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使用染色体整合子阵列作为霍乱弧菌大流行菌株的系统发育分型系统。

Use of chromosomal integron arrays as a phylogenetic typing system for Vibrio cholerae pandemic strains.

作者信息

Labbate M, Boucher Y, Joss M J, Michael C A, Gillings M R, Stokes H W

机构信息

Department of Chemistry and Biomolecular Sciences, Macquarie University, Sydney, Australia.

Department of Biological Sciences, Macquarie University, Sydney, Australia.

出版信息

Microbiology (Reading). 2007 May;153(Pt 5):1488-1498. doi: 10.1099/mic.0.2006/001065-0.

Abstract

Approximately 200 serogroups of Vibrio cholerae exist, with only two, O1 and O139, responsible for epidemic and pandemic cholera. Strains from these serogroups have evolved from a common progenitor, with lateral gene transfer largely driving their emergence. These strains are so closely related that separation using single- or multi-locus phylogeny has proven difficult. V. cholerae strains contain a genetic system called the integron that is located in the chromosome and that can integrate and excise DNA elements called mobile gene cassettes (MGCs) by site-specific recombination. Large arrays of MGCs are found in V. cholerae strains. For instance, the O1 El Tor strain N16961 contains 179 MGCs. Since integron arrays are dynamic through recombination and excision of MGCs, it was hypothesized that the MGC composition in a given V. cholerae pandemic strain would be useful as a phylogenetic typing system. To address this, a PCR-based method was used to rapidly characterize the MGC composition of V. cholerae arrays. The results showed that the MGC composition of pandemic V. cholerae cassette arrays is relatively conserved, providing further evidence that these strains have evolved from a common progenitor. Comparison of MGC composition between the V. cholerae pandemic strains was also able to resolve the evolution of O139 from a subgroup of O1 El Tor. This level of differentiation of closely related V. cholerae isolates was more sensitive than conventional single-gene phylogeny or multi-locus sequence analysis. Using this method, novel MGCs from an O1 classical strain and an Argentinian O139 isolate were also identified, and a major deletion in the MGC array in all pandemic O139 strains and a subset of O1 El Tor strains was identified. Analysis of sequenced V. cholerae integron arrays showed that their evolution can proceed by rearrangements and deletions/insertions of large portions of MGCs in addition to the insertion or excision of single MGCs.

摘要

霍乱弧菌大约有200个血清群,其中只有O1和O139这两个血清群会引发霍乱的流行和大流行。这些血清群的菌株由一个共同的祖先演化而来,横向基因转移在很大程度上推动了它们的出现。这些菌株关系非常密切,事实证明,使用单基因座或多基因座系统发育分析法进行区分很困难。霍乱弧菌菌株含有一个位于染色体上的称为整合子的遗传系统,该系统可以通过位点特异性重组整合和切除称为移动基因盒(MGC)的DNA元件。在霍乱弧菌菌株中发现了大量的MGC。例如,O1埃尔托生物型菌株N16961含有179个MGC。由于整合子阵列通过MGC的重组和切除而具有动态性,因此有人推测,特定霍乱弧菌大流行菌株中的MGC组成可作为一种系统发育分型系统。为了解决这个问题,采用了一种基于聚合酶链反应的方法来快速表征霍乱弧菌阵列的MGC组成。结果表明,霍乱弧菌大流行菌株盒式阵列的MGC组成相对保守,这进一步证明了这些菌株是由一个共同的祖先演化而来的。比较霍乱弧菌大流行菌株之间的MGC组成,还能够解析出O139是从O1埃尔托生物型的一个亚群演化而来的。这种对密切相关的霍乱弧菌分离株的区分水平比传统的单基因系统发育或多基因座序列分析更敏感。使用这种方法,还鉴定出了来自一个O1古典生物型菌株和一个阿根廷O139分离株的新型MGC,并在所有大流行的O139菌株和一部分O1埃尔托生物型菌株的MGC阵列中发现了一个主要缺失。对已测序的霍乱弧菌整合子阵列的分析表明,除了单个MGC的插入或切除外,它们的进化还可以通过MGC大部分的重排和缺失/插入来进行。

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