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确定磷脂酰肌醇3激酶γ的p101调节亚基内的功能结构域。

Assigning functional domains within the p101 regulatory subunit of phosphoinositide 3-kinase gamma.

作者信息

Voigt Philipp, Brock Carsten, Nürnberg Bernd, Schaefer Michael

机构信息

Institut für Pharmakologie, Charité-Universitätsmedizin Berlin, Campus Benjamin Franklin, Thielallee 67-73, 14195 Berlin, Germany.

出版信息

J Biol Chem. 2005 Feb 11;280(6):5121-7. doi: 10.1074/jbc.M413104200. Epub 2004 Dec 20.

Abstract

Phosphoinositide 3-Kinase (PI3K) gamma is a lipid kinase that is regulated by G-protein-coupled receptors. It plays a crucial role in inflammatory and allergic processes. Activation of PI3Kgamma is primarily mediated by Gbetagamma subunits. The regulatory p101 subunit of PI3Kgamma binds to Gbetagamma and, thereby, recruits the catalytic p110gamma subunit to the plasma membrane. Despite its crucial role in the activation of PI3Kgamma, the structural organization of p101 is still largely elusive. Employing fluorescence resonance energy transfer measurements, coimmunoprecipitation and colocalization studies with p101 deletion mutants, we show here that distinct regions within the p101 primary structure are responsible for interaction with p110gamma and Gbetagamma. The p110gamma binding site is confined to the N terminus, whereas binding to Gbetagamma is mediated by a C-terminal domain of p101. These domains appear to be highly conserved among various species ranging from Xenopus to men. In addition to establishing a domain structure for p101, our results point to the existence of a previously unknown, p101-related regulatory subunit for PI3Kgamma.

摘要

磷脂酰肌醇3激酶(PI3K)γ是一种受G蛋白偶联受体调控的脂质激酶。它在炎症和过敏过程中起关键作用。PI3Kγ的激活主要由Gβγ亚基介导。PI3Kγ的调节性p101亚基与Gβγ结合,从而将催化性p110γ亚基募集到质膜。尽管p101在PI3Kγ的激活中起关键作用,但其结构组织仍大多未知。通过荧光共振能量转移测量、与p101缺失突变体的共免疫沉淀和共定位研究,我们在此表明p101一级结构内的不同区域负责与p110γ和Gβγ相互作用。p110γ结合位点局限于N端,而与Gβγ的结合由p101的C端结构域介导。这些结构域在从非洲爪蟾到人类的各种物种中似乎高度保守。除了为p101建立结构域结构外,我们的结果还指出存在一种以前未知的、与p101相关的PI3Kγ调节亚基。

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