5-羟色胺受体1A基因C(-1019)G多态性对杏仁核反应性及特质焦虑的影响。
Effects of HTR1A C(-1019)G on amygdala reactivity and trait anxiety.
作者信息
Fakra Eric, Hyde Luke W, Gorka Adam, Fisher Patrick M, Muñoz Karen E, Kimak Mark, Halder Indrani, Ferrell Robert E, Manuck Stephen B, Hariri Ahmad R
机构信息
Hôpital de laTimone, ServiceHospitalo-Universitaire dePsychiatrie, Hôpital SteMarguerite, Marseille, France.
出版信息
Arch Gen Psychiatry. 2009 Jan;66(1):33-40. doi: 10.1001/archpsyc.66.1.33.
CONTEXT
Serotonin 1A (5-hydroxytryptamine 1A [5-HT(1A)]) autoreceptors mediate negative feedback inhibition of serotonergic neurons and play a critical role in regulating serotonin signaling involved in shaping the functional response of major forebrain targets, such as the amygdala, supporting complex behavioral processes. A common functional variation (C[-1019]G) in the human 5-HT(1A) gene (HTR1A) represents 1 potential source of such interindividual variability. Both in vitro and in vivo, -1019G blocks transcriptional repression, leading to increased autoreceptor expression. Thus, -1019G may contribute to relatively decreased serotonin signaling at postsynaptic forebrain target sites via increased negative feedback.
OBJECTIVES
To evaluate the effects of HTR1A C(-1019)G on amygdala reactivity and to use path analyses to explore the impact of HTR1A-mediated variability in amygdala reactivity on individual differences in trait anxiety. We hypothesized that -1019G, which potentially results in decreased serotonin signaling, would be associated with relatively decreased amygdala reactivity and related trait anxiety.
DESIGN
Imaging genetics in participants from an archival database.
PARTICIPANTS
Eighty-nine healthy adults.
RESULTS
Consistent with prior findings, -1019G was associated with significantly decreased threat-related amygdala reactivity. Importantly, this effect was independent of that associated with another common functional polymorphism that affects serotonin signaling, 5-HTTLPR. While there were no direct genotype effects on trait anxiety, HTR1A C(-1019)G indirectly predicted 9.2% of interindividual variability in trait anxiety through its effects on amygdala reactivity.
CONCLUSIONS
Our findings further implicate relatively increased serotonin signaling, associated with a genetic variation that mediates increased 5-HT(1A) autoreceptors, in driving amygdala reactivity and trait anxiety. Moreover, they provide empirical documentation of the basic premise that genetic variation indirectly affects emergent behavioral processes related to psychiatric disease risk by biasing the response of underlying neural circuitries.
背景
血清素1A(5-羟色胺1A [5-HT(1A)])自身受体介导血清素能神经元的负反馈抑制,并在调节血清素信号传导中发挥关键作用,血清素信号传导参与塑造主要前脑靶点(如杏仁核)的功能反应,支持复杂的行为过程。人类5-HT(1A)基因(HTR1A)中常见的功能变异(C[-1019]G)是这种个体间差异的一个潜在来源。在体外和体内,-1019G都会阻断转录抑制,导致自身受体表达增加。因此,-1019G可能通过增加负反馈,导致突触后前脑靶点部位的血清素信号相对减少。
目的
评估HTR1A C(-1019)G对杏仁核反应性的影响,并使用路径分析来探究HTR1A介导的杏仁核反应性变异对特质焦虑个体差异的影响。我们假设,可能导致血清素信号减少的-1019G,会与相对降低的杏仁核反应性及相关特质焦虑有关。
设计
对来自存档数据库的参与者进行影像遗传学研究。
参与者
89名健康成年人。
结果
与先前的研究结果一致,-1019G与显著降低的与威胁相关的杏仁核反应性有关。重要的是,这种效应独立于与另一种影响血清素信号传导的常见功能多态性5-HTTLPR相关的效应。虽然对特质焦虑没有直接的基因型效应,但HTR1A C(-1019)G通过其对杏仁核反应性的影响,间接预测了特质焦虑中9.2%的个体间变异。
结论
我们的研究结果进一步表明,与介导5-HT(1A)自身受体增加的基因变异相关的血清素信号相对增加,会驱动杏仁核反应性和特质焦虑。此外,它们为以下基本前提提供了实证依据,即基因变异通过影响潜在神经回路的反应,间接影响与精神疾病风险相关的新兴行为过程。
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