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乙醛缩合产物对人体血小板聚集的影响。

Effects of acetaldehyde condensation products on human platelet aggregation.

作者信息

Given M B, Longenecker G L

出版信息

Alcohol Drug Res. 1987;7(5-6):383-92.

PMID:3620006
Abstract

Condensation products (CP) of the ethanol metabolite, acetaldehyde, and endogenous amines, such as dopamine and serotonin, have been proposed to be effectors of some symptoms of chronic ethanol use. Since hemostatic defects are known to occur in chronic ethanol use, the effects of CP on in vitro human platelet aggregation responses induced by several agents were determined. Both isoquinoline and beta carboline type CP significantly inhibited aggregation responses induced by epinephrine, with the concentrations to produce 50% inhibition ranging from 8-347 uM. The beta-carbolines significantly inhibited ADP-induced aggregation and also inhibited aggregation induced by collagen or arachidonic acid, but at high concentrations. Effects on epinephrine aggregation and ADP aggregation were reversible. Potential mechanisms of the inhibitory effects were briefly examined. Concomitant use of the phosphodiesterase inhibitor theophylline potentiated the effect of some but not other CP, possibly indicating an involvement of cyclic AMP. Concomitant use of the non-specific beta-adrenergic inhibitor propranolol had no effect on CP inhibition, indicating that CP probably do not stimulate platelet adenylyl cyclase-coupled beta 2-adrenoceptors. Thus, general inhibition by CP of platelet responses in the circulation is unlikely, except, possibly, for epinephrine-induced aggregation, because of the high concentrations of CP required. However, local regulation of platelet responses by release of stored CP during aggregation is possible since CP are stored in platelet dense granules.

摘要

乙醇代谢产物乙醛与内源性胺(如多巴胺和血清素)的缩合产物(CP)被认为是慢性乙醇使用某些症状的效应物。由于已知慢性乙醇使用会出现止血缺陷,因此测定了CP对几种药物诱导的体外人血小板聚集反应的影响。异喹啉型和β-咔啉型CP均显著抑制肾上腺素诱导的聚集反应,产生50%抑制作用的浓度范围为8 - 347μM。β-咔啉显著抑制ADP诱导的聚集,也抑制胶原或花生四烯酸诱导的聚集,但需要高浓度。对肾上腺素聚集和ADP聚集的影响是可逆的。简要研究了抑制作用的潜在机制。同时使用磷酸二酯酶抑制剂茶碱可增强某些而非其他CP的作用,这可能表明环磷酸腺苷(cAMP)参与其中。同时使用非特异性β-肾上腺素能抑制剂普萘洛尔对CP的抑制作用无影响,表明CP可能不会刺激血小板腺苷酸环化酶偶联的β2-肾上腺素能受体。因此,除了可能对肾上腺素诱导的聚集外,CP不太可能对循环中的血小板反应产生普遍抑制,因为需要高浓度的CP。然而,由于CP储存在血小板致密颗粒中,在聚集过程中通过释放储存的CP对血小板反应进行局部调节是可能的。

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