G蛋白偶联嘌呤能受体的二聚化:增加嘌呤能受体信号反应和受体功能的多样性。

IF 2.3
Hiroyasu Nakata, Tokiko Suzuki, Kazunori Namba, Koshi Oyanagi
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引用次数: 25

摘要

G蛋白偶联受体(gpcr)排列成二聚体或高阶低聚体,可以改变gpcr的各种功能。gpcr型嘌呤能受体(即腺苷和P2Y受体)不仅与不同家族的gpcr形成异源二聚体,而且与相同家族的嘌呤能受体形成异源二聚体,从而导致功能特性的改变。在目前的综述中,我们关注的是代谢嘌呤能受体之间异二聚体的形成,这些异二聚体可以激活细胞外核苷/核苷酸的新功能,揭示了二聚体似乎用于“微调”嘌呤能信号传导。因此,腺苷和三磷酸腺苷之间的关系可能越来越密切,而不仅仅是彼此的代谢物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Dimerization of G protein-coupled purinergic receptors: increasing the diversity of purinergic receptor signal responses and receptor functions.

It is well accepted that G protein-coupled receptors (GPCRs) arrange into dimers or higher-order oligomers that may modify various functions of GPCRs. GPCR-type purinergic receptors (i.e. adenosine and P2Y receptors) tend to form heterodimers with GPCRs not only of the different families but also of the same purinergic receptor families, leading to alterations in functional properties. In the present review, we focus on current knowledge of the formation of heterodimers between metabotropic purinergic receptors that activate novel functions in response to extracellular nucleosides/nucleotides, revealing that the dimerization seems to be employed for 'fine-tuning' of purinergic signaling. Thus, the relationship between adenosine and adenosine triphosphate is likely to be more and more intimate than simply being a metabolite of the other.

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