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惊恐障碍的遗传学。

The genetics of panic disorder.

机构信息

Institute of Human Genetics, University of Bonn, Germany.

出版信息

J Med Genet. 2011 Jun;48(6):361-8. doi: 10.1136/jmg.2010.086876. Epub 2011 Apr 14.

DOI:10.1136/jmg.2010.086876
PMID:21493958
Abstract

Panic disorder (PD) is one of the most common anxiety disorders, with a prevalence of 3.4-4.7%. Although PD seems to have no known cause, and its underlying aetiology is not well understood, studies have consistently shown that genetic factors explain about half of the variance. It is likely that most cases of PD have a complex genetic basis. Existing data suggest, however, that the genetic architecture underlying PD is heterogeneous and differs between cases. For example, the degree of genetic complexity, and the pattern of genes involved might differ in familial versus non-familial cases, in early- versus late-onset cases, or when different comorbid conditions, gender and potential intermediate or sub-phenotypes are considered. At the molecular genetic level, linkage and association studies-the latter including traditional candidate gene and recent genome-wide studies-have been used to study PD. Although no robust molecular genetic findings have emerged so far, it is conceivable that the first PD susceptibility genes will be identified in the coming years via the application of modern molecular genetic methods and through multicentre collaborations to bring together combined, large datasets. Such findings could have a major impact on our understanding of the pathophysiology of this disorder, and would provide important opportunities to investigate genotype-phenotype correlations, as well as the interaction between genetic and environmental factors involved in the pathogenesis of PD. Here, the authors summarise the latest genetics findings about PD, and give an overview of anticipated future developments.

摘要

惊恐障碍(PD)是最常见的焦虑障碍之一,其患病率为 3.4-4.7%。尽管 PD 似乎没有已知的病因,其潜在的病因也尚未完全了解,但研究一直表明遗传因素解释了大约一半的变异。很可能大多数 PD 病例都有复杂的遗传基础。然而,现有数据表明,PD 潜在的遗传结构是异质的,并且在病例之间存在差异。例如,遗传复杂性的程度以及所涉及的基因模式可能在家族性与非家族性病例、早发性与晚发性病例、不同的合并症、性别以及潜在的中间或亚表型中存在差异。在分子遗传学水平上,连锁和关联研究——后者包括传统的候选基因和最近的全基因组研究——已被用于研究 PD。尽管到目前为止还没有出现稳健的分子遗传学发现,但可以想象,通过应用现代分子遗传学方法和通过多中心合作汇集组合的大型数据集,将在未来几年内确定第一个 PD 易感基因。这些发现可能会对我们对这种疾病病理生理学的理解产生重大影响,并为研究基因型-表型相关性以及 PD 发病机制中涉及的遗传和环境因素之间的相互作用提供重要机会。在这里,作者总结了 PD 的最新遗传学发现,并概述了预期的未来发展。

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