首页> 美国卫生研究院文献>PLoS Genetics >Replication and Active Partition of Integrative and Conjugative Elements (ICEs) of the SXT/R391 Family: The Line between ICEs and Conjugative Plasmids Is Getting Thinner
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Replication and Active Partition of Integrative and Conjugative Elements (ICEs) of the SXT/R391 Family: The Line between ICEs and Conjugative Plasmids Is Getting Thinner

机译:SXT / R391家族的整合和结合元件(ICE)的复制和活性分配:ICE和结合质粒之间的界线越来越细

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摘要

Integrative and Conjugative Elements (ICEs) of the SXT/R391 family disseminate multidrug resistance among pathogenic Gammaproteobacteria such as Vibrio cholerae. SXT/R391 ICEs are mobile genetic elements that reside in the chromosome of their host and eventually self-transfer to other bacteria by conjugation. Conjugative transfer of SXT/R391 ICEs involves a transient extrachromosomal circular plasmid-like form that is thought to be the substrate for single-stranded DNA translocation to the recipient cell through the mating pore. This plasmid-like form is thought to be non-replicative and is consequently expected to be highly unstable. We report here that the ICE R391 of Providencia rettgeri is impervious to loss upon cell division. We have investigated the genetic determinants contributing to R391 stability. First, we found that a hipAB-like toxin/antitoxin system improves R391 stability as its deletion resulted in a tenfold increase of R391 loss. Because hipAB is not a conserved feature of SXT/R391 ICEs, we sought for alternative and conserved stabilization mechanisms. We found that conjugation itself does not stabilize R391 as deletion of traG, which abolishes conjugative transfer, did not influence the frequency of loss. However, deletion of either the relaxase-encoding gene traI or the origin of transfer (oriT) led to a dramatic increase of R391 loss correlated with a copy number decrease of its plasmid-like form. This observation suggests that replication initiated at oriT by TraI is essential not only for conjugative transfer but also for stabilization of SXT/R391 ICEs. Finally, we uncovered srpMRC, a conserved locus coding for two proteins distantly related to the type II (actin-type ATPase) parMRC partitioning system of plasmid R1. R391 and plasmid stabilization assays demonstrate that srpMRC is active and contributes to reducing R391 loss. While partitioning systems usually stabilizes low-copy plasmids, srpMRC is the first to be reported that stabilizes a family of ICEs.
机译:SXT / R391家族的整合和共轭元件(ICEs)在诸如霍乱弧菌的致病性丙型变形杆菌中传播了多重耐药性。 SXT / R391 ICEs是可移动的遗传元件,驻留在其宿主的染色体中,并最终通过结合而自我转移至其他细菌。 SXT / R391 ICE的共轭转移涉及一种瞬时染色体外环状质粒样形式,该形式被认为是单链DNA通过交配孔易位至受体细胞的底物。这种质粒样形式被认为是非复制性的,因此被认为是高度不稳定的。我们在这里报告瑞氏普罗维登斯的ICE R391不会因细胞分裂而损失。我们已经调查了有助于R391稳定性的遗传决定因素。首先,我们发现类hipAB样毒素/抗毒素系统改善了R391的稳定性,因为其缺失导致R391损失增加了十倍。由于hipAB不是SXT / R391 ICE的保守特征,因此我们寻求替代和保守的稳定机制。我们发现,共轭本身不能稳定R391,因为traG的缺失(消除了共轭转移)不影响丢失的频率。然而,编码松弛酶的基因traI或转移起点(oriT)的缺失导致R391缺失的急剧增加,与其质粒样形式的拷贝数减少相关。该观察结果表明,由TraI在oriT处启动的复制不仅对于共轭转移至关重要,而且对于SXT / R391 ICE的稳定也是必不可少的。最后,我们发现了srpMRC,这是一个保守的基因座,编码两个与质粒R1的II型(肌动蛋白型ATPase)parMRC分配系统远距离相关的蛋白质。 R391和质粒稳定化验表明srpMRC是有活性的,有助于减少R391的损失。尽管分配系统通常可稳定低拷贝质粒,但srpMRC是第一个可稳定ICE家族的文献。

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