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葡萄球菌噬菌体和葡萄球菌致病岛整合酶在种内和种间葡萄球菌致病岛转移中的作用。

Role of staphylococcal phage and SaPI integrase in intra- and interspecies SaPI transfer.

作者信息

Maiques Elisa, Ubeda Carles, Tormo María Angeles, Ferrer María Desamparados, Lasa Iñigo, Novick Richard P, Penadés José R

机构信息

Centro de Investigación y Tecnología Animal, Instituto Valenciano de Investigaciones Agrarias, Apdo. 187, 12.400 Segorbe, Castellón, Spain.

出版信息

J Bacteriol. 2007 Aug;189(15):5608-16. doi: 10.1128/JB.00619-07. Epub 2007 Jun 1.

Abstract

SaPIbov2 is a member of the SaPI family of staphylococcal pathogenicity islands and is very closely related to SaPIbov1. Typically, certain temperate phages can induce excision and replication of one or more of these islands and can package them into special small phage-like particles commensurate with their genome sizes (referred to as the excision-replication-packaging [ERP] cycle). We have studied the phage-SaPI interaction in some depth using SaPIbov2, with special reference to the role of its integrase. We demonstrate here that SaPIbov2 can be induced to replicate by different staphylococcal phages. After replication, SaPIbov2 is efficiently encapsidated and transferred to recipient organisms, including different non-Staphylococcus aureus staphylococci, where it integrates at a SaPI-specific attachment site, att(C), by means of a self-coded integrase (Int). Phages that cannot induce the SaPIbov2 ERP cycle can transfer the island by recA-dependent classical generalized transduction and can also transfer it by a novel mechanism that requires the expression of SaPIbov2 int in the recipient but not in the donor. It is suggested that this mechanism involves the encapsidation of standard transducing fragments containing the intact island followed by int-mediated excision, circularization, and integration in the recipient.

摘要

SaPIbov2是葡萄球菌致病岛SaPI家族的成员,与SaPIbov1密切相关。通常,某些温和噬菌体可诱导这些岛中的一个或多个进行切除和复制,并能将它们包装成与其基因组大小相称的特殊小噬菌体样颗粒(称为切除-复制-包装[ERP]循环)。我们利用SaPIbov2对噬菌体与SaPI的相互作用进行了较为深入的研究,特别关注了其整合酶的作用。我们在此证明,不同的葡萄球菌噬菌体可诱导SaPIbov2进行复制。复制后,SaPIbov2被高效包装并转移至受体菌,包括不同的非金黄色葡萄球菌葡萄球菌,在那里它通过自身编码的整合酶(Int)整合到一个SaPI特异性附着位点att(C)。不能诱导SaPIbov2 ERP循环的噬菌体可通过recA依赖的经典广义转导转移该岛,也可通过一种新机制转移,该机制要求在受体菌而非供体菌中表达SaPIbov2 int。有人认为,这种机制涉及包含完整岛的标准转导片段的包装,随后通过int介导在受体菌中进行切除、环化和整合。

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