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Insights into ligand pharmacology using receptor-G-protein fusion proteins.

机译:使用受体-G-蛋白融合蛋白深入了解配体药理学。

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摘要

Production of chimeric DNAs in which the 5' end of G-protein alpha-subunits are linked directly to the 3' tail of a G-protein-coupled receptor has recently offered an unusual strategy to explore the detailed pharmacology of receptor-G-protein interactions. Expression of such fusion proteins ensures a 1:1 stoichiometry of receptor and G-protein expression and their proximity to each other. The capacity of such fusion proteins to be regarded as agonist-activated GTPases that allow simple enzyme kinetics to be applied to issues of ligand efficacy will be considered. In addition, the effects of point mutations, in both receptors and G proteins, on ligand function are particularly amenable to the types of robust quantitative analyses that can be produced using such fusion proteins.
机译:最近,G蛋白α亚基的5'末端直接与G蛋白偶联受体的3'尾连接的嵌合DNA的生产提供了一种不寻常的策略来探索受体G蛋白的详细药理作用互动。此类融合蛋白的表达可确保受体和G蛋白表达的化学计量比为1:1,以及它们彼此之间的接近度。将考虑将这种融合蛋白视为能够将简单的酶动力学应用于配体功效问题的激动剂激活的GTPases的能力。另外,受体和G蛋白中的点突变对配体功能的影响特别适合于使用此类融合蛋白可以产生的可靠的定量分析类型。

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