Receptor (norepinephrine), P-site (2',5'-dideoxyadenosine), and calcium-mediated inhibition of prostaglandin and forskolin-activated cyclic AMP-generating systems in human platelets.

A M Siegl, J W Daly
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Abstract

Prostaglandin D2, 2-chloroadenosine, forskolin and combinations of these agents increase cyclic AMP-levels in intact human platelets. The inhibition of activated cyclic AMP-generating systems by 1) alpha2-adrenergic receptor-mediated hormonal input (norepinephrine), 2) a P-site agent (2',5'-dideoxyadenosine) and 3) a divalent cation (calcium) were examined: 1) Norepinephrine produces non-competitive inhibition of both forskolin and prostaglandin D2(PGD2)-stimulated cyclic AMP-accumulation in intact human platelets. The Ki values for norepinephrine versus forskolin, PGD2 and 2-chloroadenosine are similar in magnitude, while the Ki versus a forskolin-PGD2 combination is approximately 10-fold greater. Onset of inhibition by norepinephrine of the PGD2-response is several fold faster than for the forskolin-response. When platelets stimulated by the forskolin and PGD2 combination are exposed to norepinephrine, there is a transient increase in levels of cyclic AMP due to the potentiation of a minor beta-adrenergic component. This stimulation is followed by inhibition. 2) 2',5'-Dideoxyadenosine produces a non-competitive inhibition of the forskolin-response with a Ki of 110 microM. The inhibition of the PGD2-response by 2',5'-dideoxyadenosine is competitive with a Ki of 6-13 microM, while inhibition of the forskolin-PGD2 response has a Ki of 30 microM. Onset of inhibition by 2',5'-dideoxyadenosine is identical for forskolin or PGD2-stimulated platelets. There is a lag period for inhibition of platelets stimulated with the forskolin-PGD2 combination. The PGD2-forskolin combination appears to stabilize the cyclic AMP-generating system of platelets against inhibition by either norepinephrine or 2',5'-dideoxyadenosine. 3) Calcium ions cause a similar inhibition of cyclic AMP-generation in intact platelets, regardless of the type of stimulation.

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受体(去甲肾上腺素),p位点(2',5'-二脱氧腺苷)和钙介导的抑制前列腺素和福斯克林激活的血小板环amp生成系统。
前列腺素D2, 2-氯腺苷,福斯克林和这些药物的组合增加环amp水平在完整的人血小板。1) α 2-肾上腺素能受体介导的激素输入(去甲肾上腺素),2)p位点剂(2',5'-二脱氧腺苷)和3)二价阳离子(钙)对活化的环状amp生成系统的抑制作用进行了研究:1)去甲肾上腺素对完整人血小板中福斯克林和前列腺素D2(PGD2)刺激的环状amp积累产生非竞争性抑制。去甲肾上腺素与福斯克林、PGD2和2-氯腺苷的Ki值在量级上相似,而与福斯克林-PGD2组合相比,Ki值大约高出10倍。去甲肾上腺素对pgd2反应的抑制作用比福斯克林反应快几倍。当受福斯克林和PGD2联合刺激的血小板暴露于去甲肾上腺素时,由于一种次要的-肾上腺素能成分的增强,环AMP的水平会短暂增加。这种刺激之后是抑制。2) 2',5'-二脱氧腺苷对福斯克林反应产生非竞争性抑制,Ki为110微米。2',5'-二脱氧腺苷对pgd2反应的抑制是竞争性的,Ki为6-13微米,而对forskolin-PGD2反应的抑制Ki为30微米。2',5'-二脱氧腺苷对福斯克林或pgd2刺激的血小板的抑制作用相同。forskolin-PGD2联合刺激的血小板抑制有一个滞后期。PGD2-forskolin组合似乎可以稳定血小板的循环amp生成系统,使其免受去甲肾上腺素或2',5'-二脱氧腺苷的抑制。3)无论刺激类型如何,钙离子对完整血小板循环amp生成的抑制作用相似。
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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