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双相情感障碍的遗传学研究:需要一个将复杂分子生物学与临床知情表型特征相结合的研究框架。

Genetic research into bipolar disorder: the need for a research framework that integrates sophisticated molecular biology and clinically informed phenotype characterization.

机构信息

Unit on the Genetic Basis of Mood and Anxiety Disorders, National Institute of Mental Health (NIMH), National Institutes of Health (NIH), Bethesda, MD 20892-3719, USA.

出版信息

Psychiatr Clin North Am. 2010 Mar;33(1):67-82. doi: 10.1016/j.psc.2009.10.005.

Abstract

Research into the genetic basis of bipolar disorder (BD) has reached a turning point. Genome-wide association studies (GWAS), encompassing several thousand samples, have produced replicated evidence for some novel susceptibility genes; however, the genetic variants implicated so far account for only a fraction of disease liability, a phenomenon not limited to psychiatric phenotypes but characteristic of all complex genetic traits studied to date. It appears that pure genomic approaches, such as GWAS alone, will not suffice to unravel the genetic basis of a complex illness like BD. Genomic approaches will need to be complemented by a variety of strategies, including phenomics, epigenomics, pharmacogenomics, and neurobiology, as well as the study of environmental factors. This review highlights the most promising findings from recent GWAS and candidate gene studies in BD. It furthermore sketches out a potential research framework integrating various lines of research into the molecular biological basis of BD.

摘要

双相障碍(BD)的遗传基础研究已经到了一个转折点。全基因组关联研究(GWAS)涵盖了数千个样本,为一些新的易感基因提供了可重复的证据;然而,到目前为止,所涉及的遗传变异只占疾病易感性的一小部分,这种现象不仅限于精神表型,而是目前研究的所有复杂遗传特征的特征。看来,单纯的基因组方法,如单独的 GWAS,不足以揭示像 BD 这样的复杂疾病的遗传基础。基因组方法需要辅以各种策略,包括表型组学、表观基因组学、药物基因组学和神经生物学,以及环境因素的研究。这篇综述突出了最近在 BD 的 GWAS 和候选基因研究中最有前途的发现。它还勾勒出一个潜在的研究框架,将各种研究整合到 BD 的分子生物学基础中。

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