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信号输出对酵母中G蛋白偶联受体Ste2p激动剂占有率的可变依赖性。

Variable Dependence of Signaling Output on Agonist Occupancy of Ste2p, a G Protein-coupled Receptor in Yeast.

作者信息

Sridharan Rajashri, Connelly Sara M, Naider Fred, Dumont Mark E

机构信息

From the Department of Biochemistry and Biophysics, University of Rochester Medical Center, Rochester, New York 14642.

the Department of Chemistry and Macromolecular Assembly Institute, College of Staten Island of the City University of New York, Staten Island, New York 10314, and.

出版信息

J Biol Chem. 2016 Nov 11;291(46):24261-24279. doi: 10.1074/jbc.M116.733006. Epub 2016 Sep 19.

Abstract

We report here on the relationship between ligand binding and signaling responses in the yeast pheromone response pathway, a well characterized G protein-coupled receptor system. Responses to agonist (α-factor) by cells expressing widely varying numbers of receptors depend primarily on fractional occupancy, not the absolute number of agonist-bound receptors. Furthermore, the concentration of competitive antagonist required to inhibit α-factor-dependent signaling is more than 10-fold higher than predicted based on the known ligand affinities. Thus, responses to a particular number of agonist-bound receptors can vary greatly, depending on whether there are unoccupied or antagonist-bound receptors present on the same cell surface. This behavior does not appear to be due to pre-coupling of receptors to G protein or to the Sst2p regulator of G protein signaling. The results are consistent with a signaling response that is determined by the integration of positive signals from agonist-occupied receptors and inhibitory signals from unoccupied receptors, where the inhibitory signals can be diminished by antagonist binding.

摘要

我们在此报告酵母信息素反应途径中配体结合与信号转导反应之间的关系,该途径是一个特征明确的G蛋白偶联受体系统。表达数量差异很大的受体的细胞对激动剂(α-因子)的反应主要取决于占据率,而非激动剂结合受体的绝对数量。此外,抑制α-因子依赖性信号转导所需的竞争性拮抗剂浓度比基于已知配体亲和力预测的浓度高出10倍以上。因此,对特定数量的激动剂结合受体的反应可能会有很大差异,这取决于同一细胞表面是否存在未占据或拮抗剂结合的受体。这种行为似乎并非由于受体与G蛋白的预偶联或G蛋白信号转导的Sst2p调节剂所致。这些结果与一种信号转导反应一致,该反应由激动剂占据的受体发出的正信号和未占据的受体发出的抑制信号整合决定,其中抑制信号可因拮抗剂结合而减弱。

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