首页> 美国卫生研究院文献>other >Role of Variation in the Serotonin Transporter Protein Gene (SLC6A4) in Trait Disturbances in the Ventral Anterior Cingulate in Bipolar Disorder 5-HTTLPR and Ventral Anterior Cingulate in Bipolar Disorder
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Role of Variation in the Serotonin Transporter Protein Gene (SLC6A4) in Trait Disturbances in the Ventral Anterior Cingulate in Bipolar Disorder 5-HTTLPR and Ventral Anterior Cingulate in Bipolar Disorder

机译:血清素转运蛋白基因(SLC6A4)的变化在双相情感障碍5-HTTLPR的前前扣带和双相情感障碍的前扣带特质扰动中的作用

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摘要

Bipolar disorder (BD) is associated with abnormalities of the ventral anterior cingulate cortex (vACC) and its connection sites, including the amygdala, which are key components of a corticolimbic neural system that subserves emotional regulation. Decreased functional connectivity from the vACC to the amygdala in healthy individuals is associated with the short “s” allele—as opposed to the long “l” allele—of a well-known serotonin transporter promoter polymorphism (5-HTTLPR, locus SLC6A4), as are features of BD. This study tests the hypothesis that the s allele influences dysfunction in the vACC-amygdala neural system in BD. Thirty euthymic individuals with BD (20 s carriers, 10 ll) and 48 healthy comparison (HC) participants (34 s, 14 ll) participated in an event-related functional magnetic resonance imaging scan while processing fearful, happy, or neutral faces. During fear and happy face processing, vACC activation was significantly lower in the BD compared to the HC group, and in s carriers compared to ll individuals within both the HC and BD groups, such that BD s carriers exhibited the greatest magnitude of vACC dysfunction. No significant differences were detected in amygdala activation. The findings suggest that the 5-HTTLPR s allele may contribute to a trait-related, genetically-derived, neurobiological subgroup within BD characterized by prominent vACC dysfunction. Future treatment may be optimized for this BD subgroup by targeting the serotonergic system and the vACC.
机译:躁郁症(BD)与腹侧前扣带回皮质(vACC)及其连接部位(包括杏仁核)的异常有关,后者是皮质下突神经系统的关键组成部分,可促进情绪调节。健康个体中从vACC到杏仁核的功能连接性降低与众所周知的5-羟色胺转运蛋白启动子多态性(5-HTTLPR,基因座SLC6A4)的短“ s”等位基因(而不是长“ l”等位基因)相关,和BD的功能一样。这项研究检验了s等位基因影响BD vACC-杏仁核神经系统功能障碍的假说。 30名患有BD的正常人(20 s携带者,10 ll)和48名健康比较(HC)参与者(34 s,14 ll)参与了事件相关的功能磁共振成像扫描,同时处理了恐惧,快乐或中性的面孔。在恐惧和开心的表情处理过程中,与HC组相比,BD中的vACC激活显着降低,与HC和BD组中的ll个个体相比,s携带者中的vACC激活程度最高,因此BD s携带者表现出最大程度的vACC功能障碍。在杏仁核激活中未检测到显着差异。这些发现表明,5-HTTLPR s等位基因可能与特征在于vACC功能异常的BD内与性状相关,遗传衍生的神经生物学亚组有关。通过针对血清素能系统和vACC,可以针对该BD亚组优化未来治疗。

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