Abstract

This study focused on resolving the relationship between BMI and type 2 diabetes. The availability of multiple variants associated with BMI offers a new chance to resolve the true causal effect of BMI on type 2 diabetes; however, the properties of these associations and their validity as genetic instruments need to be considered alongside established and new methods for undertaking Mendelian randomization (MR). We explore the potential for pleiotropic genetic variants to generate bias, revise existing estimates, and illustrate value in new analysis methods. A two-sample MR approach with 96 genetic variants was used with three different analysis methods, two of which (MR-Egger and the weighted median) have been developed specifically to address problems of invalid instrumental variables. We estimate an odds ratio for type 2 diabetes per unit increase in BMI (kg/m2) of between 1.19 and 1.38, with the most stable estimate using all instruments and a weighted median approach (1.26 [95% CI 1.17, 1.34]). TCF7L2(rs7903146) was identified as a complex effect or pleiotropic instrument, and removal of this variant resulted in convergence of causal effect estimates from different causal analysis methods. This indicated the potential for pleiotropy to affect estimates and differences in performance of alternative analytical methods. In a real type 2 diabetes–focused example, this study demonstrates the potential impact of invalid instruments on causal effect estimates and the potential for new approaches to mitigate the bias caused.

Keywords

Mendelian randomizationType 2 diabetesCausal inferencePleiotropyStatisticsInstrumental variableMultivariate statisticsType I and type II errorsEconometricsMedicineDiabetes mellitusBiologyMathematicsGeneticsGenetic variantsEndocrinology

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Publication Info

Year
2016
Type
article
Volume
65
Issue
10
Pages
3002-3007
Citations
188
Access
Closed

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Laura J. Corbin, Rebecca C. Richmond, Kaitlin H. Wade et al. (2016). BMI as a Modifiable Risk Factor for Type 2 Diabetes: Refining and Understanding Causal Estimates Using Mendelian Randomization. Diabetes , 65 (10) , 3002-3007. https://doi.org/10.2337/db16-0418

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DOI
10.2337/db16-0418