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首页> 外文期刊>Progress in Neuro-Psychopharmacology & Biological Psychiatry: An International Research, Review and News Journal >A Homer 1 gene variant influences brain structure and function, lithium effects on white matter, and antidepressant response in bipolar disorder: A multimodal genetic imaging study
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A Homer 1 gene variant influences brain structure and function, lithium effects on white matter, and antidepressant response in bipolar disorder: A multimodal genetic imaging study

机译:Homer 1基因变异影响脑结构和功能,对白质的锂效应,以及双相紊乱中的抗抑郁症反应:多峰遗传成像研究

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Abstract Background The Homer family of postsynaptic scaffolding proteins plays a crucial role in glutamate-mediated synaptic plasticity, a phenotype associated with Bipolar Disorder (BD). Homer is a target for antidepressants and mood stabilizers. The AA risk genotype of the Homer rs7713917 A>G SNP has been associated with mood disorders and suicide, and in healthy humans with brain function. Despite the evidence linking Homer 1 gene and function to mood disorder, as well as its involvement in animal models of depression, no study has yet investigated the role of Homer in bipolar depression and treatment response. Methods We studied 199 inpatients, affected by a major depressive episode in course of BD. 147 patients were studied with structural MRI of grey and white matter, and 50 with BOLD functional MRI of emotional processing. 158 patients were treated with combined total sleep deprivation and light therapy. Results At neuroimaging, patients with the AA genotype showed lower grey matter volumes in medial prefrontal cortex, higher BOLD fMRI neural responses to emotional stimuli in anterior cingulate cortex, and lower fractional anisotropy in bilateral frontal WM tracts. Lithium treatment increased axial diffusivity more in AA patients than in G*carriers. At clinical evaluation, the same AA homozygotes showed a worse antidepressant response to combined SD and LT. Conclusions rs7713917 influenced brain grey and white matter structure and function in BD, long term effects of lithium on white matter structure, and antidepressant response to chronotherapeutics, thus suggesting that glutamatergic neuroplasticity and Homer 1 function might play a role in BD psychopathology and response to treatment. Highlights ? rs7713917 significantly influenced grey and white matter structure and function. ? AA homozygotes showed smaller medial prefrontal cortex than G carriers. ? AA homozygotes showed higher signal responses in right dorsal anterior cingulate cortex. ? AA homozygotes showed significantly lower FA in frontal tracts than G carriers. ? rs7713917 also influenced severity of depression and response to treatment.
机译:摘要背景母亲突触脚手架蛋白质在谷氨酸介导的突触塑性中起着至关重要的作用,一种与双极障碍相关的表型(BD)。荷马是抗抑郁药和情绪稳定剂的目标。 Homer RS7713917 A> G SNP的AA风险基因型已与情绪障碍和自杀相关,以及脑功能的健康人物。尽管证据证据将Homer 1基因链接到情绪障碍,但其参与抑郁症的动物模型,尚未研究HOMER在双相抑郁和治疗反应中的作用。方法我们研究了199例住院患者,受到BD过程中的主要抑郁情节。 147名患者用灰白油和白质的结构MRI研究,50例具有粗体的情绪加工MRI。 158例患者患有组合的睡眠剥夺和光疗法。结果在神经影像动物中,AA基因型患者在内侧前额叶皮质中显示出较低的灰质体积,对前刺皮层的情绪刺激较高的大胆FMRI神经响应,以及双侧额相WM椎间盘的较低分数各向异性。锂处理比AA患者更多地增加轴向扩散,而不是G *载体。在临床评价中,相同的AA纯合子表显示了与组合SD和LT的更差的抗抑郁症反应。结论RS7713917影响了脑灰白质地结构及在BD的功能,锂对白质结构的长期影响,以及对计时器的抗抑郁药反应,从而表明谷氨酸神经塑料和HOMER 1功能可能在BD精神病理学中发挥作用并对治疗作用。 。强调 ? RS7713917显着影响灰色和白质结构和功能。还AA homozygotes显示比G载体更小的内侧前额叶皮质。还AA Homozygotes显示出右侧铰接皮质较高的信号响应。还AA Homozygotes在载体中显着降低了比G载体的FA。还RS7713917也影响了抑郁症的严重程度和对治疗的反应。

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