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噬菌体T4感染期间质粒的重组依赖性复制。

Recombination-dependent replication of plasmids during bacteriophage T4 infection.

作者信息

Kreuzer K N, Yap W Y, Menkens A E, Engman H W

机构信息

Department of Microbiology and Immunology, Duke University Medical Center, Durham, North Carolina 27710.

出版信息

J Biol Chem. 1988 Aug 15;263(23):11366-73.

PMID:3403532
Abstract

The replication of plasmids containing fragments of the T4 genome, but no phage replication origins, was analyzed as a possible model for phage secondary (recombination-dependent) replication initiation. The replication of such plasmids after T4 infection was reduced or eliminated by mutations in several phage genes (uvsY, uvsX, 46, 59, 39, and 52) that have previously been shown to be involved in secondary initiation. A series of plasmids that collectively contain about 60 kilobase pairs of the T4 genome were tested for replication after T4 infection. With the exception of those known to contain tertiary origins, every plasmid replicated in a uvsY-dependent fashion. Thus, there is no apparent requirement for an extensive nucleotide sequence in the uvsY-dependent plasmid replication. However, homology with the phage genome is required since the plasmid vector alone did not replicate after phage infection. The products of plasmid replication included long concatemeric molecules with as many as 35 tandem copies of plasmid sequence. The production of concatemers indicates that plasmid replication is an active process and not simply the result of passive replication after the integration of plasmids into the phage genome. We conclude that plasmids with homology to the T4 genome utilize the secondary initiation mechanism of the phage. This simple model system should be useful in elucidating the molecular mechanism of recombination-dependent DNA synthesis in phage T4.

摘要

分析了含有T4基因组片段但无噬菌体复制起点的质粒复制情况,将其作为噬菌体二级(依赖重组)复制起始的一种可能模型。T4感染后,此类质粒的复制因几个先前已证明参与二级起始的噬菌体基因(uvsY、uvsX、46、59、39和52)发生突变而减少或消除。检测了一系列总共包含约60千碱基对T4基因组的质粒在T4感染后的复制情况。除了那些已知含有三级起点的质粒外,每个质粒都以依赖uvsY的方式进行复制。因此,在依赖uvsY的质粒复制中,对广泛的核苷酸序列没有明显要求。然而,由于仅质粒载体在噬菌体感染后不复制,所以与噬菌体基因组的同源性是必需的。质粒复制产物包括长达35个串联质粒序列拷贝的长串联体分子。串联体的产生表明质粒复制是一个活跃过程,而不仅仅是质粒整合到噬菌体基因组后被动复制的结果。我们得出结论,与T4基因组具有同源性的质粒利用了噬菌体的二级起始机制。这个简单的模型系统应有助于阐明噬菌体T4中依赖重组的DNA合成的分子机制。

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