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氟西汀治疗偏头痛患者期间血小板功能及血血清素水平的变化。

Changes in platelet function and blood serotonin level in migraine patients during treatment with femoxetine.

作者信息

Dalsgaard-Nielsen J, le Fèvre Honoré P, Zeeberg I

出版信息

Acta Neurol Scand. 1982 Aug;66(2):191-8. doi: 10.1111/j.1600-0404.1982.tb04516.x.

Abstract

Reports have indicated that patients with migraine have abnormalities in platelet function and in the metabolism of vasoactive monoamines. On the basis of these findings, a number of compounds with a stabilizing effect on the level of free vasoactive monoamines in plasma or with anti-platelet effects have been evaluated with regard to their prophylactic effect in migraine. Femoxetine, a new phenylpiperidine derivative and a potent selective serotonin uptake inhibitor, has been suggested as a useful prophylactic drug in migraine. The present studies were designed to evaluate platelet function and blood serotonin levels in patients with migraine before and during femoxetine treatment. During the treatment of 11 patients with migraine with 300 mg femoxetine daily, blood serotonin decreased from 0.17 +/- 0.06 microgram/ml (mean +/- SD) to 0.06 +/- 0.02 microgram/ml. In 8 patients treated with 300 mg femoxetine daily for 12 weeks, 14C-serotonin uptake into platelets in vitro was reduced significantly. Unlike most drugs used in migraine prophylaxis, femoxetine did not influence platelet aggregation in vitro. The demonstration of a certain prophylactic effect of femoxetine in some patients lends support to theories of a serotonin involvement in the pathogenesis of migraine. It does not, however, exclude the possibility of a platelet abnormality as the primary cause of migraine. A hypothesis combining the 2 theories is put forward.

摘要

有报告指出,偏头痛患者存在血小板功能及血管活性单胺代谢异常。基于这些发现,已对一些对血浆中游离血管活性单胺水平有稳定作用或具有抗血小板作用的化合物在偏头痛预防方面的效果进行了评估。非莫西汀是一种新型苯基哌啶衍生物,也是一种强效选择性5-羟色胺摄取抑制剂,已被认为是一种有效的偏头痛预防药物。本研究旨在评估偏头痛患者在接受非莫西汀治疗前及治疗期间的血小板功能和血液5-羟色胺水平。在11例偏头痛患者每日服用300mg非莫西汀的治疗过程中,血液5-羟色胺水平从0.17±0.06微克/毫升(均值±标准差)降至0.06±0.02微克/毫升。在8例每日服用300mg非莫西汀、为期12周的患者中,体外14C-5-羟色胺摄取到血小板中的量显著减少。与大多数用于偏头痛预防的药物不同,非莫西汀在体外不影响血小板聚集。非莫西汀在一些患者中显示出一定的预防作用,这支持了5-羟色胺参与偏头痛发病机制的理论。然而,这并不排除血小板异常是偏头痛主要病因的可能性。提出了一个将这两种理论结合起来的假说。

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