首页> 美国卫生研究院文献>Wiley-Blackwell Online Open >The Analgesic Effect of Oxytocin in Humans: A Double‐Blind Placebo‐Controlled Cross‐Over Study Using Laser‐Evoked Potentials
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The Analgesic Effect of Oxytocin in Humans: A Double‐Blind Placebo‐Controlled Cross‐Over Study Using Laser‐Evoked Potentials

机译:催产素对人的镇痛作用:使用激光诱发电位的双盲安慰剂对照交叉研究

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摘要

Oxytocin is a neuropeptide regulating social‐affiliative and reproductive behaviour in mammals. Despite robust preclinical evidence for the antinociceptive effects and mechanisms of action of exogenous oxytocin, human studies have produced mixed results regarding the analgesic role of oxytocin and are yet to show a specific modulation of neural processes involved in pain perception. In the present study, we investigated the analgesic effects of 40 IU of intranasal oxytocin in 13 healthy male volunteers using a double‐blind, placebo‐controlled, cross‐over design and brief radiant heat pulses generated by an infrared laser that selectively activate Aδ‐ and C‐fibre nerve endings in the epidermis, at the same time as recording the ensuing laser‐evoked potentials (LEPs). We predicted that oxytocin would reduce subjective pain ratings and attenuate the amplitude of the N1, N2 and P2 components. We observed that oxytocin attenuated perceived pain intensity and the local peak amplitude of the N1 and N2 (but not of P2) LEPs, and increased the latency of the N2 component. Importantly, for the first time, the present study reports an association between the analgesic effect of oxytocin (reduction in subjective pain ratings) and the oxytocin‐induced modulation of cortical activity after noxious stimulation (attenuation of the N2 LEP). These effects indicate that oxytocin modulates neural processes contributing to pain perception. The present study reports preliminary evidence that is consistent with electrophysiological studies in rodents showing that oxytocin specifically modulates Aδ/C‐fibre nociceptive afferent signalling at the spinal level and provides further specificity to evidence obtained in humans indicating that oxytocin may be modulating pain experience by modulating activity in the cortical areas involved in pain processing.
机译:催产素是一种调节哺乳动物社交,生殖和生殖行为的神经肽。尽管有强有力的临床前证据表明外源催产素具有抗伤害感受作用和作用机制,但人体研究对催产素的止痛作用产生了不同的结果,并且尚未显示出与疼痛感知有关的神经过程的特定调节作用。在本研究中,我们使用双盲,安慰剂对照,交叉设计和由选择性激活Aδ-的红外激光产生的短暂辐射热脉冲,研究了40IU鼻内催产素对13名健康男性志愿者的镇痛作用。并记录表皮上的C纤维神经末梢,同时记录随后的激光诱发电位(LEP)。我们预测催产素会降低主观疼痛等级并减弱N1,N2和P2成分的振幅。我们观察到催产素减弱了N1和N2(而非P2)LEP的感知疼痛强度和局部峰值幅度,并增加了N2组件的潜伏期。重要的是,本研究首次报道了催产素的镇痛作用(主观疼痛等级的降低)与有毒刺激后催产素诱导的皮层活动调节(N2 LEP减弱)之间的关联。这些效果表明催产素调节神经过程,促进疼痛感。本研究报告的初步证据与啮齿动物的电生理研究一致,表明催产素可在脊髓水平上特异性调节Aδ/ C纤维伤害性传入信号,并进一步证实了人类获得的证据,表明催产素可能通过调节疼痛来调节疼痛经历。在涉及疼痛处理的皮质区域中的活动。

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