Reward system neurodynamics during menstrual pain modulated by COMT Val158Met polymorphisms

IF 3.5 3区 医学 Q2 NEUROSCIENCES Frontiers in Molecular Neuroscience Pub Date : 2024-09-03 DOI:10.3389/fnmol.2024.1457602
Pei-Shan Hsu, Ching-Hsiung Liu, Ching-Ju Yang, Lin-Chien Lee, Wei-Chi Li, Hsiang-Tai Chao, Ming-Wei Lin, Li-Fen Chen, Jen-Chuen Hsieh
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Abstract

IntroductionPrimary dysmenorrhea (PDM), characterized by cyclic pain, may involve pain modulation within the reward system (RS). The Catechol-O-methyltransferase (COMT) Val158Met polymorphism, which significantly influences dopamine activity, is linked to the regulation of both acute and chronic pain. This study examines the differential neurodynamic modulation in the RS associated with COMT Val158Met polymorphisms during menstrual pain among PDM subjects.MethodNinety-one PDM subjects underwent resting-state fMRI during menstruation and were genotyped for COMT Val158Met polymorphisms. The amplitude of low-frequency fluctuation (ALFF) and functional connectivity (FC) analyses were used to assess the RS response. Psychological evaluations included the McGill Pain Questionnaire, Pain Catastrophizing Scale, Beck Anxiety Inventory, and Beck Depression Inventory.ResultVal/Val homozygotes (n = 50) and Met carriers (n = 41) showed no significant differences in McGill Pain Questionnaire, Beck Anxiety Inventory, and Beck Depression Inventory. However, Met carriers exhibited lower scores on the Pain Catastrophizing Scale. Distinct FC patterns was observed between Val/Val homozygotes and Met carriers, specifically between the nucleus accumbens (NAc) and prefrontal cortex, NAc and inferior parietal lobe, ventral tegmental area (VTA) and prefrontal cortex, VTA and precentral gyrus, and VTA and superior parietal lobe. Only Met carriers showed significant correlations between ALFF and FC values of the NAc and VTA with pain-related metrics (McGill Pain Questionnaire and Pain Catastrophizing Scale scores). NAc ALFF and NAc-prefrontal cortex FC values positively correlated with pain-related metrics, while VTA ALFF and VTA-prefrontal cortex and VTA-superior parietal lobe FC values negatively correlated with pain-related metrics.DiscussionThis study reveals that the COMT Val158Met polymorphism results in genotype-specific functional changes in the brain’s RS during menstrual pain. In Met carriers, engagement of these regions is potentially linked to motivational reward-seeking and top-down modulation. This polymorphism likely influences the RS’s responses, significantly contributing to individual differences in pain regulation.
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经痛时奖励系统神经动力学受 COMT Val158Met 多态性调节
导言以周期性疼痛为特征的原发性痛经(PDM)可能涉及奖赏系统(RS)内的疼痛调节。儿茶酚-O-甲基转移酶(COMT)Val158Met 多态性显著影响多巴胺的活性,与急性和慢性疼痛的调节有关。本研究探讨了 PDM 受试者在经痛期间 RS 中与 COMT Val158Met 多态性相关的不同神经动力调节。方法:91 名 PDM 受试者在月经期间接受了静息态 fMRI 检查,并对 COMT Val158Met 多态性进行了基因分型。低频波动幅度(ALFF)和功能连通性(FC)分析用于评估RS反应。心理评估包括麦吉尔疼痛问卷、疼痛灾难化量表、贝克焦虑量表和贝克抑郁量表。结果Val/Val同源基因携带者(50人)和Met基因携带者(41人)在麦吉尔疼痛问卷、贝克焦虑量表和贝克抑郁量表上无显著差异。然而,Met 携带者在疼痛灾难化量表上的得分较低。在Val/Val同源基因携带者和Met基因携带者之间观察到不同的FC模式,特别是在伏隔核(NAc)和前额叶皮层之间、NAc和下顶叶之间、腹侧被盖区(VTA)和前额叶皮层之间、VTA和前中央回之间以及VTA和上顶叶之间。只有Met携带者的NAc和VTA的ALFF和FC值与疼痛相关指标(麦吉尔疼痛问卷和疼痛灾难化量表评分)有明显相关性。NAc ALFF和NAc-前额叶皮层FC值与疼痛相关指标呈正相关,而VTA ALFF和VTA-前额叶皮层以及VTA-顶叶上部FC值与疼痛相关指标呈负相关。在 Met 携带者中,这些区域的参与可能与动机奖赏寻求和自上而下的调节有关。这种多态性可能会影响RS的反应,从而在很大程度上导致疼痛调节的个体差异。
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来源期刊
CiteScore
5.70
自引率
2.10%
发文量
669
审稿时长
14 weeks
期刊介绍: Frontiers in Molecular Neuroscience is a first-tier electronic journal devoted to identifying key molecules, as well as their functions and interactions, that underlie the structure, design and function of the brain across all levels. The scope of our journal encompasses synaptic and cellular proteins, coding and non-coding RNA, and molecular mechanisms regulating cellular and dendritic RNA translation. In recent years, a plethora of new cellular and synaptic players have been identified from reduced systems, such as neuronal cultures, but the relevance of these molecules in terms of cellular and synaptic function and plasticity in the living brain and its circuits has not been validated. The effects of spine growth and density observed using gene products identified from in vitro work are frequently not reproduced in vivo. Our journal is particularly interested in studies on genetically engineered model organisms (C. elegans, Drosophila, mouse), in which alterations in key molecules underlying cellular and synaptic function and plasticity produce defined anatomical, physiological and behavioral changes. In the mouse, genetic alterations limited to particular neural circuits (olfactory bulb, motor cortex, cortical layers, hippocampal subfields, cerebellum), preferably regulated in time and on demand, are of special interest, as they sidestep potential compensatory developmental effects.
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