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儿童的工作记忆负荷对多巴胺转运体基因型的神经反应不同。

Neural response to working memory load varies by dopamine transporter genotype in children.

机构信息

Department of Psychology, Georgetown University, Washington, DC, USA.

出版信息

Neuroimage. 2010 Nov 15;53(3):970-7. doi: 10.1016/j.neuroimage.2009.12.104. Epub 2010 Jan 4.

Abstract

Inheriting two (10/10) relative to one (9/10) copy of the 10-repeat allele of the dopamine transporter genotype (DAT1) is associated with Attention Deficit Hyperactivity Disorder, a childhood disorder marked by poor executive function. We examined whether functional anatomy underlying working memory, a component process of executive function, differed by DAT1 in 7-12 year-old typically developing children. 10/10 and 9/10 carriers performed a verbal n-back task in two functional magnetic resonance imaging (fMRI) runs varying in working memory load, high (2-back vs. 1-back) and low (1-back vs. 0-back). Performance accuracy was superior in 9/10 than 10/10 carriers in the high but not low load runs. Examination of each run separately revealed that frontal-striatal-parietal regions were more activated in 9/10 than 10/10 carriers in the high load run; the groups did not differ in the low load run. Examination of load effects revealed a DAT1xLoad interaction in the right hemisphere in the caudate, our a priori region of interest. Exploratory analysis at a more liberal threshold revealed this interaction in other basal ganglia regions (putamen, and substantial nigra/subthalamic nuclei - SN/STN) and in medial parietal cortex (left precuneus). The striatal and parietal regions were more activated in 9/10 carriers under high than low load, and DAT1 differences (9/10>10/10) were evident only under high load. In contrast, SN/STN tended to be more activated in 10/10 carriers under low than high load and DAT1 differences (10/10>9/10) were evident only under low load. Thus, 10-repeat homozygosity of DAT1 was associated with reduced performance and a lack of increased basal ganglia involvement under higher working memory demands.

摘要

携带两个(10/10)拷贝的多巴胺转运体基因型(DAT1)10 重复等位基因与注意力缺陷多动障碍有关,这是一种以执行功能差为特征的儿童期疾病。我们研究了在 7-12 岁发育正常的儿童中,工作记忆(执行功能的一个组成部分)的功能解剖结构是否因 DAT1 而不同。10/10 和 9/10 携带者在两个功能磁共振成像(fMRI)运行中执行言语 n 回任务,这两个运行的工作记忆负荷不同,高(2 回比 1 回)和低(1 回比 0 回)。在高负荷运行中,9/10 携带者的表现准确性优于 10/10 携带者,但在低负荷运行中则不然。分别检查每个运行发现,在高负荷运行中,9/10 携带者比 10/10 携带者激活了更多的额-纹状体-顶叶区域;在低负荷运行中,两组没有差异。检查负荷效应发现,在右半球尾状核中存在 DAT1xLoad 相互作用,这是我们的预先确定的感兴趣区域。在更宽松的阈值下进行的探索性分析表明,这种相互作用存在于其他基底神经节区域(壳核和黑质/丘脑下核-SN/STN)和内侧顶叶皮层(左楔前叶)中。在高负荷下,9/10 携带者的纹状体和顶叶区域比低负荷下更活跃,而且只有在高负荷下才会出现 DAT1 差异(9/10>10/10)。相比之下,在低负荷下,SN/STN 倾向于在 10/10 携带者中更活跃,而且只有在低负荷下才会出现 DAT1 差异(10/10>9/10)。因此,DAT1 的 10 重复纯合子与较高工作记忆需求下的表现下降和基底神经节参与不足有关。

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