Dopamine D2 receptor signaling via the arachidonic acid cascade: modulation by cAMP-dependent protein kinase A and prostaglandin E2.

Journal of lipid mediators Pub Date : 1993-03-01
D Piomelli, V Di Marzo
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Abstract

Recent studies have shown that, in Chinese hamster ovary cells transfected with D2-receptor cDNA, CHO(D2) cells, D2 agonists are potent in enhancing the release of [3H]arachidonic acid (AA) induced by stimulation of constitutive purinergic receptors or by application of Ca2+ ionophores. This facilitatory action is further amplified by the concomitant activation of D1 receptors, which per se have no effect on evoked [3H]AA release. Here, we review a series of experiments aimed at examining the molecular mechanism of this synergistic interaction. The results show that, in CHO(D2) cells: (a) application of 8-Br-cAMP or stimulation of constitutive prostaglandin (PG)E2 receptors augment the AA response produced by D2 agonists; (b) in CHO(D2) cells transfected with human beta 2-receptor cDNA, the beta-agonist, isoproterenol, produces a similar effect; (c) the potentiation of [3H]AA release produced by PGE2 and 8-Br-cAMP is prevented by overexpressing either a protein inhibitor of cAMP-dependent protein kinase (PKA) or a mutated form of pKA regulatory subunit incapable of binding cAMP; (d) mock-synergism is obtained in CHO(D2) cells overexpressing the catalytic subunit of PKA; (e) PGE2 is a major AA metabolite in stimulated CHO(D2) cells and its formation may contribute to the effect of D2 agonists on AA release. The results indicate that cAMP-induced activation of PKA represents a likely molecular basis for D1/D2 receptor synergism on AA release. They also suggest that additional membrane receptors, colocalized with D2 and positively linked to adenylyl cyclase, may exert a similar action. Furthermore, stimulation of PGE2 receptors by endogenously produced prostaglandin may participate in AA signaling at the D2 receptor, by providing a paracrine positive feedback loop.

通过花生四烯酸级联的多巴胺D2受体信号:camp依赖性蛋白激酶A和前列腺素E2的调节。
最近的研究表明,在转染了D2受体cDNA的中国仓鼠卵巢细胞中,CHO(D2)细胞、D2激动剂可以通过刺激组成型嘌呤能受体或应用Ca2+离子载体来促进[3H]花生四烯酸(AA)的释放。伴随D1受体的激活进一步放大了这种促进作用,而D1受体本身对诱发的[3H]AA释放没有影响。在这里,我们回顾了一系列旨在研究这种协同相互作用的分子机制的实验。结果表明,在CHO(D2)细胞中:(a)应用8-Br-cAMP或刺激构成型前列腺素(PG)E2受体可增强D2激动剂产生的AA反应;(b)在转染人β 2受体cDNA的CHO(D2)细胞中,β受体激动剂异丙肾上腺素产生类似的效果;(c) PGE2和8-Br-cAMP产生的[3H]AA释放的增强可以通过过表达cAMP依赖性蛋白激酶(PKA)的蛋白抑制剂或不能结合cAMP的PKA调节亚基的突变形式来阻止;(d)在过表达PKA催化亚基的CHO(D2)细胞中获得模拟协同作用;(e) PGE2是受刺激的CHO(D2)细胞中主要的AA代谢物,其形成可能有助于D2激动剂对AA释放的影响。结果表明,camp诱导的PKA活化可能是D1/D2受体协同AA释放的分子基础。他们还表明,与D2共定位并与腺苷酸环化酶正相关的其他膜受体可能发挥类似的作用。此外,内源性前列腺素刺激PGE2受体可能通过提供旁分泌正反馈回路参与D2受体的AA信号传导。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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