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首页> 外文期刊>Biological psychiatry >Kinetics and Dose Dependency of Intranasal Oxytocin Effects on Amygdala Reactivity
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Kinetics and Dose Dependency of Intranasal Oxytocin Effects on Amygdala Reactivity

机译:鼻内催产素对杏仁菌反应性的影响动力学和剂量依赖性

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摘要

Abstract Background Current neuroimaging perspectives on a variety of mental disorders emphasize dysfunction of the amygdala. The neuropeptide oxytocin (OXT), a key mediator in the regulation of social cognition and behavior, accumulates in cerebrospinal fluid after intranasal administration in macaques and humans and modulates amygdala reactivity in both species. However, the translation of neuromodulatory OXT effects to novel treatment approaches is hampered by the absence of studies defining the most effective dose and dose–response latency for targeting the amygdala. Methods To address this highly relevant issue, a total of 116 healthy men underwent functional magnetic resonance imaging using a randomized, double-blind, placebo-controlled crossover study design. The experimental rationale was to systematically vary dose–test latencies (15–40, 45–70, and 75–100 minutes) and doses of OXT (12, 24, and 48 international units) in order to identify the most robust effects on amygdala reactivity. During functional magnetic resonance imaging, subjects completed an emotional face recognition task including stimuli with varying intensities ranging from low (highly ambiguous) to high (less ambiguous). Results Our results indicate that the OXT-induced inhibition of amygdala responses to fear was most effective in a time window between 45 and 70 minutes after administration of a dose of 24 international units. Furthermore, the observed effect was most evident in subjects scoring high on measures of autistic-like traits. Behavioral response patterns suggest that OXT specifically reduced an emotional bias in the perception of ambiguous faces. Conclusions These findings provide initial evidence of the most effective dose and dose–test interval for future experimental or therapeutic regimens aimed at targeting amygdala functioning using intranasal OXT administration.
机译:摘要背景目前各种精神障碍的神经影像术视角强调了Amygdala的功能障碍。神经肽催产素(OXT)是社会认知和行为调控中的关键介质,在猕猴和人类鼻内给药后积累脑脊液,并在两种物种中调节Amygdala反应性。然而,由于没有研究靶向氨基达拉的最有效剂量和剂量 - 反应潜伏期,没有研究缺乏研究,使神经调节性OXT效应对新的处理方法的翻译受到阻碍。解决这一高度相关问题的方法,共有116名健康男士使用随机,双盲,安慰剂控制的交叉研究设计进行了功能磁共振成像。实验理由是系统地改变剂量 - 测试延迟(15-40,45-70和75-100分钟),以及OXT(12,24和48个国际单位)的剂量,以确定对Amygdala的最强大的影响反应性。在功能磁共振成像期间,受试者完成了一种情绪面部识别任务,包括刺激,其强度从低(高度暧昧)到高(不太模糊)。结果我们的结果表明,在给予24个国际单位剂量后45至70分钟的时间窗口中,OXT诱导的Amygdala反应对恐惧的抑制最有效。此外,观察到的效果在对自闭症样力测量的受试者中最明显。行为响应模式表明OXT在暧昧面孔的感知中明确地减少了情绪偏见。结论这些发现提供了未来实验或治疗方案最有效的剂量和剂量试验间隔的初步证据,其旨在使用鼻内OXT管理靶向Amygdala功能。

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