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Dopamine multilocus genetic profiles predict sex differences in reactivity of the human reward system

机译:多巴胺多层遗传型材预测人类奖励系统的反应性的性别差异

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Sex differences in the neural processing of decision-making are of high interest as they may have pronounced effects on reward- and addiction-related processes. In these, the neurotransmitter dopamine plays a central role by modulating the responsiveness of the reward circuitry. The present functional magnetic resonance imaging study aimed to explore sex and dopamine transmission interactions in decision-making. 172 subjects (111 women) performed a behavioral self-control task assessing reward-related activation during acceptance and rejection of conditioned rewards. Participants were genotyped for six key genetic polymorphisms in the dopamine system that have previously been associated with individual differences in reward sensitivity or dopaminergic transmission in the human striatum, such as rs7118900 (dopamine receptor D2 (DRD2) Taq1A), rs1554929 (DRD2 C957T), rs907094 (DARPP-32), rs12364283 (DRD2), rs6278 (DRD2), and rs107656 (DRD2). The selected polymorphisms were combined in a so-called multilocus genetic composite (MGC) score reflecting the additive effect of different alleles conferring relative increased dopamine transmission in every individual. We successfully demonstrated that reward-related activation in the ventral striatum and ventral tegmental area (VTA) was significantly modulated by biologically informed MGC profiles and sex. When comparing men and women with low MGC profiles that may indicate lower dopamine transmission, only women displayed a reduced down-regulation of activation in the mesolimbic system during reward rejection and additionally, a significant non-linear u-shape relationship between MGC score and VTA activation. Taken together, by integrating neuroimaging and genetics, the present findings contribute to a better understanding of the effects of sex differences on the human brain.
机译:决策神经处理的性别差异是高兴趣,因为它们可能对奖励和成瘾相关的流程有关的影响。在这些中,神经递质多巴胺通过调制奖励电路的响应性而起到核心作用。目前的功能性磁共振成像研究旨在探讨决策中的性别和多巴胺传输相互作用。 172名科目(111名妇女)在接受和拒绝条件奖励期间进行了行为自我控制任务评估奖励相关的激活。参与者对多巴胺系统中的六种关键遗传多态性进行了基因分型,其先前已经与人体纹状体中的奖励敏感性或多巴胺能传播中的个体差异相关,例如RS7118900(多巴胺受体D2(DRD2)Taq1a),Rs1554929(DRD2 C957T), RS907094(DARPP-32),RS12364283(DRD2),RS6278(DRD2)和RS107656(DRD2)。将所选择的多态性组合在所谓的多体块遗传复合物(MGC)评分中,反映不同等位基因赋予相对增加的多巴胺传播的不同等位基因的添加剂。我们成功证明,通过生物信息的MGC型材和性别,腹侧纹状体和腹侧特区(VTA)中的奖励相关激活显着调节。在将男性和女性与低MGC型材进行比较时,可能表明多巴胺传播的低MGC型材,只有女性在奖励抑制期间均显示在培制抑制中的培养基系统中激活的降低调节,另外,MGC得分和VTA之间的显着非线性U形关系激活。通过整合神经影像动物和遗传学,目前的研究结果有助于更好地了解性别差异对人类脑的影响。

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