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Derivatives of ColE1 cer show altered topological specificity in site-specific recombination.

机译:ColE1 cer的衍生物在位点特异性重组中显示出改变的拓扑特异性。

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摘要

ColE1 contains a 250-bp sequence (cer) which is required in cis for the conversion of plasmid dimers to monomers. Recombination between cer and parB (a dimer resolution site from plasmid CloDF13) occurs in vivo at low frequency. The properties of the resulting hybrid sites have been studied. The type I hybrid closely resembles wild-type cer. It supports intramolecular recombination and requires the products of the chromosomal xerA, xerB and xerC genes together with the 250-bp site. In contrast, the type II hybrid (although differing from type I by only 2 bp) functions independently of the topological relationship of the participating sites, supporting both inter- and intramolecular recombination. Furthermore, recombination between type II sites is independent of the products of the xerA and xerB genes and requires a site of less than 50 bp.
机译:ColE1包含一个250 bp的序列(cer),这是顺式将质粒二聚体转化为单体所需的序列。 cer和parB(质粒CloDF13的二聚体解析位点)之间的重组在体内以低频发生。已经研究了所得杂交位点的性质。 I型杂种非常类似于野生型cer。它支持分子内重组,并需要染色体xerA,xerB和xerC基因的产物以及250 bp的位点。相反,II型杂种(尽管与I型杂种仅相差2 bp)的功能独立于参与位点的拓扑关系,从而支持分子间和分子内重组。此外,II型位点之间的重组与xerA和xerB基因的产物无关,并且需要小于50 bp的位点。

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