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Psychiatric polygenic risk associates with cortical morphology and functional organization in aging

机译:精神病多基因风险与衰老中的皮质形态和功能组织有关

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Common brain abnormalities in cortical morphology and functional organization are observed in psychiatric disorders and aging, reflecting shared genetic influences. This preliminary study aimed to examine the contribution of a polygenetic risk for psychiatric disorders (PRScross) to aging brain and to identify molecular mechanisms through the use of multimodal brain images, genotypes, and transcriptome data. We showed age-related cortical thinning in bilateral inferior frontal cortex (IFC) and superior temporal gyrus and alterations in the functional connectivity between bilateral IFC and between right IFC and right inferior parietal lobe as a function of PRScross. Interestingly, the genes in PRScross, that contributed most to aging neurodegeneration, were expressed in the functioanlly connected cortical regions. Especially, genes identified through the genotype-functional connectivity association analysis were commonly expressed in both cortical regions and formed strong gene networks with biological processes related to neural plasticity and synaptogenesis, regulated by glutamatergic and GABAergic transmission, neurotrophin signaling, and metabolism. This study suggested integrating genotype and transcriptome with neuroimage data sheds new light on the mechanisms of aging brain.
机译:在精神疾病和衰老中观察到常见的大脑皮质形态和功能组织异常,反映出共同的遗传影响。这项初步研究旨在检验精神疾病的多基因风险(PRS cross )对大脑衰老的贡献,并通过使用多模式大脑图像,基因型和转录组数据确定分子机制。我们显示了年龄相关的双侧下额叶皮层(IFC)和颞上回皮层变薄以及双侧IFC之间以及右IFC和右下顶叶之间的功能连通性的变化,这是PRS cross 的函数。有趣的是,在衰老的神经变性中起主要作用的PRS cross 基因在功能连接的皮质区域表达。特别是,通过基因型-功能连通性关联分析确定的基因通常在两个皮层区域表达,并形成强大的基因网络,其生物学过程涉及神经可塑性和突触形成,受谷氨酸和GABA能传递,神经营养蛋白信号传导和代谢调控。这项研究表明,将基因型和转录组与神经影像数据相结合,为大脑衰老的机制提供了新的思路。

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