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位于核糖体肽基转移酶中心A位点结构域的蛋白质L23-RNA复合物的结构。

Structure of a protein L23-RNA complex located at the A-site domain of the ribosomal peptidyl transferase centre.

作者信息

Vester B, Garrett R A

出版信息

J Mol Biol. 1984 Nov 5;179(3):431-52. doi: 10.1016/0022-2836(84)90074-3.

Abstract

Protein L23 from the ribosome of Escherichia coli is the primary ribosomal product cross-linked to affinity-labelled puromycin; it lies, therefore, within the A-site domain of the peptidyl transferase centre on the 50 S subunit. We have characterized this functional domain by isolating and sequencing the RNA binding site of protein L23; it consists of two main fragments of 25 and 105 nucleotides that strongly interact and are separated by 172 nucleotides in the primary sequence. The higher-order structure of the RNA moiety was probed by chemical reagents, and by single-strand and double-strand-specific ribonucleases; a secondary structural model and a tertiary structural interaction are proposed on the basis of these data that are compatible with phylogenetic sequence comparisons. Several nucleotides exhibited altered chemical reactivity, both lower and higher, in the presence of protein L23, thereby implicating a large proportion of the RNA structure in the protein binding. The sites were located mainly at the extremities of the helices and at nucleotides that were putatively bulged out from the helices. The RNA moiety and an adjacent excised fragment contain several highly conserved sequences and a modified adenosine. Such sequences constitute important functional domains of the RNA and may contribute to the putative role of this RNA region in the peptidyl transferase centre.

摘要

来自大肠杆菌核糖体的蛋白质L23是与亲和标记嘌呤霉素交联的主要核糖体产物;因此,它位于50 S亚基肽基转移酶中心的A位点结构域内。我们通过分离和测序蛋白质L23的RNA结合位点对该功能结构域进行了表征;它由两个分别为25和105个核苷酸的主要片段组成,这两个片段强烈相互作用,在一级序列中被172个核苷酸隔开。用化学试剂以及单链和双链特异性核糖核酸酶探测了RNA部分的高级结构;基于这些数据并与系统发育序列比较相兼容,提出了一个二级结构模型和一个三级结构相互作用。在蛋白质L23存在的情况下,几个核苷酸的化学反应性发生了改变,有降低的也有升高的,从而表明蛋白质结合涉及RNA结构的很大一部分。这些位点主要位于螺旋的末端以及假定从螺旋中凸出的核苷酸处。RNA部分和一个相邻的切除片段包含几个高度保守的序列和一个修饰的腺苷。这些序列构成了RNA的重要功能结构域,可能有助于该RNA区域在肽基转移酶中心的假定作用。

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