High-affinity 3H-imipramine binding: a new biological marker in depression.

S Z Langer, E Zarifian, M Briley, R Raisman, D Sechter
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引用次数: 50

Abstract

High-affinity binding of the tricyclic antidepressant drug, 3H-imipramine, has been demonstrated in the brain of various species including man. These specific binding sites have many of the characteristics to be expected for the specific site of action of a drug and appear to be associated with the neuronal uptake mechanism for serotonin. Chronic administration of tricyclic antidepressant drugs or the prolonged application of other antidepressant therapies, such as electroshock and sleep-deprivation, resulted in decreases in the density of 3H-imipramine binding sites. Apparently identical 3H-imipramine binding sites have been found in blood platelets from a variety of species including man. Clinical studies have shown that untreated severely depressed patients have a lower density of binding sites in their platelets than control volunteers. Longitudinal studies of these patients indicate that the density of 3H-imipramine binding sites tends not to change during treatment with tricyclic antidepressant drugs and the subsequent recovery from depression. 3H-imipramine binding in brain and platelets is proposed as a new biological marker in depression and as a useful research tool in biochemical and clinical pharmacological studies in affective disorders.

高亲和力3h -丙咪嗪结合:抑郁症的新生物标志物。
三环抗抑郁药物3h -丙咪嗪的高亲和力结合已在包括人类在内的各种物种的大脑中得到证实。这些特异结合位点具有药物特异作用位点的许多特征,似乎与5 -羟色胺的神经元摄取机制有关。长期服用三环类抗抑郁药物或长期使用其他抗抑郁疗法,如电击和剥夺睡眠,会导致3h -丙咪嗪结合位点的密度降低。显然,在包括人类在内的许多物种的血小板中都发现了相同的3h -丙咪嗪结合位点。临床研究表明,未经治疗的严重抑郁症患者的血小板结合位点密度低于对照组志愿者。对这些患者的纵向研究表明,3h -丙咪嗪结合位点的密度在三环类抗抑郁药物治疗和随后的抑郁症康复期间趋于不变。3h -丙咪嗪在脑和血小板中的结合被认为是抑郁症的一种新的生物学标志物,在情感性障碍的生化和临床药理学研究中具有重要的应用价值。
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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