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Oxytocin treatment attenuates amygdala activity in autism: a treatment-mechanism study with long-term follow-up

机译:催产素治疗衰减术中的Amygdala活性:长期随访的治疗机制研究

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Intranasal administration of the neuropeptide oxytocin (IN-OT) is increasingly considered as a potential treatment for targeting the core symptoms of autism spectrum disorder (ASD), but the effects of continual use on neural substrates are fairly unexplored and long-term effects are unknown. In this double-blind, randomized, placebo-controlled study, we investigated the effects of single-dose and multiple-dose IN-OT treatment (4 weeks of daily (24 IU) administrations) on brain activity related to processing emotional states. Thirty-eight adult men with ASD (aged between 18 and 35 years) underwent functional magnetic resonance imaging of the posterior superior temporal gyrus (pSTS) and amygdala regions while processing emotional states from point-light biological motion. In line with prior research, a single dose of IN-OT induced a reliable increase in pSTS brain activity during the processing of point-light biological motion, but no consistent long-term changes in pSTS activity were induced after the multiple-dose treatment. In terms of bilateral amygdala, the multiple-dose treatment induced a consistent attenuation in brain activity, which outlasted the period of actual administrations until four weeks and one year post-treatment. Critically, participants with stronger attenuations in amygdala-activity showed greater behavioral improvements, particularly in terms of self-reported feelings of avoidant attachment and social functioning. Together, these observations provide initial insights into the long-lasting neural consequences of chronic IN-OT use on amygdala functioning and provide first indications that the acute versus chronic effects of IN-OT administration may be qualitatively different. Larger studies are however warranted to further elucidate the long-term impact of IN-OT treatment on human neural substrates and its behavioral consequences.
机译:鼻内给予神经肽催产素(In-OT)越来越多地被认为是靶向自闭症谱系疾病(ASD)的核心症状的潜在治疗,但持续使用对神经基质的影响是相当未探明的,并且长期效应是未知的。在这种双盲,随机的安慰剂对照研究中,我们研究了单剂量和多剂量in-Ot-propedy的影响(每日4周(24个IU)施用的脑部活动与加工情绪状态相关的脑活动。三十八名成年男性亚型亚型款(18至35岁)接受后验颞血(PSTS)和Amygdala地区的功能性磁共振成像,同时加工来自点光生物运动的情绪状态。符合现有研究,在加工点光生物学运动期间,单剂量在-S-OT诱导Psts脑活动中的可靠增加,但在多剂量处理后,诱导PSTS活性的一致性长期变化。就双侧杏仁达拉而言,多剂量治疗诱导脑活动中一致的衰减,这持续了实际施用的时间,直到四周和一年的治疗后。批判性地,在Amygdala-Activity中具有更强的衰减的参与者表现出更大的行为改进,特别是在自我报告的避税依恋和社会功能方面。这些观察结果在一起提供了初步见解,对慢性急性使用的慢性In-Ot使用的长期神经后果在杏仁醛作用上提供,并提供了第一项急性对局部给药的慢性效应可以定性不同。然而,较大的研究是为了进一步阐明OT-OT治疗对人类神经基质的长期影响及其行为后果。

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