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Invited Commentary: Detecting Individual and Global Horizontal Pleiotropy in Mendelian Randomization—A Job for the Humble Heterogeneity Statistic?

机译:特邀评论:在孟德尔随机化中检测个体和全局水平多向性-一项简朴的异质性统计工作?

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摘要

Mendelian randomization (MR) is gaining in recognition and popularity as a method for strengthening causal inference in epidemiology by utilizing genetic variants as instrumental variables. Concurrently with the explosion in empirical MR studies, there has been the steady production of new approaches for MR analysis. The recently proposed “global and individual tests for direct effects” (GLIDE) approach fits into a family of methods that aim to detect horizontal pleiotropy—at the individual single nucleotide polymorphism level and at the global level—and to adjust the analysis by removing outlying single nucleotide polymorphisms. In this commentary, we explain how existing methods can (and indeed are) being used to detect pleiotropy at the individual and global levels, although not explicitly using this terminology. By doing so, we show that the true comparator for GLIDE is not MR-Egger regression (as Dai et al., the authors of the accompanying article (Am J Epidemiol. 2018;187(12):2672–2680), claim) but rather the humble heterogeneity statistic.
机译:孟德尔随机化(MR)作为一种通过利用遗传变异作为工具变量来加强流行病学中因果关系推断的方法,已得到认可和普及。在经验性MR研究的爆炸式增长的同时,不断有新的MR分析方法产生。最近提出的“全局和单个直接效应测试”(GLIDE)方法适合一系列方法,旨在检测水平多效性(在单个单核苷酸多态性水平和全局水平),并通过消除外围因素来调整分析单核苷酸多态性。在这篇评论中,我们将解释如何(甚至确实)使用现有方法在个体和全局级别上检测多效性,尽管并未明确使用此术语。通过这样做,我们表明GLIDE的真正比较器不是MR-Egger回归(如Dai等人,随附文章的作者(Am J Epidemiol。2018; 187(12):2672–2680)声称)。而是卑微的异质性统计数据。

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