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育亨宾对人类听觉惊跳反射的促进作用。

Yohimbine-facilitated acoustic startle reflex in humans.

作者信息

Morgan C A, Southwick S M, Grillon C, Davis M, Krystal J H, Charney D S

机构信息

National Center for Post Traumatic Stress Disorder, Department of Veterans Affairs Medical Center, New Haven, CT 06516.

出版信息

Psychopharmacology (Berl). 1993;110(3):342-6. doi: 10.1007/BF02251291.

DOI:10.1007/BF02251291
PMID:7831429
Abstract

Preclinical studies have suggested the acoustic startle reflex (ASR) may be a useful animal model to investigate the neurochemical basis of anxiety and fear states. This work has revealed that the anxiogenic alpha-2 receptor antagonist, yohimbine, increases the amplitude of the ASR in laboratory animals. The present investigation evaluated the effects of yohimbine on the ASR in healthy subjects. Seven healthy subjects received IV yohimbine (0.4 mg/kg) or saline placebo on two separate days in a randomized double blind placebo control design. A trial of 2 tone frequencies with varied intensity (90, 96, 102, 108, 114 dB) white noise, instantaneous rise time, was delivered binaurally through headphones. Tones were delivered every 25-60 sec, for a 30 ms duration. Startle testing was done 80 minutes post infusion and lasted 15-20 minutes. Sign rank testing indicated yohimbine caused an overall increase in startle amplitude, as well as significant augmentation of startle amplitude at 96, 102, 108, 114 decibels but not at the 90 dB intensity. Sign rank tests indicated a significant reduction of startle latency by yohimbine at only the 96 dB intensity. Significant correlations were observed between startle and peak anxiety, startle and plasma MHPG, peak anxiety and plasma MHPG. This study demonstrates in healty human subjects an excitatory effect of yohimbine on the magnitude of the ASR and a decrease in its latency. In the context of the key role of this reflex in the alarm response, this finding adds to the array of documented behavioral, biochemical and cardiovascular effects of yohimbine in humans which support the relationship between increased noradrenergic function and anxiety states.

摘要

临床前研究表明,听觉惊吓反射(ASR)可能是一种用于研究焦虑和恐惧状态神经化学基础的有用动物模型。这项研究揭示,致焦虑的α-2受体拮抗剂育亨宾可增加实验动物的ASR幅度。本研究评估了育亨宾对健康受试者ASR的影响。在随机双盲安慰剂对照设计中,7名健康受试者在两个不同的日子分别接受静脉注射育亨宾(0.4mg/kg)或生理盐水安慰剂。通过耳机双耳传递2种不同强度(90、96、102、108、114分贝)的纯音、白噪声,瞬时上升时间。每间隔25 - 60秒发出一次纯音,持续30毫秒。在输注后80分钟进行惊吓测试,持续15 - 20分钟。符号秩检验表明,育亨宾使惊吓幅度总体增加,在96、102、108、114分贝时惊吓幅度显著增大,但在90分贝强度时无此现象。符号秩检验表明,育亨宾仅在96分贝强度时使惊吓潜伏期显著缩短。在惊吓与峰值焦虑、惊吓与血浆3-甲氧基-4-羟基苯乙二醇(MHPG)、峰值焦虑与血浆MHPG之间观察到显著相关性。本研究证明,在健康人类受试者中,育亨宾对ASR的幅度有兴奋作用,并使其潜伏期缩短。鉴于该反射在警报反应中的关键作用,这一发现进一步补充了育亨宾在人类中已被记录的行为、生化和心血管效应,支持了去甲肾上腺素能功能增强与焦虑状态之间的关系。

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