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蛋白质转运起始过程中信号识别颗粒的GTP结合与水解

GTP binding and hydrolysis by the signal recognition particle during initiation of protein translocation.

作者信息

Miller J D, Wilhelm H, Gierasch L, Gilmore R, Walter P

机构信息

Department of Biochemistry and Biophysics, University of California Medical School, San Francisco 94143-0448.

出版信息

Nature. 1993 Nov 25;366(6453):351-4. doi: 10.1038/366351a0.

Abstract

The signal recognition particle (SRP) consists of one RNA and six protein subunits. The N-terminal domain of the 54K subunit contains a putative GTP-binding site, whereas the C-terminal domain binds signal sequences and SRP RNA. Binding of SRP to the signal sequence as it emerges from the ribosome creates a cytosolic targeting complex containing the nascent polypeptide chain, the translating ribosome, and SRP. This complex is directed to the endoplasmic reticulum membrane as a result of its interaction with the SRP receptor, a membrane protein composed of two subunits, SR alpha and SR beta, each of which also contains a GTP-binding domain. In the presence of GTP, SRP receptor binding to SRP causes the latter to dissociate from both the signal sequence and the ribosome. GTP is then hydrolysed so that SRP can be released from the SRP receptor and returned to the cytosol. Here we show that the 54K subunit (M(r) 54,000) of SRP (SRP54) is a GTP-binding protein stabilized in a nucleotide-free state by signal sequences, and that the SRP receptor both increases the affinity of SRP54 for GTP and activates its GTPase. We propose that nucleotide-mediated conformational changes in SRP54 regulate the release of signal sequences and the docking of ribosomes at the endoplasmic reticulum.

摘要

信号识别颗粒(SRP)由一个RNA和六个蛋白质亚基组成。54K亚基的N端结构域含有一个假定的GTP结合位点,而C端结构域则结合信号序列和SRP RNA。当信号序列从核糖体中出现时,SRP与之结合,形成一个包含新生多肽链、正在翻译的核糖体和SRP的胞质靶向复合物。由于该复合物与SRP受体相互作用,它被导向内质网膜,SRP受体是一种由两个亚基SRα和SRβ组成的膜蛋白,每个亚基也含有一个GTP结合结构域。在GTP存在的情况下,SRP受体与SRP结合会导致后者从信号序列和核糖体上解离。然后GTP被水解,使得SRP能够从SRP受体上释放并返回胞质溶胶。我们在此表明,SRP的54K亚基(Mr 54,000,即SRP54)是一种通过信号序列稳定在无核苷酸状态的GTP结合蛋白,并且SRP受体既能增加SRP54对GTP的亲和力,又能激活其GTP酶。我们提出,SRP54中由核苷酸介导的构象变化调节信号序列的释放以及核糖体在内质网上的对接。

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