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磷脂酶C-β的一种独特折叠介导二聚化以及与Gαq的相互作用。

A unique fold of phospholipase C-beta mediates dimerization and interaction with G alpha q.

作者信息

Singer Alex U, Waldo Gary L, Harden T Kendall, Sondek John

机构信息

Department of Pharmacology, The University of North Carolina at Chapel Hill, North Carolina 27599, USA.

出版信息

Nat Struct Biol. 2002 Jan;9(1):32-6. doi: 10.1038/nsb731.

Abstract

GTP-bound subunits of the Gq family of G alpha subunits directly activate phospholipase C-beta (PLC-beta) isozymes to produce the second messengers inositol 1,4,5-trisphosphate and diacylglycerol. PLC-betas are GTPase activating proteins (GAPs) that also promote the formation of GDP-bound, inactive G beta subunits. Both phospholipase activation by G alpha-GTP subunits and GAP activity require a C-terminal region unique to PLC-beta isozymes. The crystal structure of the C-terminal region from an avian PLC-beta, determined at 2.4 A resolution, reveals a novel fold composed almost entirely of three long helices forming a coiled-coil that dimerizes along its long axis in an antiparallel orientation. The dimer interface is extensive ( approximately 3,200 A(2)), and, based on gel exclusion chromatography, full length PLC-betas are dimeric, indicating that PLC-betas likely function as dimers. Sequence conservation, mutational data and molecular modeling show that an electrostatically positive surface of the dimer contains the major determinants for binding G beta q. Effector dimerization, as highlighted by PLC-betas, provides a viable mechanism for regulating signaling cascades linked to heterotrimeric G proteins.

摘要

Gα亚基的Gq家族中与GTP结合的亚基直接激活磷脂酶C-β(PLC-β)同工酶,以产生第二信使肌醇1,4,5-三磷酸和二酰基甘油。PLC-β是GTP酶激活蛋白(GAP),也促进形成与GDP结合的无活性Gβ亚基。Gα-GTP亚基对磷脂酶的激活以及GAP活性都需要PLC-β同工酶特有的C末端区域。以2.4埃分辨率测定的禽源PLC-β C末端区域的晶体结构揭示了一种几乎完全由三个长螺旋组成的新型折叠结构,这些螺旋形成一个卷曲螺旋,沿其长轴以反平行方向二聚化。二聚体界面广泛(约3200 Ų),基于凝胶排阻色谱法,全长PLC-β是二聚体,表明PLC-β可能以二聚体形式发挥作用。序列保守性、突变数据和分子建模表明,二聚体的一个带正电的表面包含结合Gβq的主要决定因素。如PLC-β所突出显示的,效应器二聚化为调节与异源三聚体G蛋白相关的信号级联提供了一种可行的机制。

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