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核糖核酸酶P——一朵“紫蘩蒌”。 (注:“Scarlet Pimpernel”直译为“紫蘩蒌”,这里可能是将RNase P比喻成紫蘩蒌这种植物,结合语境看可能是取其某种特性来形容核糖核酸酶P,比如紫蘩蒌比较神秘难以捉摸等特点来类比RNase P相关特性,但仅从字面翻译就是“紫蘩蒌” )

RNase P--a 'Scarlet Pimpernel'.

作者信息

Kirsebom L A

机构信息

Department of Microbiology, Biomedical Centre, Uppsala, Sweden.

出版信息

Mol Microbiol. 1995 Aug;17(3):411-20. doi: 10.1111/j.1365-2958.1995.mmi_17030411.x.

Abstract

RNase P is responsible for the maturation of the 5'-termini of tRNA molecules in all cells studied to date. This ribonucleoprotein has to recognize and identify its cleavage site on a large number of different precursors. This review covers what is currently known about the function of the catalytic subunit of Escherichia coli RNase P, M1 RNA, and the protein subunit, C5, in particular with respect to cleavage-site selection. Recent genetic and biochemical data show that the two C residues in the 3'-terminal CCA sequence of a precursor interact with the enzyme through Watson-Crick base-pairing. This is suggested to result in unfolding of the amino acid acceptor-stem and exposure of the cleavage site. Furthermore, other close contact points between M1 RNA and its substrate have recently been identified. These data, together with the two existing three-dimensional structure models of M1 RNA in complex with its substrate, establish a platform that will enable us to seek an understanding of the underlying mechanism of cleavage by this elusive enzyme.

摘要

核糖核酸酶P(RNase P)负责迄今所有已研究细胞中转运RNA(tRNA)分子5'末端的成熟。这种核糖核蛋白必须识别并确定大量不同前体上的切割位点。本综述涵盖了目前已知的大肠杆菌核糖核酸酶P的催化亚基M1 RNA和蛋白质亚基C5的功能,特别是关于切割位点选择方面。最近的遗传和生化数据表明,前体3'末端CCA序列中的两个C残基通过沃森-克里克碱基配对与该酶相互作用。这被认为会导致氨基酸接受茎的展开并暴露切割位点。此外,最近还确定了M1 RNA与其底物之间的其他紧密接触点。这些数据,连同现有的两个M1 RNA与其底物复合物的三维结构模型,建立了一个平台,将使我们能够深入了解这种难以捉摸的酶的切割潜在机制。

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