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编码一种核糖体相关伴侣蛋白的SSB与核糖体蛋白基因协同调控。

SSB, encoding a ribosome-associated chaperone, is coordinately regulated with ribosomal protein genes.

作者信息

Lopez N, Halladay J, Walter W, Craig E A

机构信息

Department of Bacteriology, University of Wisconsin, Madison, Wisconsin 53706, USA.

出版信息

J Bacteriol. 1999 May;181(10):3136-43. doi: 10.1128/JB.181.10.3136-3143.1999.

Abstract

Genes encoding ribosomal proteins and other components of the translational apparatus are coregulated to efficiently adjust the protein synthetic capacity of the cell. Ssb, a Saccharomyces cerevisiae Hsp70 cytosolic molecular chaperone, is associated with the ribosome-nascent chain complex. To determine whether this chaperone is coregulated with ribosomal proteins, we studied the mRNA regulation of SSB under several environmental conditions. Ssb and the ribosomal protein rpL5 mRNAs were up-regulated upon carbon upshift and down-regulated upon amino acid limitation, unlike the mRNA of another cytosolic Hsp70, Ssa. Ribosomal protein and Ssb mRNAs, like many mRNAs, are down-regulated upon a rapid temperature upshift. The mRNA reduction of several ribosomal protein genes and Ssb was delayed by the presence of an allele, EXA3-1, of the gene encoding the heat shock factor (HSF). However, upon a heat shock the EXA3-1 mutation did not significantly alter the reduction in the mRNA levels of two genes encoding proteins unrelated to the translational apparatus. Analysis of gene fusions indicated that the transcribed region, but not the promoter of SSB, is sufficient for this HSF-dependent regulation. Our studies suggest that Ssb is regulated like a core component of the ribosome and that HSF is required for proper regulation of SSB and ribosomal mRNA after a temperature upshift.

摘要

编码核糖体蛋白和翻译装置其他组分的基因受到协同调控,以有效调节细胞的蛋白质合成能力。Ssb是酿酒酵母的一种胞质Hsp70分子伴侣,与核糖体-新生链复合体相关。为了确定这种分子伴侣是否与核糖体蛋白协同调控,我们研究了在几种环境条件下SSB的mRNA调控情况。与另一种胞质Hsp70即Ssa的mRNA不同,Ssb和核糖体蛋白rpL5的mRNA在碳源增加时上调,在氨基酸限制时下调。核糖体蛋白和Ssb的mRNA与许多mRNA一样,在温度快速上升时下调。编码热休克因子(HSF)的基因的一个等位基因EXA3-1的存在延迟了几种核糖体蛋白基因和Ssb的mRNA减少。然而,在热休克时,EXA3-1突变并没有显著改变两个编码与翻译装置无关蛋白质的基因的mRNA水平的降低。基因融合分析表明,SSB的转录区域而非启动子对于这种HSF依赖性调控是足够的。我们的研究表明,Ssb的调控方式类似于核糖体的核心组分,并且在温度上升后,HSF对于SSB和核糖体mRNA的正确调控是必需的。

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