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D-麦角酸二乙酰胺与兔血小板的相互作用:形态变化和特异性结合。

Interaction of D-LSD with blood platelets of rabbits: shape change and specific binding.

作者信息

Laubscher A, Pletscher A, Noll H

出版信息

J Pharmacol Exp Ther. 1981 Feb;216(2):385-9.

PMID:6109775
Abstract

In blood platelets of rabbits, the shape change-inducing effect of D-lysergic acid diethylamide (D-LSD) has been compared with the D-LSD-binding. D-LSD, but not L-LSD, caused a shape change reaction (EC50 1.3 x 10(-9) M) which was inhibited by various 5-HT antagonists (methergoline and neuroleptic drugs), butaclamol showing marked stereospecificity. Strong inhibitors of 5 HT uptake were only weak in counteracting the D-LSD-induced shape change. Furthermore, D-[3H]LSD bound to platelets at a single saturable, high affinity, stereoselective site [Kd = (31.1 +/- 3.3) x 10(-9) M; Bmax = 28.9 +/- 2.7 fmols per 10(8) platelets]. This binding was strongly antagonized by D-LSD and methergoline and less by the hallucinogenic drugs, psilocin, bufotenin and N'N'-dimethyltryptamine. L-LSD an 5 HT, inhibitors of 5 HT uptake and neuroleptics, especially spiroperidol and butaclamol, had only a weak antagonistic effect. The latter showed stereospecificity. It is concluded that 1) the shape change reaction caused by D-LSD in platelets is mediated by the specific 5 HT-receptor, 2) the sites mediating the D-LSD-induced shape change reaction are not identical with those responsible for D-[3H]LSD-binding and both these sites are different from the 5 HT-transport sites and 3) with respect to D-LSD-binding sites, platelets and neurons are not exactly identical.

摘要

在兔的血小板中,已将二乙麦角酰胺(D-LSD)的形状改变诱导效应与D-LSD结合情况进行了比较。D-LSD而非L-LSD引起了形状改变反应(半数有效浓度为1.3×10⁻⁹ M),该反应受到多种5-羟色胺拮抗剂(美西麦角和抗精神病药物)的抑制,布他拉莫表现出明显的立体特异性。5-羟色胺摄取的强抑制剂在对抗D-LSD诱导的形状改变方面作用较弱。此外,D-[³H]LSD以单一的可饱和、高亲和力、立体选择性位点与血小板结合[解离常数 = (31.1 ± 3.3)×10⁻⁹ M;最大结合量 = 每10⁸个血小板28.9 ± 2.7飞摩尔]。这种结合受到D-LSD和美西麦角强烈拮抗,而致幻药物、裸盖菇素、蟾蜍色胺和N,N'-二甲基色胺的拮抗作用较弱。L-LSD以及5-羟色胺、5-羟色胺摄取抑制剂和抗精神病药物,尤其是螺哌啶醇和布他拉莫,只有较弱的拮抗作用。后者表现出立体特异性。得出的结论是:1)D-LSD在血小板中引起的形状改变反应是由特异性5-羟色胺受体介导的;2)介导D-LSD诱导的形状改变反应的位点与负责D-[³H]LSD结合的位点不同,且这两个位点均与5-羟色胺转运位点不同;3)就D-LSD结合位点而言,血小板和神经元并不完全相同。

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