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首页> 外文期刊>Journal of cell biology >Regulated degradation of HMG-CoA reductase, an integral membrane protein of the endoplasmic reticulum, in yeast.
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Regulated degradation of HMG-CoA reductase, an integral membrane protein of the endoplasmic reticulum, in yeast.

机译:HMG-CoA还原酶(一种内质网的整合膜蛋白)在酵母中的调控降解。

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摘要

Numerous integral membrane proteins are degraded in the mammalian ER. HMG-CoA reductase (HMG-R), a key enzyme in the mevalonate pathway by which isoprenoids and sterols are synthesized, is one substrate of ER degradation. The degradation of HMG-R is modulated by feedback signals from the mevalonate pathway. We investigated the role of regulated degradation of the two isozymes of HMG-R, Hmg1p and Hmg2p, in the physiology of Saccharomyces cerevisiae. Hmg1p was quite stable, whereas Hmg2p was rapidly degraded. Degradation of Hmg2p proceeded independently of vacuolar proteases or secretory traffic, indicating that Hmg2p degradation occurred at the ER. Hmg2p stability was strongly affected by modulation of the mevalonate pathway through pharmacological or genetic means. Decreased mevalonate pathway flux resulted in decreased degradation of Hmg2p. One signal for degradation of Hmg2p was a nonsterol, mevalonate-derived molecule produced before the synthesis of squalene. Genetic evidence indicated that a farnesylated protein may also be necessary for Hmg2p degradation. Studies with reporter genes demonstrated that the stability of each isozyme was determined by its noncatalytic NH2-terminal domain. Our data show that ER protein degradation is widely conserved among eukaryotes, and that feedback control of HMG-R degradation is an ancient paradigm of regulation.
机译:在哺乳动物的ER中,许多完整的膜蛋白被降解。 HMG-CoA还原酶(HMG-R)是甲羟戊酸途径中合成类异戊二烯和固醇的关键酶,是ER降解的一种底物。 HMG-R的降解受甲羟戊酸途径的反馈信号调节。我们调查了酿酒酵母的生理中HMG-R的两个同工酶Hmg1p和Hmg2p的调控降解作用。 Hmg1p非常稳定,而Hmg2p则迅速降解。 Hmg2p的降解独立于液泡状蛋白酶或分泌运输而进行,表明Hmg2p降解发生在ER。 Hmg2p的稳定性受到药理学或遗传学手段对甲羟戊酸途径的调节的强烈影响。甲羟戊酸途径通量减少导致Hmg2p降解降低。 Hmg2p降解的一个信号是在角鲨烯合成之前产生的非甾醇,甲羟戊酸酯衍生的分子。遗传证据表明,法尼基化蛋白对于Hmg2p降解也可能是必需的。报告基因的研究表明,每种同工酶的稳定性取决于其非催化的NH2末端结构域。我们的数据表明,ER蛋白降解在真核生物中被广泛保存,而HMG-R降解的反馈控制是一种古老的调控模式。

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