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噬菌体Mu基因B突变体介导的异常共整合结构:它们与基因功能的关系。

Abnormal cointegrate structures mediated by gene B mutants of phage Mu: their implications with regard to gene function.

作者信息

Coelho A, Maynard-Smith S, Symonds N

出版信息

Mol Gen Genet. 1982;185(2):356-62. doi: 10.1007/BF00330812.

Abstract

A system where the transposition of MupApl (a derivative of phage Mu carrying a determinant coding for ampicillin resistance) is followed from the small plasmid pML2 into the conjugative plasmid R388 has been used to investigate the influence on Mu transposition of B, an early Mu gene which is involved in normal phage DNA synthesis. In the absence of active B protein a low level (about 1% of normal) of transposition was detected. Roughly a third of these transpositional events was found to lead to the formation of cointegrate DNA structures which were shown to consist of R388, two complete copies of Mu and part only of pML2. The pML2 deletions vary in size but all those investigated appear to originate at an end of Mu. An explanation of these observations is proposed which envisages the B protein as part of the normal transposition complex.

摘要

已使用一种系统来研究早期 Mu 基因 B(参与正常噬菌体 DNA 合成)对 Mu 转座的影响,该系统中 MupApl(携带氨苄青霉素抗性编码决定簇的噬菌体 Mu 的衍生物)从小质粒 pML2 转座到接合质粒 R388 中。在没有活性 B 蛋白的情况下,检测到低水平(约为正常水平的 1%)的转座。发现大约三分之一的这些转座事件会导致共整合 DNA 结构的形成,这些结构显示由 R388、两个完整的 Mu 拷贝和仅部分 pML2 组成。pML2 的缺失大小各异,但所有研究的缺失似乎都起源于 Mu 的一端。提出了对这些观察结果的一种解释,该解释设想 B 蛋白是正常转座复合体的一部分。

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