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生殖支原体中mgpB基因的菌株内异质性在体外和体内都很广泛,这表明变异是通过与重复染色体序列的重组产生的。

Intrastrain heterogeneity of the mgpB gene in Mycoplasma genitalium is extensive in vitro and in vivo and suggests that variation is generated via recombination with repetitive chromosomal sequences.

作者信息

Iverson-Cabral Stefanie L, Astete Sabina G, Cohen Craig R, Rocha Eduardo P C, Totten Patricia A

机构信息

Department of Medicine, Harborview Medical Center, R&T Building, 325 9th Avenue, Box 359779, Seattle, WA 98104, USA.

出版信息

Infect Immun. 2006 Jul;74(7):3715-26. doi: 10.1128/IAI.00239-06.

DOI:10.1128/IAI.00239-06
PMID:16790744
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1489687/
Abstract

Mycoplasma genitalium is associated with reproductive tract disease in women and may persist in the lower genital tract for months, potentially increasing the risk of upper tract infection and transmission to uninfected partners. Despite its exceptionally small genome (580 kb), approximately 4% is composed of repeated elements known as MgPar sequences (MgPa repeats) based on their homology to the mgpB gene that encodes the immunodominant MgPa adhesin protein. The presence of these MgPar sequences, as well as mgpB variability between M. genitalium strains, suggests that mgpB and MgPar sequences recombine to produce variant MgPa proteins. To examine the extent and generation of diversity within single strains of the organism, we examined mgpB variation within M. genitalium strain G-37 and observed sequence heterogeneity that could be explained by recombination between the mgpB expression site and putative donor MgPar sequences. Similarly, we analyzed mgpB sequences from cervical specimens from a persistently infected woman (21 months) and identified 17 different mgpB variants within a single infecting M. genitalium strain, confirming that mgpB heterogeneity occurs over the course of a natural infection. These observations support the hypothesis that recombination occurs between the mgpB gene and MgPar sequences and that the resulting antigenically distinct MgPa variants may contribute to immune evasion and persistence of infection.

摘要

生殖支原体与女性生殖道疾病相关,可能在女性下生殖道持续存在数月,这有可能增加上生殖道感染以及传播给未感染伴侣的风险。尽管其基因组异常小(580 kb),但约4%由重复元件组成,这些重复元件基于与编码免疫显性MgPa黏附蛋白的mgpB基因的同源性,被称为MgPar序列(MgPa重复序列)。这些MgPar序列的存在,以及生殖支原体菌株之间mgpB的变异性,表明mgpB和MgPar序列会重组以产生变异的MgPa蛋白。为了研究该生物体单一菌株内多样性的程度和产生方式,我们检测了生殖支原体G - 37菌株内mgpB的变异情况,并观察到序列异质性,这可以通过mgpB表达位点与假定的供体MgPar序列之间的重组来解释。同样,我们分析了一名持续感染女性(21个月)宫颈标本中的mgpB序列,在单一感染的生殖支原体菌株中鉴定出17种不同的mgpB变体,证实了mgpB异质性在自然感染过程中会出现。这些观察结果支持了这样的假设,即mgpB基因与MgPar序列之间会发生重组,并且由此产生的抗原性不同的MgPa变体可能有助于免疫逃逸和感染的持续存在。

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Intrastrain heterogeneity of the mgpB gene in Mycoplasma genitalium is extensive in vitro and in vivo and suggests that variation is generated via recombination with repetitive chromosomal sequences.生殖支原体中mgpB基因的菌株内异质性在体外和体内都很广泛,这表明变异是通过与重复染色体序列的重组产生的。
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Sequence-based typing of Mycoplasma genitalium reveals sexual transmission.基于序列的生殖支原体分型揭示了性传播。
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Comparative and evolutionary analysis of the bacterial homologous recombination systems.细菌同源重组系统的比较与进化分析
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