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糖原合酶激酶 3β 相互作用蛋白作为 A-激酶锚定蛋白发挥作用。

Glycogen synthase kinase 3beta interaction protein functions as an A-kinase anchoring protein.

机构信息

Leibniz Institute for Molecular Pharmacology, Robert-Rössle-Strasse 10, 13125 Berlin, Germany.

出版信息

J Biol Chem. 2010 Feb 19;285(8):5507-21. doi: 10.1074/jbc.M109.047944. Epub 2009 Dec 11.

Abstract

A-kinase anchoring proteins (AKAPs) include a family of scaffolding proteins that target protein kinase A (PKA) and other signaling proteins to cellular compartments and thereby confine the activities of the associated proteins to distinct regions within cells. AKAPs bind PKA directly. The interaction is mediated by the dimerization and docking domain of regulatory subunits of PKA and the PKA-binding domain of AKAPs. Analysis of the interactions between the dimerization and docking domain and various PKA-binding domains yielded a generalized motif allowing the identification of AKAPs. Our bioinformatics and peptide array screening approaches based on this signature motif identified GSKIP (glycogen synthase kinase 3beta interaction protein) as an AKAP. GSKIP directly interacts with PKA and GSK3beta (glycogen synthase kinase 3beta). It is widely expressed and facilitates phosphorylation and thus inactivation of GSK3beta by PKA. GSKIP contains the evolutionarily conserved domain of unknown function 727. We show here that this domain of GSKIP and its vertebrate orthologues binds both PKA and GSK3beta and thereby provides a mechanism for the integration of PKA and GSK3beta signaling pathways.

摘要

A-激酶锚定蛋白(AKAPs)包括一组支架蛋白,可将蛋白激酶 A(PKA)和其他信号蛋白靶向到细胞区室,从而将相关蛋白的活性限制在细胞内的特定区域。AKAPs 直接与 PKA 结合。这种相互作用是由 PKA 调节亚基的二聚化和对接结构域和 AKAPs 的 PKA 结合结构域介导的。对二聚化和对接结构域与各种 PKA 结合结构域之间的相互作用的分析产生了一个通用基序,允许鉴定 AKAPs。我们基于该特征基序的生物信息学和肽阵列筛选方法将 GSKIP(糖原合酶激酶 3β相互作用蛋白)鉴定为 AKAP。GSKIP 直接与 PKA 和 GSK3β(糖原合酶激酶 3β)相互作用。它广泛表达,并促进 PKA 对 GSK3β的磷酸化和失活。GSKIP 包含进化上保守的未知功能域 727。我们在这里表明,GSKIP 的这个结构域及其脊椎动物同源物结合 PKA 和 GSK3β,从而为 PKA 和 GSK3β 信号通路的整合提供了一种机制。

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