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Common Polymorphisms in the Age of Research Domain Criteria (RDoC): Integration and Translation

机译:研究领域标准(RDoC)时代的常见多态性:整合和翻译

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摘要

The value of common polymorphisms in guiding clinical psychiatry is limited by the complex polygenic architecture of psychiatric disorders. Common polymorphisms have too small an effect on risk for psychiatric disorders as defined by clinical phenomenology to guide clinical practice. To identify polymorphic effects that are large and reliable enough to serve as biomarkers requires detailed analysis of a polymorphism's biology across levels of complexity from molecule to cell to circuit and behavior. Emphasis on behavioral domains rather than clinical diagnosis, as proposed in the Research Domain Criteria framework, facilitates the use of mouse models that recapitulate human polymorphisms because effects on equivalent phenotypes can be translated across species and integrated across levels of analysis. A knockin mouse model of a common polymorphism in the brain-derived neurotrophic factor gene (BDNF) provides examples of how such a vertically integrated translational approach can identify robust genotype-phenotype relationships that have relevance to psychiatric practice.
机译:常见的多态性在指导临床精神病学方面的价值受到精神病性疾病复杂的多基因结构的限制。常见的多态性对精神病风险的影响太小,如临床现象学所定义,以指导临床实践。为了识别足够大且可靠的多态性效应以用作生物标记,需要从分子到细胞,到电路和行为的复杂性水平对多态性生物学进行详细分析。正如研究领域标准框架中所建议的那样,着重于行为领域而不是临床诊断,这有助于简化人类多态性的小鼠模型的使用,因为对等价表型的影响可以跨物种进行转化,并且可以跨分析水平进行整合。脑源性神经营养因子基因(BDNF)中常见多态性的敲入小鼠模型提供了这种垂直整合的翻译方法如何识别与精神病学实践相关的稳健的基因型与表型关系的示例。

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