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反向 GWAS:利用遗传学识别和建立表型亚型模型。

Reverse GWAS: Using genetics to identify and model phenotypic subtypes.

机构信息

Department of Medicine, UCSF, San Francisco, California, United States of America.

Wellcome Sanger Institute, Cambridge, United Kingdom.

出版信息

PLoS Genet. 2019 Apr 5;15(4):e1008009. doi: 10.1371/journal.pgen.1008009. eCollection 2019 Apr.

Abstract

Recent and classical work has revealed biologically and medically significant subtypes in complex diseases and traits. However, relevant subtypes are often unknown, unmeasured, or actively debated, making automated statistical approaches to subtype definition valuable. We propose reverse GWAS (RGWAS) to identify and validate subtypes using genetics and multiple traits: while GWAS seeks the genetic basis of a given trait, RGWAS seeks to define trait subtypes with distinct genetic bases. Unlike existing approaches relying on off-the-shelf clustering methods, RGWAS uses a novel decomposition, MFMR, to model covariates, binary traits, and population structure. We use extensive simulations to show that modelling these features can be crucial for power and calibration. We validate RGWAS in practice by recovering a recently discovered stress subtype in major depression. We then show the utility of RGWAS by identifying three novel subtypes of metabolic traits. We biologically validate these metabolic subtypes with SNP-level tests and a novel polygenic test: the former recover known metabolic GxE SNPs; the latter suggests subtypes may explain substantial missing heritability. Crucially, statins, which are widely prescribed and theorized to increase diabetes risk, have opposing effects on blood glucose across metabolic subtypes, suggesting the subtypes have potential translational value.

摘要

近期和经典的研究揭示了复杂疾病和特征中具有生物学和医学意义的亚类型。然而,相关的亚类型通常是未知的、未测量的或存在争议的,因此自动化的统计方法对于亚类型定义非常有价值。我们提出了反向 GWAS(RGWAS),使用遗传学和多种特征来识别和验证亚类型:GWAS 旨在寻找给定特征的遗传基础,而 RGWAS 则旨在定义具有不同遗传基础的特征亚类型。与依赖现成聚类方法的现有方法不同,RGWAS 使用一种新颖的分解方法 MFMR 来建模协变量、二分类特征和群体结构。我们使用广泛的模拟来表明,对这些特征进行建模对于功效和校准可能至关重要。我们通过在重度抑郁症中恢复最近发现的应激亚类型在实践中验证了 RGWAS 的有效性。然后,我们通过识别三种新的代谢特征亚类型来展示 RGWAS 的实用性。我们使用 SNP 水平的测试和一种新的多基因测试来对这些代谢亚类型进行生物学验证:前者可以恢复已知的代谢 GxE SNP;后者表明,亚类型可能可以解释大量的遗传缺失。至关重要的是,他汀类药物被广泛开处方,并被认为会增加糖尿病的风险,但在代谢亚类型中对血糖有相反的影响,这表明这些亚类型具有潜在的转化价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1086/6469799/8e2f9dbc133d/pgen.1008009.g001.jpg

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