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氨基端和羧基端序列在调控Chp非典型Rho GTP酶生物活性中的关键且独特作用。

Critical and distinct roles of amino- and carboxyl-terminal sequences in regulation of the biological activity of the Chp atypical Rho GTPase.

作者信息

Chenette Emily J, Abo Arie, Der Channing J

机构信息

Curriculum in Genetics and Molecular Biology, University of North Carolina, Chapel Hill, North Carolina 27599-7295, USA.

出版信息

J Biol Chem. 2005 Apr 8;280(14):13784-92. doi: 10.1074/jbc.M411300200. Epub 2005 Jan 21.

DOI:10.1074/jbc.M411300200
PMID:15664990
Abstract

Chp (Cdc42 homologous protein) shares significant sequence and functional identity with the human Cdc42 small GTPase, and like Cdc42, promotes formation of filopodia and activates the p21-activated kinase serine/threonine kinase. However, unlike Cdc42, Chp contains unique amino- and carboxyl-terminal extensions. Here we determined whether Chp, like Cdc42, can promote growth transformation and evaluated the role of the amino- and carboxyl-terminal sequences in Chp function. Surprisingly, we found that a GTPase-deficient mutant of Chp exhibited low transforming activity but that deletion of the amino terminus of Chp greatly enhanced its transforming activity. Thus, the amino terminus may serve as a negative regulator of Chp function. The carboxyl terminus of Cdc42 contains a CAAX (where C is cysteine, A is aliphatic amino acid, X is terminal amino acid) tetrapeptide sequence that signals for the posttranslational modification critical for Cdc42 membrane association and biological function. Although Chp lacks aCAAXmotif, we found that Chp showed carboxyl terminus-dependent localization to the plasma membrane and to endosomes. Furthermore, an intact carboxyl terminus was required for Chp transforming activity. However, treatment with inhibitors of protein palmitoylation, but not prenylation, caused Chp to mislocalize to the cytoplasm. Thus, Chp depends on palmitoylation, rather than isoprenylation, for membrane association and function. In summary, Chp is implicated in cell transformation, and the unique amino and carboxyl termini of Chp represent atypical mechanisms of regulation of Rho GTPase function.

摘要

Chp(Cdc42同源蛋白)与人类Cdc42小GTP酶具有显著的序列和功能一致性,并且与Cdc42一样,促进丝状伪足的形成并激活p21激活激酶丝氨酸/苏氨酸激酶。然而,与Cdc42不同的是,Chp含有独特的氨基末端和羧基末端延伸。在这里,我们确定Chp是否像Cdc42一样能够促进生长转化,并评估了氨基末端和羧基末端序列在Chp功能中的作用。令人惊讶的是,我们发现Chp的一个GTP酶缺陷型突变体表现出低转化活性,但Chp氨基末端的缺失极大地增强了其转化活性。因此,氨基末端可能作为Chp功能的负调节因子。Cdc42的羧基末端包含一个CAAX(其中C是半胱氨酸,A是脂肪族氨基酸,X是末端氨基酸)四肽序列,该序列为Cdc42膜结合和生物学功能所必需的翻译后修饰发出信号。虽然Chp缺乏CAAX基序,但我们发现Chp表现出依赖羧基末端定位于质膜和内体。此外,完整的羧基末端是Chp转化活性所必需的。然而,用蛋白质棕榈酰化抑制剂而非异戊二烯化抑制剂处理会导致Chp错误定位于细胞质。因此,Chp的膜结合和功能依赖于棕榈酰化而非异戊二烯化。总之,Chp与细胞转化有关,Chp独特的氨基末端和羧基末端代表了Rho GTP酶功能调节的非典型机制。

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