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血清素转运体基因分型对青少年杏仁核和前额叶皮质功能的年龄相关影响。

Age-related effect of serotonin transporter genotype on amygdala and prefrontal cortex function in adolescence.

作者信息

Wiggins Jillian Lee, Bedoyan Jirair K, Carrasco Melisa, Swartz Johnna R, Martin Donna M, Monk Christopher S

机构信息

Department of Psychology, University of Michigan, Ann Arbor, Michigan.

出版信息

Hum Brain Mapp. 2014 Feb;35(2):646-58. doi: 10.1002/hbm.22208. Epub 2012 Nov 5.

Abstract

The S and LG alleles of the serotonin transporter-linked polymorphic region (5-HTTLPR) lower serotonin transporter expression. These low-expressing alleles are linked to increased risk for depression and brain activation patterns found in depression (increased amygdala activation and decreased amygdala-prefrontal cortex connectivity). Paradoxically, serotonin transporter blockade relieves depression symptoms. Rodent models suggest that decreased serotonin transporter in early life produces depression that emerges in adolescence, whereas decreased serotonin transporter that occurs later in development ameliorates depression. However, no brain imaging research has yet investigated the moderating influence of human development on the link between 5-HTTLPR and effect-related brain function. We investigated the age-related effect of 5-HTTLPR on amygdala activation and amygdala-prefrontal cortex connectivity using a well-replicated probe, an emotional face task, in children and adolescents aged 9-19 years. A significant genotype-by-age interaction predicted amygdala activation, such that the low-expressing genotype (S/S and S/LG ) group showed a greater increase in amygdala activation with age compared to the higher expressing (LA /LA and S/LA ) group. Additionally, compared to the higher expressing group, the low-expressing genotype group exhibited decreased connectivity between the right amygdala and ventromedial prefrontal cortex with age. Findings indicate that low-expressing genotypes may not result in the corticolimbic profile associated with depression risk until later adolescence.

摘要

血清素转运体相关多态性区域(5-HTTLPR)的S和LG等位基因会降低血清素转运体的表达。这些低表达等位基因与抑郁症风险增加以及抑郁症中发现的大脑激活模式有关(杏仁核激活增加,杏仁核-前额叶皮层连接性降低)。矛盾的是,血清素转运体阻断可缓解抑郁症状。啮齿动物模型表明,生命早期血清素转运体减少会导致青春期出现抑郁症,而发育后期血清素转运体减少则可改善抑郁症。然而,尚无脑成像研究探讨人类发育对5-HTTLPR与效应相关脑功能之间联系的调节作用。我们使用一项经过充分验证的探测任务——情绪面孔任务,对9至19岁的儿童和青少年进行研究,以探究5-HTTLPR与年龄相关的对杏仁核激活及杏仁核-前额叶皮层连接性的影响。显著的基因型与年龄交互作用可预测杏仁核激活情况,即与高表达基因型(LA /LA 和S/LA )组相比,低表达基因型(S/S和S/LG )组的杏仁核激活随年龄增长的增幅更大。此外,与高表达组相比,低表达基因型组随着年龄增长,右侧杏仁核与腹内侧前额叶皮层之间的连接性降低。研究结果表明,低表达基因型可能直到青春期后期才会导致与抑郁症风险相关的皮质边缘特征。

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