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编码人翻译起始因子3(eIF3)p35亚基同源物的酿酒酵母HCR1基因是酵母eIF3的Rpg1p亚基中温度敏感突变的高拷贝抑制子。

The Saccharomyces cerevisiae HCR1 gene encoding a homologue of the p35 subunit of human translation initiation factor 3 (eIF3) is a high copy suppressor of a temperature-sensitive mutation in the Rpg1p subunit of yeast eIF3.

作者信息

Valásek L, Hasek J, Trachsel H, Imre E M, Ruis H

机构信息

Vienna Biocenter, Institute of Biochemistry and Molecular Cell Biology, University of Vienna, A-1030 Vienna, Austria.

出版信息

J Biol Chem. 1999 Sep 24;274(39):27567-72. doi: 10.1074/jbc.274.39.27567.

Abstract

The complex eukaryotic initiation factor 3 (eIF3) was shown to promote the formation of the 43 S preinitiation complex by dissociating 40 S and 60 S ribosomal subunits, stabilizing the ternary complex, and aiding mRNA binding to 40 S ribosomal subunits. Recently, we described the identification of RPG1 (TIF32), the p110 subunit of the eIF3 core complex in yeast. In a screen for Saccharomyces cerevisiae multicopy suppressors of the rpg1-1 temperature-sensitive mutant, an unknown gene corresponding to the open reading frame YLR192C was identified. When overexpressed, the 30-kDa gene product, named Hcr1p, was able to support, under restrictive conditions, growth of the rpg1-1 temperature-sensitive mutant, but not of a Rpg1p-depleted mutant. An hcr1 null mutant was viable, but showed slight reduction of growth when compared with the wild-type strain. Physical interaction between the Hcr1 and Rpg1 proteins was shown by co-immunoprecipitation analysis. The combination of Deltahcr1 and rpg1-1 mutations resulted in a synthetic enhancement of the slow growth phenotype at a semipermissive temperature. In a computer search, a significant homology to the human p35 subunit of the eIF3 complex was found. We assume that the yeast Hcr1 protein participates in translation initiation likely as a protein associated with the eIF3 complex.

摘要

复杂的真核生物起始因子3(eIF3)被证明可通过解离40S和60S核糖体亚基、稳定三元复合物以及协助mRNA与40S核糖体亚基结合来促进43S前起始复合物的形成。最近,我们描述了酵母中eIF3核心复合物的p110亚基RPG1(TIF32)的鉴定。在对rpg1-1温度敏感突变体的酿酒酵母多拷贝抑制子进行筛选时,鉴定出了一个与开放阅读框YLR192C对应的未知基因。当该基因过表达时,其30 kDa的基因产物(命名为Hcr1p)能够在限制条件下支持rpg1-1温度敏感突变体的生长,但不能支持Rpg1p缺失突变体的生长。hcr1缺失突变体是有活力的,但与野生型菌株相比,其生长略有下降。通过免疫共沉淀分析显示Hcr1和Rpg1蛋白之间存在物理相互作用。Deltahcr1和rpg1-1突变的组合导致在半允许温度下缓慢生长表型的合成增强。在计算机搜索中,发现与eIF3复合物的人类p35亚基有显著同源性。我们推测酵母Hcr1蛋白可能作为与eIF3复合物相关的蛋白质参与翻译起始。

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