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抑制蛋白与视紫红质的相互作用:概念模型

Arrestin interaction with rhodopsin: conceptual models.

作者信息

Modzelewska Anna, Filipek Slawomir, Palczewski Krzysztof, Park Paul S-H

机构信息

International Institute of Molecular and Cell Biology, 02-109 Warsaw, Poland.

出版信息

Cell Biochem Biophys. 2006;46(1):1-15. doi: 10.1385/CBB:46:1:1.

Abstract

It is becoming increasingly apparent that G protein-coupled receptors (GPCRs) can exist and function as oligomers. This notion differs from the classical view of signaling wherein the receptor has been presumed to be monomeric. Despite this shift in views, the interpretation of data related to GPCR function is still largely carried out within the framework of a monomeric receptor. Rhodopsin is a prototypical GPCR that initiates phototransduction. Like other GPCRs, the activity of rhodopsin is regulated by phosphorylation and the binding of arrestin. In the current investigation, we have explored by modeling methods the interaction of rhodopsin and arrestin under the assumption that either one or two rhodopsin molecules bind each arrestin molecule. The dimeric receptor framework may provide a more accurate representation of the system and is therefore likely to lead to a better and more accurate understanding of GPCR signaling.

摘要

越来越明显的是,G蛋白偶联受体(GPCRs)可以以寡聚体的形式存在并发挥功能。这一概念不同于传统的信号传导观点,在传统观点中,受体被认为是单体形式。尽管观点发生了这种转变,但与GPCR功能相关的数据解释仍主要在单体受体的框架内进行。视紫红质是一种启动光转导的典型GPCR。与其他GPCR一样,视紫红质的活性受磷酸化和抑制蛋白结合的调节。在当前的研究中,我们通过建模方法探讨了视紫红质与抑制蛋白的相互作用,假设每个抑制蛋白分子结合一个或两个视紫红质分子。二聚体受体框架可能为该系统提供更准确的表征,因此可能会导致对GPCR信号传导有更好、更准确的理解。

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