Variations of the µ-opioid receptor gene OPRM1 have been shown to modulate pain perception with some evidence pointing towards a modulation of not only physical but also "psychological pain". In line with suggestions of a common neural network involved in the processing of physical pain and negative and distressing stimuli, like social rejection as a psychologically harmful event, we examined the influence of the A118G polymorphism on the neural processing of physical and non-physical pain. Using fMRI, we investigated a sample of 23 females with the more frequent AA genotype, and eight females with the relatively rare but more pain-sensitive AG genotype during electrical stimulation to the dorsum of the non-dominant hand. Non-physical pain was investigated using Cyberball, a virtual ball-tossing game, to induce experiences of non-self-dependent social rejection. A Go/NoGo task with an increased risk of self-dependent erroneous performance was used as a control task to investigate the effects of negative feedback as a more cognitive form of distress. Relative to A118G homozygous A-allele carriers, G-allele carriers showed significantly increased activation of the supplementary motor area/superior frontal gyrus and the precentral gyrus during electrical stimulation. Increased activation of the secondary sensorimotor cortex (SII) was found during social exclusion and during negative feedback. We demonstrate that brain regions particularly related to the somatosensory component of pain processing are modulated by variations in OPRM1. Influences were evident for both physical and psychological pain processing supporting the assumption of shared neural pathways.

译文

:μ阿片受体基因OPRM1的变化已显示出可调节疼痛感,一些证据表明不仅对生理上的而且对“心理上的疼痛”也有调节作用。根据涉及处理身体疼痛以及负面和令人沮丧的刺激的常见神经网络的建议(例如社会排斥是一种对心理有害的事件),我们研究了A118G多态性对身体和非身体疼痛的神经处理的影响。使用fMRI,我们在电刺激非优势手背的过程中调查了23位AA基因型频率更高的女性和8位相对罕见但对疼痛敏感的AG基因型的女性。使用虚拟投球游戏Cyber​​ball调查了非身体上的疼痛,以引发非自立型社会排斥的经历。自我控制错误行为风险增加的Go / NoGo任务被用作控制任务,以调查负反馈作为一种更痛苦的认知形式的影响。相对于A118G纯合的A等位基因携带者,G等位基因携带者在电刺激过程中显示补充运动区/上额回和中央前回的激活显着增加。在社交排斥和负反馈过程中,发现次级感觉运动皮层(SII)的激活增加。我们证明,与疼痛处理的体感成分特别相关的大脑区域受到OPRM1变异的调节。生理和心理疼痛处理的影响均很明显,这支持了共享神经通路的假设。

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