鼻内催产素在儿科人群中的应用:探索减少易怒和调节神经反应的潜力:一个小型综述。

Journal of psychiatry and brain science Pub Date : 2023-01-01 Epub Date: 2023-08-31 DOI:10.20900/jpbs.20230008
Kennet Sorenson, Emilee Kendall, Hannah Grell, Minjoo Kang, Christopher Shaffer, Soonjo Hwang
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引用次数: 0

摘要

内源性神经肽催产素(OXT)在调节亲社会行为和对社会/情绪刺激的神经反应中起重要作用。鼻内给药是最常用的给药方法。鼻内OXT已用于各种精神疾病的临床研究,但结果好坏参半,主要与缺乏可靠的药效学和药代动力学模型有关。由于鼻内OXT的机制降低了涉及情绪反应和情绪调节的神经区域的激活,因此具有这种目标机制的精神病理学可能是未来临床试验的潜在优秀候选人。在这方面,青少年的易怒可能是鼻内OXT临床研究的一个非常有希望的目标。在这里,我们提供了15个随机对照试验的小回顾,这些试验是在诊断为自闭症谱系障碍(ASD), Prader-Willi综合征(PWS)或Phelan-McDermid综合征(PMS)的儿科患者中进行的。大多数研究样本量小,剂量不同,易怒的变化,主要是不良事件(ae)。神经影像学结果显示,鼻内给药可调节奖励处理系统和涉及社会情绪信息处理的神经区域。需要进一步的研究来确定OXT治疗的最有效剂量和持续时间,仔细选择目标精神病理,验证目标参与,并测量不良事件概况。
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Intranasal Oxytocin in Pediatric Populations: Exploring the Potential for Reducing Irritability and Modulating Neural Responses: A Mini Review.

Endogenous neuropeptide Oxytocin (OXT) plays a crucial role in modulating pro-social behavior and the neural response to social/emotional stimuli. Intranasal administration is the most common method of delivering OXT. Intranasal OXT has been implemented in clinical studies of various psychiatric disorders with mixed results, mainly related to lack of solid pharmacodynamics and pharmacokinetics model. Due to intranasal OXT's mechanism of reducing the activation of neural areas implicated in emotional responding and emotion regulation, a psychopathology with this target mechanism could be potentially excellent candidate for future clinical trial. In this regard, irritability in youth may be a very promising target for clinical studies of intranasal OXT. Here we provide a mini-review of fifteen randomized controlled trials in pediatric patients with diagnoses of autism spectrum disorder (ASD), Prader-Willi syndrome (PWS), or Phelan-McDermid syndrome (PMS). Most studies had small sample sizes and varying dosages, with changes in irritability, mainly as adverse events (AEs). Neuroimaging results showed modulation of the reward processing system and the neural areas implicated in social-emotional information processing by intranasal OXT administration. Further research is needed to determine the most effective dose and duration of OXT treatment, carefully select target psychopathologies, verify target engagement, and measure adverse event profiles.

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