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RGSZ1,一种G蛋白信号的Gz选择性调节剂,其作用对Gzα的磷酸化状态敏感。

RGSZ1, a Gz-selective regulator of G protein signaling whose action is sensitive to the phosphorylation state of Gzalpha.

作者信息

Glick J L, Meigs T E, Miron A, Casey P J

机构信息

Department of Biochemistry, Duke University Medical Center, Durham, North Carolina 27710-3686, USA.

出版信息

J Biol Chem. 1998 Oct 2;273(40):26008-13. doi: 10.1074/jbc.273.40.26008.

Abstract

Regulators of G protein signaling (RGS) are a family of proteins that attenuate the activity of the trimeric G proteins. RGS proteins act as GTPase-activating proteins (GAPs) for the alpha subunits of several trimeric G proteins, much like the GAPs that regulate the activity of monomeric G proteins such as Ras. RGS proteins have been cloned from many eukaryotes, and those whose biochemical activity has been characterized regulate the members of the Gi family of G proteins; some forms can also act on Gq proteins. In an ongoing effort to elucidate the role of Gzalpha in cell signaling, the yeast two-hybrid system was employed to identify proteins that could interact with a mutationally activated form of Gzalpha. A novel RGS, termed RGSZ1, was identified that is most closely related to two existing RGS proteins termed RetRGS1 and GAIP. Northern blot analysis revealed that expression of RGSZ1 was limited to brain, and expression was particularly high in the caudate nucleus. Biochemical characterization of recombinant RGSZ1 protein revealed that RGSZ1 was indeed a GAP and, most significantly, showed a marked preference for Gzalpha over other members of the Gialpha family. Phosphorylation of Gzalpha by protein kinase C, an event known to occur in cells and that was previously shown to influence alpha-betagamma interactions of Gz, rendered the G protein much less susceptible to RGSZ1 action.

摘要

G蛋白信号调节因子(RGS)是一类可减弱三聚体G蛋白活性的蛋白质家族。RGS蛋白作为几种三聚体G蛋白α亚基的GTP酶激活蛋白(GAP),这与调节诸如Ras等单体G蛋白活性的GAP非常相似。RGS蛋白已从许多真核生物中克隆出来,那些已被表征其生化活性的RGS蛋白可调节G蛋白Gi家族的成员;一些形式的RGS蛋白也可作用于Gq蛋白。为了不断阐明Gzα在细胞信号传导中的作用,采用酵母双杂交系统来鉴定能够与突变激活形式的Gzα相互作用的蛋白质。一种名为RGSZ1的新型RGS被鉴定出来,它与两种现有的RGS蛋白RetRGS1和GAIP关系最为密切。Northern印迹分析表明,RGSZ1的表达仅限于大脑,并且在尾状核中表达特别高。重组RGSZ1蛋白的生化特性表明,RGSZ1确实是一种GAP,并且最显著的是,与Gαi家族的其他成员相比,它对Gzα表现出明显的偏好。蛋白激酶C对Gzα的磷酸化作用(这是已知在细胞中发生的事件,并且先前已证明会影响Gz的αβγ相互作用)使G蛋白对RGSZ1作用的敏感性大大降低。

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