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一种保守的最小核糖核酸酶E肽保留了核心催化功能,该肽缺乏形成四聚体所需的结构域。

Retention of core catalytic functions by a conserved minimal ribonuclease E peptide that lacks the domain required for tetramer formation.

作者信息

Caruthers Jonathan M, Feng Yanan, McKay David B, Cohen Stanley N

机构信息

Department of Structural Biology, Stanford University School of Medicine, Stanford, California 94305, USA.

出版信息

J Biol Chem. 2006 Sep 15;281(37):27046-51. doi: 10.1074/jbc.M602467200. Epub 2006 Jul 19.

Abstract

Ribonuclease E (RNase E) is a multifunctional endoribonuclease that has been evolutionarily conserved in both Gram-positive and Gram-negative bacteria. X-ray crystallography and biochemical studies have concluded that the Escherichia coli RNase E protein functions as a homotetramer formed by Zn linkage of dimers within a region extending from amino acid residues 416 through 529 of the 116-kDa protein. Using fragments of RNase E proteins from E. coli and Haemophilus influenzae, we show here that RNase E derivatives that are as short as 395 amino acid residues and that lack the Zn-link region shown previously to be essential for tetramer formation (i.e. amino acid residues 400-415) are catalytically active enzymes that retain the 5' to 3' scanning ability and cleavage site specificity characteristic of full-length RNase E and that also confer colony forming ability on rne null mutant bacteria. Further truncation leads to loss of these properties. Our results, which identify a minimal catalytically active RNase E sequence, indicate that contrary to current models, a tetrameric quaternary structure is not required for RNase E to carry out its core enzymatic functions.

摘要

核糖核酸酶E(RNase E)是一种多功能内切核糖核酸酶,在革兰氏阳性菌和革兰氏阴性菌中都具有进化保守性。X射线晶体学和生化研究得出结论,大肠杆菌RNase E蛋白作为一种同四聚体发挥作用,该四聚体由116 kDa蛋白中从氨基酸残基416到529的区域内的二聚体通过锌连接形成。我们利用来自大肠杆菌和流感嗜血杆菌的RNase E蛋白片段在此表明,长度仅为395个氨基酸残基且缺乏先前显示对四聚体形成至关重要的锌连接区域(即氨基酸残基400 - 415)的RNase E衍生物是具有催化活性的酶,它们保留了全长RNase E特有的5'到3'扫描能力和切割位点特异性,并且还赋予rne基因缺失突变细菌形成菌落的能力。进一步截短会导致这些特性丧失。我们的结果确定了一个最小的具有催化活性的RNase E序列,表明与当前模型相反,RNase E执行其核心酶功能并不需要四聚体四级结构。

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