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热休克元件结构是热休克转录因子的温度和反式激活结构域要求的重要决定因素。

Heat shock element architecture is an important determinant in the temperature and transactivation domain requirements for heat shock transcription factor.

作者信息

Santoro N, Johansson N, Thiele D J

机构信息

Department of Biological Chemistry, The University of Michigan Medical School, Ann Arbor, Michigan 48109-0606, USA.

出版信息

Mol Cell Biol. 1998 Nov;18(11):6340-52. doi: 10.1128/MCB.18.11.6340.

Abstract

The baker's yeast Saccharomyces cerevisiae possesses a single gene encoding heat shock transcription factor (HSF), which is required for the activation of genes that participate in stress protection as well as normal growth and viability. Yeast HSF (yHSF) contains two distinct transcriptional activation regions located at the amino and carboxyl termini. Activation of the yeast metallothionein gene, CUP1, depends on a nonconsensus heat shock element (HSE), occurs at higher temperatures than other heat shock-responsive genes, and is highly dependent on the carboxyl-terminal transactivation domain (CTA) of yHSF. The results described here show that the noncanonical (or gapped) spacing of GAA units in the CUP1 HSE (HSE1) functions to limit the magnitude of CUP1 transcriptional activation in response to heat and oxidative stress. The spacing in HSE1 modulates the dependence for transcriptional activation by both stresses on the yHSF CTA. Furthermore, a previously uncharacterized HSE in the CUP1 promoter, HSE2, modulates the magnitude of the transcriptional activation of CUP1, via HSE1, in response to stress. In vitro DNase I footprinting experiments suggest that the occupation of HSE2 by yHSF strongly influences the manner in which yHSF occupies HSE1. Limited proteolysis assays show that HSF adopts a distinct protease-sensitive conformation when bound to the CUP1 HSE1, providing evidence that the HSE influences DNA-bound HSF conformation. Together, these results suggest that CUP1 regulation is distinct from that of other classic heat shock genes through the interaction of yHSF with two nonconsensus HSEs. Consistent with this view, we have identified other gene targets of yHSF containing HSEs with sequence and spacing features similar to those of CUP1 HSE1 and show a correlation between the spacing of the GAA units and the relative dependence on the yHSF CTA.

摘要

面包酵母酿酒酵母拥有一个编码热休克转录因子(HSF)的单一基因,该基因对于激活参与应激保护以及正常生长和生存能力的基因是必需的。酵母HSF(yHSF)在氨基和羧基末端包含两个不同的转录激活区域。酵母金属硫蛋白基因CUP1的激活取决于一个非共有热休克元件(HSE),发生在比其他热休克反应基因更高的温度下,并且高度依赖于yHSF的羧基末端反式激活结构域(CTA)。此处描述的结果表明,CUP1 HSE(HSE1)中GAA单元的非规范(或有间隔)间距起到限制CUP1转录激活对热和氧化应激反应的幅度的作用。HSE1中的间距调节两种应激对yHSF CTA转录激活的依赖性。此外,CUP1启动子中一个先前未被表征的HSE,HSE2,通过HSE1调节CUP1对应激反应的转录激活幅度。体外DNase I足迹实验表明,yHSF对HSE2的占据强烈影响yHSF占据HSE1的方式。有限蛋白酶解分析表明,当HSF与CUP1 HSE1结合时,它会采用一种独特的对蛋白酶敏感的构象,这证明HSE会影响与DNA结合的HSF构象。总之,这些结果表明,通过yHSF与两个非共有HSE的相互作用,CUP1的调控与其他经典热休克基因不同。与此观点一致,我们已经鉴定出yHSF的其他基因靶点,其含有与CUP1 HSE1具有相似序列和间距特征的HSE,并显示GAA单元的间距与对yHSF CTA的相对依赖性之间存在相关性。

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