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Reassembly and protection of small nuclear ribonucleoprotein particles by heat shock proteins in yeast cells.

机译:酵母细胞中的热激蛋白重新组装和保护核小核糖核蛋白小颗粒。

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摘要

The process of mRNA splicing is sensitive to in vivo thermal inactivation, but can be protected by pretreatment of cells under conditions that induce heat-shock proteins (Hsps). This latter phenomenon is known as "splicing thermotolerance". In this article we demonstrate that the small nuclear ribonucleoprotein particles (snRNPs) are in vivo targets of thermal damage within the splicing apparatus in heat-shocked yeast cells. Following a heat shock, levels of the tri-snRNP (U4/U6.U5), free U6 snRNP, and a pre-U6 snRNP complex are dramatically reduced. In addition, we observe multiple alterations in U1, U2, U5, and U4/U6 snRNP profiles and the accumulation of precursor forms of U4- and U6-containing snRNPs. Reassembly of snRNPs following a heat shock is correlated with the recovery of mRNA splicing and requires both Hsp104 and the Ssa Hsp70 family of proteins. Furthermore, we correlate splicing thermotolerance with the protection of a subset of snRNPs by Ssa proteins but not Hsp104, and show that Hsp70 directly associates with U4- and U6-containing snRNPs in splicing thermotolerant cells. In addition, our results show that Hsp70 plays a role in snRNP assembly under normal physiological conditions.
机译:mRNA剪接的过程对体内的热失活很敏感,但是可以通过在诱导热激蛋白(Hsps)的条件下对细胞进行预处理来对其进行保护。后一种现象称为“拼接耐热性”。在本文中,我们证明了小核糖核糖核蛋白颗粒(snRNPs)是热激酵母细胞中剪接设备内热损伤的体内靶标。热冲击后,三-snRNP(U4 / U6.U5),游离的U6 snRNP和U6之前的snRNP复合物的水平显着降低。此外,我们观察到U1,U2,U5和U4 / U6 snRNP配置文件中的多个变化以及包含U4和U6的snRNP的前体形式的积累。热休克后snRNPs的重组与mRNA剪接的恢复相关,并且需要Hsp104和Ssa Hsp70家族的蛋白质。此外,我们将剪接的耐热性与Ssa蛋白而不是Hsp104对snRNPs子集的保护相关联,并显示Hsp70在剪接的耐热细胞中直接与含U4和U6的snRNPs关联。此外,我们的结果表明,在正常生理条件下,Hsp70在snRNP装配中起作用。

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    Bracken, A P; Bond, U;

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  • 年度 1999
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  • 正文语种 en
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