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首页> 外文期刊>Expert review of neurotherapeutics >Genetics of panic disorder: focus on association studies and therapeutic perspectives.
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Genetics of panic disorder: focus on association studies and therapeutic perspectives.

机译:恐慌症的遗传学:专注于关联研究和治疗观点。

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There is evidence for either genetic heterogeneity or complex inheritance with an interaction of environmental factors and multiple single genes in the etiology of panic disorder. Although linkage analyses of panic disorder have implicated several chromosomal regions including 1q, 2q, 4q, 7p, 9q, 12q, 13q, 15q and 22q, they so far have not been able to identify a major gene responsible for panic disorder. Several genes of classical candidate neurotransmitter systems have been reported to be associated with panic disorder. Genetic variation in genes of monoamine oxidase A, catechol-O-methyltransferase, adenosine receptor (ADORA2A) and cholecystokinin B receptor have been inconsistently replicated. There are multiple lines of evidence for highly relevant effects of gender and ethnicity. Future research strategies might focus on broad phenotypes defined by comorbidity or intermediate phenotypes and include the use of animal models for identifying candidate genes, such as the regulator of G-protein signaling (RGS2) gene, genome-wide association studies in large samples, studies of gene-gene and gene-environment interactions and pharmacogenetic studies. The identification of novel pathophysiological pathways may provide the basis for the development of novel therapeutic interventions.
机译:在恐慌症的病因中,有证据表明遗传异质性或复杂遗传与环境因素和多个单一基因的相互作用。尽管恐慌症的连锁分析涉及几个染色体区域,包括1q,2q,4q,7p,9q,12q,13q,15q和22q,但到目前为止,他们还不能鉴定出引起恐慌症的主要基因。据报道,经典候选神经递质系统的几种基因与恐慌症有关。不一致地复制了单胺氧化酶A,邻苯二酚-O-甲基转移酶,腺苷受体(ADORA2A)和胆囊收缩素B受体基因的遗传变异。有多种证据表明性别和种族高度相关。未来的研究策略可能集中于由合并症或中间表型定义的广泛表型,包括使用动物模型来识别候选基因,例如G蛋白信号(RGS2)基因的调节剂,大样本中的全基因组关联研究,研究基因-基因和基因-环境相互作用的研究以及药物遗传学研究。新的病理生理途径的鉴定可为新的治疗干预措施的发展提供基础。

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