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多巴胺D2/血管紧张素AT1嵌合受体:D2受体第三细胞内环影响受体与…
引用本文:陈泓,张幼怡.多巴胺D2/血管紧张素AT1嵌合受体:D2受体第三细胞内环影响受体与…[J].中国药理学报,1997,18(3):209-213.
作者姓名:陈泓  张幼怡
作者单位:北京医科大学第三医院血管医学研究所
摘    要:

关 键 词:多巴胺D2  血管紧张素  受体  PCR  G蛋白  偶联

Chimeric dopamine D2/angiotensin AT1 receptors: role of the length of third intracellular loop of D2 receptors in conferring specificity of receptor binding and G-protein coupling.
H Chen,Y Y Zhang,Q D Han.Chimeric dopamine D2/angiotensin AT1 receptors: role of the length of third intracellular loop of D2 receptors in conferring specificity of receptor binding and G-protein coupling.[J].Acta Pharmacologica Sinica,1997,18(3):209-213.
Authors:H Chen  Y Y Zhang  Q D Han
Institution:Institute of Vascular Medicine, Third Hospital, Beijing Medical University, China.
Abstract:AIM: To define roles of the third intracellular loop (IL3) length of G-protein coupled receptors in conferring the specificity for receptor binding and G-protein coupling. METHODS: By polymerase chain reaction (PCR), the IL3 of D2 receptor was replaced with the counter part of AT1 receptor which has the shortest loop among all G-protein coupled receptors. D2/AT1 receptor cDNA was then stably transfected into Chinese hamster ovary cells and a clone with high level expression was obtained for receptor binding and agonist-induced phosphatidylinositols (PI) turnover experiments. RESULTS: Comparing to the D2 receptor, D2/AT1 chimeric receptor had lower affinities for all D2 receptor antagonists tested (spiperone, haloperidol, (+)-butaclamol, chlopromazine, clozapine, trifluoperdazine) and different affinity profiles to agonists (apomorphine, dopamine, quinpirole, bromocriptine). But the chimeric receptor failed to couple to G-protein and subsequent stimulation of PI turnover. CONCLUSION: The length of IL3 of D2 receptor participates defining recpetor binding sites conformation, and structure beyond IL3 may affect receptor G-protein coupling.
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