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5-羟色胺1A受体探针[3H]8-羟基二丙胺基四氢萘可标记人血小板中的5-羟色胺转运体。

The 5-HT1A receptor probe [3H]8-OH-DPAT labels the 5-HT transporter in human platelets.

作者信息

Ieni J R, Meyerson L R

机构信息

Medical Research Division of American Cyanamid Company, Ramapo College, Mahwah, New Jersey 07430.

出版信息

Life Sci. 1988;42(3):311-20. doi: 10.1016/0024-3205(88)90640-6.

Abstract

The present study characterizes a serotonin (5-HT) binding site on human platelet membranes, using [3H]8-OH-DPAT as the radioligand. [3H]8-OH-DPAT binds specifically and saturably to a site on human platelet membranes with an average KD of 43 nM and Bmax of 1078 fmol/mg protein. Determinations of IC50 values for various serotonergic characterizing agents in platelets for displacement of [3H]8-OH-DPAT were performed. For example, 8-OH-DPAT 5HT1A had an IC50 of 117 nM; TFMPP 5HT1B (2.3 microM0 and PAPP 1A + 5HT2 (9 microM); ipsapirone 5HT1A (21.1 microM) and buspirone 5HT1A (greater than 100 microM); ketanserin 5HT2 (greater than 100 microM); 5-HT uptake inhibitors: paroxetine (13 nM); chlorimipramine (73 nM) and fluoxetine (653 nM). The pharmacological inhibitory profile of the platelet 8-OH-DPAT site is not consistent with profiles reported for brain. 8-OH-DPAT does not inhibit [3H]imipramine binding, however, it does inhibit [3H]5-HT uptake in human platelets near 5-HT's Km value (IC50 = 2-4 microM). These results suggest that the human platelet site labeled by [3H]8-OH-DPAT is pharmacologically different from the neuronal site and probably is a component of the 5-HT transporter.

摘要

本研究以[3H]8-羟基二丙胺为放射性配体,对人血小板膜上的5-羟色胺(5-HT)结合位点进行了表征。[3H]8-羟基二丙胺与人血小板膜上的一个位点特异性且饱和性结合,平均解离常数(KD)为43 nM,最大结合容量(Bmax)为1078 fmol/mg蛋白质。测定了多种血清素能特征性药物在血小板中取代[3H]8-羟基二丙胺的半数抑制浓度(IC50)值。例如,8-羟基二丙胺5-HT1A的IC50为117 nM;三氟甲基苯基哌嗪5-HT1B(2.3 μM)和对氨基苯磷酸1A + 5-HT2(9 μM);伊沙匹隆5-HT1A(21.1 μM)和丁螺环酮5-HT1A(大于100 μM);酮色林5-HT2(大于100 μM);5-羟色胺摄取抑制剂:帕罗西汀(13 nM);氯米帕明(73 nM)和氟西汀(653 nM)。血小板8-羟基二丙胺位点的药理学抑制特征与脑内报道的特征不一致。8-羟基二丙胺不抑制[3H]丙咪嗪结合,然而,它确实在接近5-羟色胺的米氏常数(Km)值(IC50 = 2 - 4 μM)时抑制人血小板中[3H]5-羟色胺的摄取。这些结果表明,由[3H]8-羟基二丙胺标记的人血小板位点在药理学上与神经元位点不同,可能是5-羟色胺转运体的一个组成部分。

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