作者
Kunhong Xiao, Daniel B McClatchy, Arun K Shukla, Yang Zhao, Minyong Chen, Sudha K Shenoy, John R Yates III, Robert J Lefkowitz
发表日期
2007/7/17
期刊
Proceedings of the National Academy of Sciences
卷号
104
期号
29
页码范围
12011-12016
出版商
National Academy of Sciences
简介
β-arrestins are cytosolic proteins that form complexes with seven-transmembrane receptors after agonist stimulation and phosphorylation by the G protein-coupled receptor kinases. They play an essential role in receptor desensitization and endocytosis, and they also serve as receptor-regulated signaling scaffolds and adaptors. Moreover, in the past decade, a growing list of protein–protein interactions of β-arrestins pertinent to these functions has been documented. The discovery of several novel functions of β-arrestins stimulated us to perform a global proteomics analysis of β-arrestin-interacting proteins (interactome) as modulated by a model seven-transmembrane receptor, the angiotensin II type 1a receptor, in an attempt to assess the full range of functions of these versatile molecules. As determined by LC tandem MS, 71 proteins interacted with β-arrestin 1, 164 interacted with β-arrestin 2, and 102 interacted …
引用总数
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学术搜索中的文章
K Xiao, DB McClatchy, AK Shukla, Y Zhao, M Chen… - Proceedings of the National Academy of Sciences, 2007