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氟化铝和GDP而非GTPγS激活G蛋白α亚基时对分子内结构域相互作用的需求。

Requirement for intramolecular domain interaction in activation of G protein alpha subunit by aluminum fluoride and GDP but not by GTP gamma S.

作者信息

Codina J, Birnbaumer L

机构信息

Department of Cell Biology, Baylor College of Medicine, Houston, Texas 77030.

出版信息

J Biol Chem. 1994 Nov 25;269(47):29339-42.

PMID:7961906
Abstract

An ion-counterion interaction between the lysine of the NKXD motif in the GTPase domain and an aspartate in the inserted helical domain of alpha subunits of heterotrimeric G proteins, Lys-278 and Asp-158, respectively, of Gs alpha is shown to be essential for activation by AlF4- and partially so for interaction with beta gamma dimers and activation by GTP and receptor. However, this domain interaction is not required for activation by the non-hydrolyzable analog guanosine 5'-3-O-(thio)triphosphate. Proximity of the helical domain to the GTPase domain is thus involved in the fundamental inactive-->active transition of the protein in a way that further distinguishes alpha subunits of heterotrimeric G proteins from ras and ras-like GTPases that lack helical domains and are neither activated by AlF4- nor combine with beta gamma dimers.

摘要

已表明,异源三聚体G蛋白α亚基中GTP酶结构域的NKXD基序的赖氨酸与插入的螺旋结构域中的天冬氨酸之间的离子-反离子相互作用(分别为Gsα的Lys-278和Asp-158)对于AlF4-激活至关重要,对于与βγ二聚体相互作用以及被GTP和受体激活则部分重要。然而,这种结构域相互作用对于不可水解类似物鸟苷5'-3-O-(硫代)三磷酸的激活并非必需。因此,螺旋结构域与GTP酶结构域的接近以一种进一步将异源三聚体G蛋白的α亚基与缺乏螺旋结构域、既不被AlF4-激活也不与βγ二聚体结合的ras和ras样GTP酶区分开来的方式,参与了蛋白质从根本的无活性到活性的转变。

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