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将质粒携带的tuf突变转移至染色体作为研究大肠杆菌细胞中EF-TuA和EF-TuB功能的遗传工具。

Transfer of plasmid-borne tuf mutations to the chromosome as a genetic tool for studying the functioning of EF-TuA and EF-TuB in the E. coli cell.

作者信息

Vijgenboom E, Bosch L

机构信息

Department of Biochemistry, Leiden University, The Netherlands.

出版信息

Biochimie. 1987 Oct;69(10):1021-30. doi: 10.1016/0300-9084(87)90002-2.

Abstract

The elongation factor EF-Tu of E. coli is a multifunctional protein that lends itself extremely well to studies concerning structure-function relationships. It is encoded by two genes: tufA and tufB. Mutant species of EF-Tu have been obtained by various genetic manipulations, including site- and segment-directed mutagenesis of tuf genes on a vector. The presence of multiple tuf genes in the cell, both chromosomal and plasmid-borne, hampers the characterization of the mutant EF-Tu. We describe a procedure for transferring plasmid-borne tuf gene mutations to the chromosome. Any mutation engineered by genetic manipulation of tuf genes on a vector can be transferred both to the tufA and the tufB position on the chromosome. The procedure facilitated the functional characterization of some of our recently obtained tuf mutations. Of particular relevance is, that it enabled us for the first time to obtain a mutant tufB on the chromosome, encoding an EF-TuB resistant to kirromycin. It thus became possible to study the consequences for growth of tufA inactivation by insertion of bacteriophage Mu. The preliminary evidence obtained suggests that an EF-TuA, active in polypeptide synthesis, is essential for growth whereas such an EF-TuB is dispensable.

摘要

大肠杆菌的延伸因子EF-Tu是一种多功能蛋白质,非常适合用于有关结构-功能关系的研究。它由两个基因编码:tufA和tufB。通过各种基因操作已获得EF-Tu的突变体,包括对载体上tuf基因进行位点和片段定向诱变。细胞中存在多个tuf基因,包括染色体上的和质粒携带的,这妨碍了突变型EF-Tu的表征。我们描述了一种将质粒携带的tuf基因突变转移到染色体上的方法。通过对载体上tuf基因进行基因操作设计的任何突变都可以转移到染色体上的tufA和tufB位置。该方法有助于对我们最近获得的一些tuf突变进行功能表征。特别相关的是,它使我们首次在染色体上获得了一个tufB突变体,其编码对奇霉素耐药的EF-TuB。因此,通过插入噬菌体Mu来研究tufA失活对生长的影响成为可能。获得的初步证据表明,在多肽合成中起作用的EF-TuA对生长至关重要,而这种EF-TuB则是可有可无的。

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