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前胰岛素原跨内质网膜的转运。新生多肽大小与信号识别颗粒介导的蛋白质合成抑制程度之间的关系。

Translocation of preproinsulin across the endoplasmic reticulum membrane. The relationship between nascent polypeptide size and extent of signal recognition particle-mediated inhibition of protein synthesis.

作者信息

Okun M M, Shields D

机构信息

Department of Developmental Biology and Cancer, Albert Einstein College of Medicine, Bronx, New York 10461.

出版信息

J Biol Chem. 1992 Jun 5;267(16):11476-82.

PMID:1317869
Abstract

Signal recognition particle (SRP) induces elongation arrest of nascent presecretory proteins as the signal peptide protrudes from the large ribosomal subunit. To examine the relationship between the size of the precursor and extent of SRP mediated inhibition of polypeptide chain elongation, we performed in vitro translation experiments in the presence of SRP using a series of truncated preproinsulin mRNA molecules. These precursors possessed the same NH2 terminus as native preproinsulin followed by progressively shorter COOH termini. SRP inhibited translation of precursors as short as 64 amino acids in length, however, the extent of inhibition diminished for shorter precursors. This correlated with a reduction in the time required for ribosomes to transit through the mRNA encoding the shortened precursors. By exploiting a chimeric protein comprising the first 71 residues of preproinsulin fused to the bacterial cytoplasmic enzyme chloramphenicol acetyltransferase, we demonstrate that the largest size a nascent chain can reach and still be susceptible to SRP-mediated elongation arrest is approximately 17 kDa. Our data support the model that SRP binding to the signal peptide is a reversible process even in the absence of microsomal membranes, and that SRP can arrest polypeptide chain elongation at multiple stages during translation.

摘要

当信号肽从大核糖体亚基突出时,信号识别颗粒(SRP)会诱导新生的分泌前体蛋白的延伸停滞。为了研究前体大小与SRP介导的多肽链延伸抑制程度之间的关系,我们使用一系列截短的胰岛素原mRNA分子,在存在SRP的情况下进行了体外翻译实验。这些前体具有与天然胰岛素原相同的NH2末端,随后COOH末端逐渐变短。SRP抑制长度仅为64个氨基酸的前体的翻译,然而,对于更短的前体,抑制程度有所降低。这与核糖体穿过编码缩短前体的mRNA所需时间的减少相关。通过利用一种嵌合蛋白,该蛋白由胰岛素原的前71个残基与细菌细胞质酶氯霉素乙酰转移酶融合而成,我们证明新生链能够达到且仍易受SRP介导的延伸停滞影响的最大大小约为17 kDa。我们的数据支持这样的模型,即即使在没有微粒体膜的情况下,SRP与信号肽的结合也是一个可逆过程,并且SRP可以在翻译过程的多个阶段阻止多肽链的延伸。

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