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ISPa20通过插入诱变和基因组重排促进了从囊性纤维化患者中分离出的铜绿假单胞菌克隆C亚克隆C13菌株的个体进化。

ISPa20 advances the individual evolution of Pseudomonas aeruginosa clone C subclone C13 strains isolated from cystic fibrosis patients by insertional mutagenesis and genomic rearrangements.

作者信息

Kresse Andreas U, Blöcker Helmut, Römling Ute

机构信息

Research Group Clonal Variability, Division of Cell- and Immune Biology, GBF - German Research Centre for Biotechnology, Mascheroder Weg 1, 38124, Braunschweig, Germany.

出版信息

Arch Microbiol. 2006 May;185(4):245-54. doi: 10.1007/s00203-006-0089-5. Epub 2006 Feb 11.

Abstract

Pseudomonas aeruginosa clone C strains, which chronically colonize the lungs of cystic fibrosis patients reorganize their genome structure. In this study, a novel member of the IS3 subfamily of IS elements, ISPa20, was detected which was specific for clone C subclone C13 strains. ISPa20, which was present in high copy number, mediated events of genomic reorganization. ISPa20 was inserted into P. aeruginosa backbone genes leading to adaptation to the cystic fibrosis lung habitat and into DNA acquired through horizontal gene transfer. Further on, large chromosomal inversions were mediated by ISPa20. In contrast to strains of other subclonal linages high rates of genomic rearrangements of subclone C13 strains were observed in vitro. The acquisition of mobile elements by P. aeruginosa clone C strains in the lungs of cystic fibrosis patients supports the chronic colonization by insertional mutagenesis and chromosome restructuring leading to microevolution within clone C that reflects macroevolution observed on the species level.

摘要

长期定植于囊性纤维化患者肺部的铜绿假单胞菌克隆C菌株会重组其基因组结构。在本研究中,检测到一种IS元件IS3亚家族的新成员ISPa20,它对克隆C亚克隆C13菌株具有特异性。高拷贝数存在的ISPa20介导了基因组重组事件。ISPa20插入到铜绿假单胞菌的主干基因中,导致其适应囊性纤维化肺部环境,并插入到通过水平基因转移获得的DNA中。此外,ISPa20介导了大型染色体倒位。与其他亚克隆谱系的菌株相比,在体外观察到亚克隆C13菌株的基因组重排率很高。囊性纤维化患者肺部的铜绿假单胞菌克隆C菌株获得移动元件,通过插入诱变和染色体重组支持了慢性定植,导致克隆C内的微进化,这反映了在物种水平上观察到的宏观进化。

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