfa) fimbria gene clusters. All four loci were shown previously to be associated with pathogenicity islands of uropathogenic E. coli isolates. The hly, kps, sfa, and pap regions each have an unexpected clustered distribution among the E. coli collection of reference (ECOR) strains, but all these regions were absent from a collection of diarrheagenic E. coli isolates. Strains in the ECOR subgroup B2 typically had a combination of at least three of the four loci, and all strains in subgroup D had a copy of the kps and pap clusters. In contrast, only four strains in subgroup A had either hly, kps, sfa, or pap, and no subgroup A strains had all four together. Strains of subgroup B1 were devoid of all four virulence regions, with the exception of one isolate that had a copy of the sfa gene cluster. This phylogenetic distribution of strain-specific sequences corresponds to the ECOR groups with the largest genome size, namely, B2 and D. We propose that the pathogenicity islands are ancestral to subgroups B2 and D and were acquired after speciation, with subsequent horizontal transfer into some group A, B1, and E lineages. These results suggest that the hly, kps, sfa, and pap pathogenicity determinants may play a role in the evolution of enteric bacteria quite apart from, and perhaps with precedence over, their ability to cause disease.

摘要

我们通过检查致病分离株特有的染色体区域,研究了大肠杆菌中与毒力相关基因的起源。所检测的四个毒力决定因素是α-溶血素(hly)基因座hlyI和hlyII、II型荚膜基因簇kps以及P(pap)和S(sfa)菌毛基因簇。先前已证明所有这四个基因座都与尿路致病性大肠杆菌分离株的致病岛相关。hly、kps、sfa和pap区域在大肠杆菌参考(ECOR)菌株集合中各自具有意外的聚集分布,但所有这些区域在一组致泻性大肠杆菌分离株中均不存在。ECOR亚组B2中的菌株通常具有这四个基因座中至少三个的组合,并且亚组D中的所有菌株都有kps和pap簇的一个拷贝。相比之下,亚组A中只有四个菌株具有hly、kps、sfa或pap,并且没有亚组A菌株同时具有所有四个。B1亚组的菌株除了一个具有sfa基因簇拷贝的分离株外,都没有所有四个毒力区域。这种菌株特异性序列的系统发育分布与基因组大小最大的ECOR组,即B2和D相对应。我们提出致病岛是B2和D亚组的祖先,在物种形成后获得,随后水平转移到一些A、B1和E谱系组中。这些结果表明,hly、kps、sfa和pap致病决定因素可能在肠道细菌的进化中发挥作用,这与其致病能力完全不同,甚至可能优先于其致病能力。

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