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SCS1是hsp60 - ts突变等位基因的多拷贝抑制子,它不编码靶向线粒体的蛋白质。

SCS1, a multicopy suppressor of hsp60-ts mutant alleles, does not encode a mitochondrially targeted protein.

作者信息

Shu Y, Hallberg R L

机构信息

Department of Biology, Syracuse University, New York 13244, USA.

出版信息

Mol Cell Biol. 1995 Oct;15(10):5618-26. doi: 10.1128/MCB.15.10.5618.

Abstract

We identified and isolated a Saccharomyces cerevisiae gene which, when overexpressed, suppressed the temperature-sensitive phenotype of cells expressing a mutant allele of the gene encoding the mitochondrial chaperonin, Hsp60. This gene, SCS1 (suppressor of chaperonin sixty-1), encodes a 757-amino-acid protein of as yet unknown function which, nonetheless, has human, rice, and Caenorhabditis elegans homologs with high degrees (ca. 60%) of amino acid sequence identity. SCS1 is not an essential gene, but SCS1-null strains do not grow above 37 degrees C and show some growth-related defects at 30 degrees C as well. This gene is expressed at both 30 and 38 degrees C, producing little or no differences in mRNA levels at these two temperatures. Overexpression of SCS1 could not complement an HSP60-null allele, indicating that suppression was not due to the bypassing of Hsp60 activity. Of 10 other hsp60-ts alleles tested, five could also be suppressed by SCS1 overexpression. There were no common mutant phenotypes of the strains expressing these alleles that give any clue as to why they were suppressible while others were not. An epitope (influenza virus hemagglutinin)-tagged form of SCS1 in single copy complemented an SCS1-null allele. The Scs1-hemagglutinin protein was found to be at comparable levels and in similar multiply modified forms in cells growing at both 30 and 38 degrees C. Surprisingly, when localized either by cell fractionation procedures or by immunocytochemistry, these proteins were found not in mitochondria but in the cytosol. The overexpression of SCS1 had significant effects on the cellular levels of mRNAs encoding the proteins Cpn10 and Mgel, two other mitochondrial protein cochaperones, but not on mRNAs encoding a number of other mitochondrial or cytosolic proteins analyzed. The implications of these findings are discussed.

摘要

我们鉴定并分离出一个酿酒酵母基因,该基因过表达时,可抑制表达线粒体伴侣蛋白Hsp60编码基因突变等位基因的细胞的温度敏感表型。这个基因,即SCS1(伴侣蛋白60-1的抑制因子),编码一个757个氨基酸的蛋白质,其功能尚不清楚,不过,它在人类、水稻和秀丽隐杆线虫中有同源物,氨基酸序列同一性程度较高(约60%)。SCS1不是必需基因,但缺失SCS1的菌株在37摄氏度以上无法生长,在30摄氏度时也表现出一些与生长相关的缺陷。该基因在30摄氏度和38摄氏度时均有表达,在这两个温度下mRNA水平几乎没有差异。SCS1的过表达不能弥补HSP60缺失等位基因,这表明抑制作用不是由于绕过了Hsp60的活性。在测试的其他10个hsp60-ts等位基因中,有5个也可被SCS1过表达所抑制。表达这些等位基因的菌株没有共同的突变表型,无法提供任何线索来解释为什么有些等位基因可被抑制而其他等位基因则不能。单拷贝的带有表位(流感病毒血凝素)标签的SCS1形式可弥补SCS1缺失等位基因。发现Scs1-血凝素蛋白在30摄氏度和38摄氏度生长的细胞中的水平相当,且修饰形式相似。令人惊讶的是,通过细胞分级分离程序或免疫细胞化学进行定位时,发现这些蛋白不在线粒体中,而是在细胞质中。SCS1的过表达对编码另外两种线粒体蛋白伴侣Cpn10和Mgel的mRNA的细胞水平有显著影响,但对编码其他一些分析过的线粒体或细胞质蛋白的mRNA没有影响。本文讨论了这些发现的意义。

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