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面部模仿不受多巴胺 D2/3 和阿片受体拮抗剂的调节。

Facial mimicry is not modulated by dopamine D2/3 and opioid receptor antagonism.

机构信息

Department of Psychology, University of Essex, Essex, UK.

Department of Cognition, Emotion, and Methods in Psychology, University of Vienna, Vienna, Austria.

出版信息

Psychopharmacology (Berl). 2023 Oct;240(10):2081-2091. doi: 10.1007/s00213-023-06426-3. Epub 2023 Jul 21.

Abstract

RATIONALE

According to theories of embodied cognition, facial mimicry - the spontaneous, low-intensity imitation of a perceived emotional facial expression - is first an automatic motor response, whose accompanying proprioceptive feedback contributes to emotion recognition. Alternative theoretical accounts, however, view facial mimicry as an emotional response to a rewarding stimulus, and/or an affiliative signal, and thus reject the view of an automatic motor copy.

OBJECTIVES

To contribute to this debate and further investigate the neural basis of facial mimicry, as well as its relation to reward processing, we measured facial reactions to dynamic happy and angry faces after pharmacologically manipulating the opioid and dopamine systems - respectively, thought to subserve 'liking' and 'wanting' of rewards.

METHODS

In a placebo-controlled, double-blind experiment, 130 volunteers received in a between-subjects design 50 mg of the opioidergic antagonist naltrexone, 400 mg of the dopaminergic antagonist amisulpride, or placebo.

RESULTS

Clear occurrence of facial mimicry, measured 4 h after drug intake with electromyography (EMG) of the zygomaticus major and corrugator supercilii muscles, was found. However, facial mimicry was not affected by either compound, as shown with both frequentist statistics, and a Bayesian asymptotic regression model.

CONCLUSIONS

This null finding does not support the hypothesis that facial mimicry (of happiness) reflects an emotional response to a rewarding stimulus, leaving open the possibility of facial mimicry being an automatic motor copy. The results are relevant to the discussion about the psychological nature and the neural basis of facial mimicry, although they should be considered preliminary, given the challenges of interpreting null findings when targeting a novel effect of unknown size.

摘要

理论依据

根据具身认知理论,面部模仿——自发的、低强度的感知情绪面部表情模仿——首先是一种自动的运动反应,其伴随的本体感受反馈有助于情绪识别。然而,替代的理论解释将面部模仿视为对奖励刺激的情绪反应,和/或一种亲和信号,因此拒绝自动运动复制的观点。

目的

为了促进这一辩论,并进一步研究面部模仿的神经基础,以及它与奖励处理的关系,我们在药物干预阿片和多巴胺系统后测量了对动态快乐和愤怒面孔的面部反应——分别被认为是奖励的“喜欢”和“想要”的基础。

方法

在一项安慰剂对照、双盲实验中,130 名志愿者以被试间设计接受了 50 毫克阿片受体拮抗剂纳曲酮、400 毫克多巴胺受体拮抗剂氨磺必利或安慰剂。

结果

在药物摄入后 4 小时,通过颧大肌和皱眉肌的肌电图(EMG)测量到明显的面部模仿发生。然而,无论是哪种化合物都没有影响面部模仿,这通过频率统计和贝叶斯渐近回归模型都得到了证明。

结论

这一零发现不支持面部模仿(快乐)反映对奖励刺激的情绪反应的假设,这使得面部模仿成为一种自动运动复制的可能性仍然存在。虽然考虑到针对未知大小的新型效应解释零发现的挑战,这些结果是相关的,但由于它们是初步的,因此应该被认为是初步的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e9e6/10506945/6c272d4a959f/213_2023_6426_Fig1_HTML.jpg

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