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首页> 外文期刊>Journal of Cognitive Neuroscience >C957T-mediated Variation in Ligand Affinity Affects the Association between ~(11)C-raclopride Binding Potential and Cognition
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C957T-mediated Variation in Ligand Affinity Affects the Association between ~(11)C-raclopride Binding Potential and Cognition

机译:C957T介导的配体亲和力变化影响〜(11)C-雷氯必利结合电位与认知之间的关联。

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摘要

The dopamine (DA) system plays an important role in cognition. Accordingly, normal variation in DA genes has been found to predict individual differences in cognitive performance. However, little is known of the impact of genetic differences on the link between empirical indicators of the DA system and cognition in humans. The present work used PET with C-11-raclopride to assess DA D2-receptor binding potential (BP) and links to episodic memory, working memory, and perceptual speed in 179 healthy adults aged 64-68 years. Previously, the T-allele of a DA D2-receptor single-nucleotide polymorphism, C957T, was associated with increased apparent affinity of C-11-raclopride, giving rise to higher BP values despite similar receptor density values between allelic groups. Consequently, we hypothesized that C-11-raclopride BP measures inflated by affinity rather than D2-receptor density in T-allele carriers would not be predictive of DA integrity and therefore prevent finding an association between C-11-raclopride BP and cognitive performance. In accordance with previous findings, we show that C-11-raclopride BP was increased in T-homozygotes. Importantly, C-11-raclopride BP was only associated with cognitive performance in groups with low or average ligand affinity (C-allele carriers of C957T, n = 124), but not in the high-affinity group (T-homozygotes, n = 55). The strongest C-11-raclopride BP-cognition associations and the highest level of performance were found in C-homozygotes. These findings show that genetic differences modulate the link between BP and cognition and thus have important implications for the interpretation of DA assessments with PET and C-11-raclopride in multiple disciplines ranging from cognitive neuroscience to psychiatry and neurology.
机译:多巴胺(DA)系统在认知中起着重要作用。因此,已经发现DA基因的正常变异可预测认知表现的个体差异。但是,关于遗传差异对DA系统的经验指标与人类认知之间的联系的影响知之甚少。目前的工作是使用PET与C-11-raclopride来评估DA D2受体结合潜能(BP),并与179名64-68岁的健康成年人的情节记忆,工作记忆和知觉速度相关。以前,DA D2受体单核苷酸多态性C957T的T等位基因与C-11- raclopride的表观亲和力增加相关,尽管等位基因组之间的受体密度值相似,但产生了更高的BP值。因此,我们假设C-11-raclopride BP的测量值是由T-等位基因携带者的亲和力而非D2受体密度来充实的,因此不能预测DA的完整性,因此无法发现C-11-raclopride BP与认知能力之间的关联。根据以前的发现,我们显示C-11-raclopride BP在T-纯合子中增加。重要的是,C-11-raclopride BP仅与具有低或平均配体亲和力的组(C957T的C等位基因携带者,n = 124)相关,而与高亲和力组(T-纯合体,n = 55)。在C-纯合子中发现最强的C-11-raclopride BP认知关联和最高水平的表现。这些发现表明,遗传差异调节了BP与认知之间的联系,因此,对于从认知神经科学到精神病学和神经病学等多个学科的PET和C-11-raclopride的DA评估的解释具有重要意义。

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