[酿酒酵母中的Ras蛋白,它们的伴侣和它们的激活]。

M Jacquet
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引用次数: 0

摘要

Ras蛋白通过GTP和gdp结合状态之间的构象变化发挥分子开关的作用。在酵母中,它们由两个部分冗余基因RAS1和RAS2编码,但基因表达模式不同。它们对生长至关重要,因为它们是激活腺苷酸环化酶和蛋白激酶A途径所必需的。其他可能的生物学功能仍有待确定。为了实现它们的生物学功能,它们在合成后需要进行加工,它们在CaaX盒的c端被修饰法酰化和棕榈酰化。棕榈酰化参与膜定位,对生长不是必需的,但对葡萄糖信号传导是必需的,而法尼酰化似乎参与腺苷酸环化酶激活。在gtp结合状态下,ras蛋白通过其保守的效应域与腺苷酸环化酶(CYR1/CDC35基因的产物)相互作用。它们还与由IRA1和IRA2编码的GTPase激活蛋白相互作用。这些蛋白质是酵母ras所特有的。研究表明,Ira2p可以识别哺乳动物ras所不具有的酵母ras的特定残基。与CDC25家族的鸟嘌呤核苷酸交换因子(GEF)的相互作用被RAS2ala22等显性负突变增强。利用两种混合方法,我们发现了Ras2p中80位的关键作用,并证实了ras的另一个开关部分a2螺旋参与了这种相互作用和诱导效应。作为对应物,我们已经确定了HGRF55在其他参与ras相互作用的GEF中保守的位置。ras激活的触发元件:GEF Cdc25p和Sdc25p是ras系统的限制性元件。Cdc25p是与细胞膜相关的多分子复合物的一部分。我们已经证明它可以与Sdc25p形成同二聚体和异二聚体。它是一种含有细胞周期蛋白破坏盒的不稳定蛋白质。因此,其对ras的活性可以通过控制其细胞含量来调节。
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[Ras proteins in Saccharomyces cerevisiae, their partners and their activation].

Ras proteins play the role of molecular switches by conformational change between a GTP and a GDP-bound state. In the yeast Saccharomyces cerevisiae, they are encoded by two partially redundant genes RAS1 and RAS2 with a different pattern of gene expression. They are essential for growth because they are required for the activation of the adenylate cyclase and thus the protein kinase A pathway. Other possible biological functions remains to be established. To achieve their biological function, they need to be processed after their synthesis, they are modified farnesylated and palmitoylated at their C-terminal end at their CaaX box. Palmitoylation, involved in membrane localization, is not essential for growth but required for glucose signaling whereas farnesylation appears to participate in adenylate cyclase activation. In the GTP-bound state ras proteins interact through their conserved effector domain with the adenylate cyclase, the product of the CYR1/CDC35 gene. They also interact with GTPase activating proteins encoded by IRA1 and IRA2. These proteins are specific for yeast ras. It has been shown that Ira2p recognizes specific residues of yeast ras not shared by mammalian ras. The interaction with the guanine nucleotide exchange factor (GEF) of the CDC25 family is enhanced by dominant negative mutations such as RAS2ala22. Using the two hybrid approach, we have showed the key role of position 80 in Ras2p and confirmed the involvement of the a2 helix, the other switching part of ras, in this interaction and the induced effect. As a counterpart we have identified positions in HGRF55 conserved in other GEF involved in ras interaction. The triggering elements of ras activation: the GEF Cdc25p and Sdc25p are limiting components of the ras system. Cdc25p is part of a multimolecular complex associated with the membrane. We have shown that it can form homodimers and heterodimers with Sdc25p. It is an unstable protein containing a cyclin destruction box. Therefore its activity on ras could be regulated by controlling its cellular content.

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