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一个通过特异性靶向基因盒重组位点影响整合子的插入序列家族,即IS1111-attC组。

A family of insertion sequences that impacts integrons by specific targeting of gene cassette recombination sites, the IS1111-attC Group.

作者信息

Tetu Sasha G, Holmes Andrew J

机构信息

School of Molecular and Microbial Biosciences, University of Sydney, Sydney, New South Wales, Australia.

出版信息

J Bacteriol. 2008 Jul;190(14):4959-70. doi: 10.1128/JB.00229-08. Epub 2008 May 16.

Abstract

Integrons facilitate the evolution of complex phenotypes by physical and transcriptional linkage of genes. They can be categorized as chromosomal integrons (CIs) or mobile resistance integrons (MRIs). The significance of MRIs for the problem of multiple antibiotic resistance is well established. CIs are more widespread, but their only demonstrated significance is as a reservoir of gene cassettes for MRIs. In characterizing CIs associated with Pseudomonas, we discovered a subfamily of insertion sequences, termed the IS1111-attC group, that insert into the recombination sites of gene cassettes (attC site) by site-specific recombination. IS1111-attC elements appear to have recently spread from Pseudomonas species to clinical class 1 integrons. Such elements are expected to significantly impact integrons. To explore this further, we examined CIs in 24 strains representing multiple levels of evolutionary divergence within the genus Pseudomonas. Cassette arrays frequently had a degenerated "footprint" of an IS1111-attC group element at their terminus and in three cases were occupied by multiple functional IS1111-attC elements. Within Pseudomonas spp. the IS-integron interaction appears to follow an evolutionarily rapid cycle of infection, expansion, and extinction. The final outcome is extinction of the IS element and modification of the right-hand boundary of the integron. This system represents an unusual example of convergent evolution whereby heterologous families of site-specific recombinases of distinct genetic elements have adopted the same target site. The interactions described here represent a model for evolutionary processes that offer insights to a number of aspects of the biology of integrons and other mosaic genetic elements.

摘要

整合子通过基因的物理连接和转录连接促进复杂表型的进化。它们可分为染色体整合子(CIs)或移动抗性整合子(MRIs)。MRIs对多重抗生素耐药性问题的重要性已得到充分证实。CIs更为普遍,但它们唯一已证实的重要性是作为MRIs基因盒的储存库。在对与假单胞菌相关的CIs进行特征描述时,我们发现了一个插入序列亚家族,称为IS1111-attC组,它通过位点特异性重组插入基因盒的重组位点(attC位点)。IS1111-attC元件似乎最近从假单胞菌属物种传播到临床1类整合子。预计此类元件会对整合子产生重大影响。为进一步探究这一点,我们检查了代表假单胞菌属内多个进化分歧水平的24株菌株中的CIs。基因盒阵列在其末端经常有一个退化的IS1111-attC组元件“足迹”,在三个案例中被多个功能性IS1111-attC元件占据。在假单胞菌属内,IS-整合子相互作用似乎遵循一个感染、扩展和灭绝的进化快速循环。最终结果是IS元件灭绝和整合子右手边界的改变。这个系统代表了趋同进化的一个不寻常例子,即不同遗传元件的位点特异性重组酶异源家族采用了相同的靶位点。这里描述的相互作用代表了一个进化过程模型,为整合子和其他镶嵌遗传元件生物学的多个方面提供了见解。

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