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Activation of Heat Shock Genes Is Not Necessary for Protection by Heat Shock Transcription Factor 1 against Cell Death Due to a Single Exposure to High Temperatures

机译:热休克转录因子1不需要保护热休克基因的激活以防止由于一次暴露于高温而导致的细胞死亡

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摘要

Heat shock response, which is characterized by the induction of a set of heat shock proteins, is essential for induced thermotolerance and is regulated by heat shock transcription factors (HSFs). Curiously, HSF1 is essential for heat shock response in mammals, whereas in avian HSF3, an avian-specific factor is required for the burst activation of heat shock genes. Amino acid sequences of chicken HSF1 are highly conserved with human HSF1, but those of HSF3 diverge significantly. Here, we demonstrated that chicken HSF1 lost the ability to activate heat shock genes through the amino-terminal domain containing an alanine-rich sequence and a DNA-binding domain. Surprisingly, chicken and human HSF1 but not HSF3 possess a novel function that protects against a single exposure to mild heat shock, which is not mediated through the activation of heat shock genes. Overexpression of HSF1 mutants that could not bind to DNA did not restore the susceptibility to cell death in HSF1-null cells, suggesting that the new protective role of HSF1 is mediated through regulation of unknown target genes other than heat shock genes. These results uncover a novel role of vertebrate HSF1, which has been masked underthe roles of heat shock proteins.
机译:热激反应的特征是诱导一组热激蛋白,对诱导的耐热性至关重要,并受热激转录因子(HSF)调控。奇怪的是,HSF1对于哺乳动物的热激反应至关重要,而在禽类HSF3中,热激基因的爆发激活需要禽类特异性因子。鸡HSF1的氨基酸序列与人HSF1高度保守,但HSF3的氨基酸序列差异很大。在这里,我们证明了鸡HSF1通过包含富含丙氨酸的序列和DNA结合域的氨基末端域失去了激活热激基因的能力。出人意料的是,鸡和人的HSF1(而非HSF3)具有一种新颖的功能,可以防止单次暴露于轻度热激,而这种暴露不是通过热激基因的激活来介导的。无法与DNA结合的HSF1突变体的过表达不能恢复HSF1无细胞中细胞死亡的易感性,这表明HSF1的新保护作用是通过调节除热激基因以外的未知靶基因来介导的。这些结果揭示了脊椎动物HSF1的新作用,该作用已在热激蛋白的作用下被掩盖。

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