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与未接受过5-羟色胺摄取抑制剂治疗的抑郁症患者血小板结合的[3H]-丙咪嗪的最大结合量降低。

Reduced Bmax of [3H]-imipramine binding to platelets of depressed patients free of previous medication with 5HT uptake inhibitors.

作者信息

Poirier M F, Benkelfat C, Loo H, Sechter D, Zarifian E, Galzin A M, Langer S Z

出版信息

Psychopharmacology (Berl). 1986;89(4):456-61. doi: 10.1007/BF02412121.

Abstract

The high-affinity binding sites for [3H]-imipramine (IMI) present in human platelets are associated with the neuronal uptake system for 5HT. It was recently demonstrated that previous antidepressant therapy with drugs which inhibit 5HT uptake could down-regulate [3H]-IMI binding and that this effect could persist up to 1 month after the end of treatment. We therefore re-examined the reported differences in Bmax of [3H]-IMI binding in platelets between control and depressed untreated patients, to evaluate the residual influence of previous antidepressant medication. The saturation characteristics of [3H]-IMI binding were compared in platelets from 17 depressed patients carefully selected according to previous antidepressant therapy and washout period, who were closely matched, for age and sex, with a group of control healthy volunteers. The results reveal a significant decrease by 47% in the Bmax of [3H]-IMI binding in platelets of untreated depressed patients when compared with controls. There was no significant modification of Kd values for platelet [3H]-IMI binding between the depressed and the control groups. Our results support the view that platelet [3H]-IMI binding is a useful tool as a biological marker in depression.

摘要

人血小板中存在的[3H] - 丙咪嗪(IMI)高亲和力结合位点与5-羟色胺(5HT)的神经元摄取系统相关。最近有研究表明,先前使用抑制5HT摄取的药物进行抗抑郁治疗可使[3H] - IMI结合下调,且这种效应在治疗结束后可持续长达1个月。因此,我们重新审视了已报道的未治疗的对照患者和抑郁症患者血小板中[3H] - IMI结合的最大结合量(Bmax)差异,以评估先前抗抑郁药物治疗的残留影响。我们比较了17名根据先前抗抑郁治疗和洗脱期精心挑选的抑郁症患者血小板中[3H] - IMI结合的饱和特性,这些患者在年龄和性别上与一组对照健康志愿者密切匹配。结果显示,与对照组相比,未治疗的抑郁症患者血小板中[3H] - IMI结合的Bmax显著降低了47%。抑郁症组和对照组之间血小板[3H] - IMI结合的解离常数(Kd)值没有显著变化。我们的结果支持这样一种观点,即血小板[3H] - IMI结合作为抑郁症的生物标志物是一种有用的工具。

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