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焦虑障碍的汇聚功能基因组学:基因、生物标志物、途径和机制的转化鉴定。

Convergent functional genomics of anxiety disorders: translational identification of genes, biomarkers, pathways and mechanisms.

机构信息

Department of Psychiatry, Indiana University School of Medicine, Indianapolis, IN 46202, USA.

出版信息

Transl Psychiatry. 2011 May 24;1(5):e9. doi: 10.1038/tp.2011.9.

Abstract

Anxiety disorders are prevalent and disabling yet understudied from a genetic standpoint, compared with other major psychiatric disorders such as bipolar disorder and schizophrenia. The fact that they are more common, diverse and perceived as embedded in normal life may explain this relative oversight. In addition, as for other psychiatric disorders, there are technical challenges related to the identification and validation of candidate genes and peripheral biomarkers. Human studies, particularly genetic ones, are susceptible to the issue of being underpowered, because of genetic heterogeneity, the effect of variable environmental exposure on gene expression, and difficulty of accrual of large, well phenotyped cohorts. Animal model gene expression studies, in a genetically homogeneous and experimentally tractable setting, can avoid artifacts and provide sensitivity of detection. Subsequent translational integration of the animal model datasets with human genetic and gene expression datasets can ensure cross-validatory power and specificity for illness. We have used a pharmacogenomic mouse model (involving treatments with an anxiogenic drug--yohimbine, and an anti-anxiety drug--diazepam) as a discovery engine for identification of anxiety candidate genes as well as potential blood biomarkers. Gene expression changes in key brain regions for anxiety (prefrontal cortex, amygdala and hippocampus) and blood were analyzed using a convergent functional genomics (CFG) approach, which integrates our new data with published human and animal model data, as a translational strategy of cross-matching and prioritizing findings. Our work identifies top candidate genes (such as FOS, GABBR1, NR4A2, DRD1, ADORA2A, QKI, RGS2, PTGDS, HSPA1B, DYNLL2, CCKBR and DBP), brain-blood biomarkers (such as FOS, QKI and HSPA1B), pathways (such as cAMP signaling) and mechanisms for anxiety disorders--notably signal transduction and reactivity to environment, with a prominent role for the hippocampus. Overall, this work complements our previous similar work (on bipolar mood disorders and schizophrenia) conducted over the last decade. It concludes our programmatic first pass mapping of the genomic landscape of the triad of major psychiatric disorder domains using CFG, and permitted us to uncover the significant genetic overlap between anxiety and these other major psychiatric disorders, notably the under-appreciated overlap with schizophrenia. PDE10A, TAC1 and other genes uncovered by our work provide a molecular basis for the frequently observed clinical co-morbidity and interdependence between anxiety and other major psychiatric disorders, and suggest schizo-anxiety as a possible new nosological domain.

摘要

与双相情感障碍和精神分裂症等其他主要精神疾病相比,焦虑症从遗传学角度来看更为普遍、多样且被认为是正常生活的一部分,但研究却相对较少。此外,与其他精神疾病一样,在确定候选基因和外周生物标志物方面存在技术挑战。由于遗传异质性、环境暴露对基因表达的影响以及难以获得大量、表型良好的队列,人类研究,特别是遗传研究,容易出现研究能力不足的问题。在遗传上同质且易于实验的动物模型基因表达研究中,可以避免假象,并提高检测的敏感性。随后,将动物模型数据集与人类遗传和基因表达数据集进行转化整合,可以确保疾病的交叉验证能力和特异性。我们使用了一种药物基因组学小鼠模型(涉及使用一种焦虑药物——育亨宾和一种抗焦虑药物——地西泮进行治疗),作为鉴定焦虑候选基因和潜在血液生物标志物的发现引擎。使用会聚功能基因组学(CFG)方法分析了焦虑相关关键大脑区域(前额叶皮层、杏仁核和海马体)和血液中的基因表达变化,该方法整合了我们的新数据以及已发表的人类和动物模型数据,作为一种跨匹配和优先考虑发现的转化策略。我们的工作确定了顶级候选基因(如 FOS、GABBR1、NR4A2、DRD1、ADORA2A、QKI、RGS2、PTGDS、HSPA1B、DYNLL2、CCKBR 和 DBP)、脑-血生物标志物(如 FOS、QKI 和 HSPA1B)、途径(如 cAMP 信号转导)和焦虑症的机制——尤其是信号转导和对环境的反应性,其中海马体起着重要作用。总的来说,这项工作补充了我们过去十年进行的类似工作(双相情感障碍和精神分裂症)。它总结了我们使用 CFG 对主要精神障碍领域三联体基因组景观进行的初步映射计划,并使我们能够发现焦虑症与这些其他主要精神疾病之间存在显著的遗传重叠,尤其是与精神分裂症之间被低估的重叠。我们的工作揭示的 PDE10A、TAC1 和其他基因提供了焦虑症与其他主要精神疾病之间经常观察到的临床共病和相互依赖性的分子基础,并暗示了作为一个可能的新分类学领域的“精神分裂症-焦虑症”。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d71b/3309477/bbba11d97fa7/tp20119f1.jpg

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