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由丝氨酸蛋白酶和AAA-ATP酶同源物组成的新型毒素-抗毒素系统决定了致瘤质粒pTiC58的高度稳定性和不相容性。

Novel toxin-antitoxin system composed of serine protease and AAA-ATPase homologues determines the high level of stability and incompatibility of the tumor-inducing plasmid pTiC58.

作者信息

Yamamoto Shinji, Kiyokawa Kazuya, Tanaka Katsuyuki, Moriguchi Kazuki, Suzuki Katsunori

机构信息

Department of Biological Science, Graduate School of Science, Hiroshima University, Higashi Hiroshima, Japan.

出版信息

J Bacteriol. 2009 Jul;191(14):4656-66. doi: 10.1128/JB.00124-09. Epub 2009 May 15.

Abstract

Stability of plant tumor-inducing (Ti) plasmids differs among strains. A high level of stability prevents basic and applied studies including the development of useful strains. The nopaline type Ti plasmid pTiC58 significantly reduces the transconjugant efficiency for incoming incompatible plasmids relative to the other type, such as octopine-type plasmids. In this study we identified a region that increases the incompatibility and stability of the plasmid. This region was located on a 4.3-kbp segment about 38 kbp downstream of the replication locus, repABC. We named two open reading frames in the segment, ietA and ietS, both of which were essential for the high level of incompatibility and stability. Plasmid stabilization by ietAS was accomplished by a toxin-antitoxin (TA) mechanism, where IetS is the toxin and IetA is the antitoxin. A database search revealed that putative IetA and IetS proteins are highly similar to AAA-ATPases and subtilisin-like serine proteases, respectively. Amino acid substitution experiments in each of the highly conserved characteristic residues, in both putative enzymes, suggested that the protease activity is essential and that ATP binding activity is important for the operation of the TA system. The ietAS-containing repABC plasmids expelled Ti plasmids even in strains which were tolerant to conventional Ti-curing treatments.

摘要

植物肿瘤诱导(Ti)质粒的稳定性在不同菌株间存在差异。高水平的稳定性会妨碍包括有用菌株开发在内的基础研究和应用研究。相比于其他类型(如章鱼碱型质粒),胭脂碱型Ti质粒pTiC58显著降低了导入不相容质粒的转接合效率。在本研究中,我们鉴定出了一个能提高质粒不相容性和稳定性的区域。该区域位于复制位点repABC下游约38 kbp处的一个4.3 kbp片段上。我们将该片段中的两个开放阅读框命名为ietA和ietS,它们对于高水平的不相容性和稳定性都是必需的。ietAS介导的质粒稳定作用是通过一种毒素-抗毒素(TA)机制实现的,其中IetS是毒素,IetA是抗毒素。数据库搜索显示,推测的IetA和IetS蛋白分别与AAA-ATP酶和枯草杆菌蛋白酶样丝氨酸蛋白酶高度相似。对这两种推测酶中每个高度保守特征性残基进行的氨基酸取代实验表明,蛋白酶活性是必需的,而ATP结合活性对于TA系统的运作很重要。含有ietAS的repABC质粒即使在对传统Ti消除处理具有耐受性的菌株中也能排出Ti质粒。

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