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首页> 外文期刊>Journal of clinical psychopharmacology >Rapid Antidepressant Response After Nocturnal TRH Administration in Patients With Bipolar Type I and Bipolar Type II Major Depression.
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Rapid Antidepressant Response After Nocturnal TRH Administration in Patients With Bipolar Type I and Bipolar Type II Major Depression.

机译:患有双相I型和双相II型严重抑郁症的患者夜间服用TRH后的快速抗抑郁反应。

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摘要

BACKGROUND:: Thyrotropin-releasing hormone (TRH) is a tripeptide that produces endocrine and behavioral effects in animals and humans. Some studies have shown transient antidepressant activity after morning administration of TRH. We hypothesized that nocturnal administration of TRH, when the circadian sensitivity of the TRH receptor is at its peak, may result in a more robust antidepressant effect. METHODS:: Twenty patients with bipolar (BP) type I or BP type II major depressive episode (MDE) were given nocturnal intravenous TRH 500 mug (n = 10) or saline (n = 10) at midnight in a randomized, double-blind fashion. Antidepressant activity was assessed using the Hamilton Depression Rating (HAM-D), Young Mania Rating (YMR), and Profile of Mood (POMS) scales over a 48-hour period. Thyrotropin (TSH), total T4, and free T3 concentrations were measured before and after TRH administration. Data were analyzed using chi test, Fisher exact test, and repeated-measures ANOVA. RESULTS:: Sixty percent of the TRH group and 10% of the saline group showed a >/=50% reduction in baseline total HAM-D score within 24 hours (P = 0.03). HAM-D ratings fell by an average of 52% after TRH administration versus 12% after saline administration (P = 0.038). There was a modest increase in YMR scores after TRH compared with saline (P < 0.032). No manic or hypomanic episodes were observed. Antidepressant effects of TRH lasted up to 48 hours. There was no correlation between DeltaTSH, DeltaT4, or DeltaT3 measures after TRH (or saline) administration and the change in HAM-D scores. CONCLUSIONS:: Nocturnal TRH administration may produce a rapid antidepressant effect in some patients with BP I and BP II MDE.
机译:背景:促甲状腺激素释放激素(TRH)是一种三肽,可在动物和人类中产生内分泌和行为作用。一些研究表明早晨服用TRH后有短暂的抗抑郁活性。我们假设当TRH受体的昼夜节律敏感性达到峰值时,夜间给予TRH可能会产生更强大的抗抑郁作用。方法:20名I型或BP型双相情感障碍严重抑郁发作(MDE)的患者在午夜时分随机双盲接受夜间静脉TRH 500杯(n = 10)或生理盐水(n = 10)。时尚。在48小时内,使用汉密尔顿抑郁等级(HAM-D),年轻躁狂等级(YMR)和情绪曲线(POMS)量表评估抗抑郁药的活性。在施用TRH之前和之后测量促甲状腺素(TSH),总T4和游离T3浓度。使用卡氏检验,费舍尔精确检验和重复测量方差分析对数据进行分析。结果:TRH组的60%和生理盐水组的10%在24小时内基线HAM-D基线总评分降低> / = 50%(P = 0.03)。给予TRH后的HAM-D评分平均下降了52%,而给予盐水后为12%(P = 0.038)。与盐水相比,TRH后的YMR评分有适度增加(P <0.032)。未观察到躁狂或躁狂发作。 TRH的抗抑郁作用持续长达48小时。在施用TRH(或生理盐水)后,DeltaTSH,DeltaT4或DeltaT3测量值与HAM-D得分的变化之间没有相关性。结论:夜间服用TRH可能对某些BP I和BP II MDE患者产生快速的抗抑郁作用。

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