Random glucose GWAS in 493,036 individuals provides insights into diabetes pathophysiology, complications and treatment stratification
Author:
Lagou Vasiliki, Jiang Longda, Ulrich Anna, Zudina Liudmila, González Karla Sofia Gutiérrez, Balkhiyarova Zhanna, Faggian Alessia, Chen Shiqian, Todorov Petar, Sharapov Sodbo, David AlessiaORCID, Marullo Letizia, Mägi Reedik, Rujan Roxana-Maria, Ahlqvist Emma, Thorleifsson Gudmar, Gao He, Evangelou EvangelosORCID, Benyamin Beben, Scott Robert, Isaacs Aaron, Zhao Jing Hua, Willems Sara M, Johnson Toby, Gieger Christian, Grallert Harald, Meisinger Christa, Müller-Nurasyid Martina, Strawbridge Rona JORCID, Goel Anuj, Rybin Denis, Albrecht Eva, Jackson Anne U, Stringham Heather M, Corrêa Ivan RORCID, Eric Farber-Eber, Steinthorsdottir Valgerdur, Uitterlinden André G, Munroe Patricia B, Brown Morris J, Julian Schmidberger, Holmen Oddgeir, Thorand Barbara, Hveem Kristian, Wilsgaard Tom, Mohlke Karen L, Kratzer Wolfgang, Mark Haenle, Koenig Wolfgang, Boehm Bernhard O, Tan Tricia M, Tomas Alejandra, Salem Victoria, Barroso InêsORCID, Tuomilehto Jaakko, Boehnke Michael, Florez Jose C, Hamsten Anders, Watkins Hugh, Njølstad Inger, Wichmann H-Erich, Caulfield Mark J, Khaw Kay-Tee, van Duijn Cornelia, Hofman AlbertORCID, Wareham Nicholas J, Langenberg ClaudiaORCID, Whitfield John B, Martin Nicholas G, Montgomery Grant, Scapoli Chiara, Tzoulaki IoannaORCID, Elliott PaulORCID, Thorsteinsdottir Unnur, Stefansson Kari, Brittain Evan L, McCarthy Mark I, Froguel Philippe, Sexton Patrick M, Wootten Denise, Groop Leif, Dupuis Josée, Meigs James B, Deganutti Giuseppe, Demirkan Ayse, Pers Tune H, Reynolds Christopher A, Aulchenko Yurii S, Kaakinen Marika A, Jones Ben, Prokopenko Inga
Abstract
AbstractHomeostatic control of blood glucose requires different physiological responses in the fasting and post-prandial states. We reasoned that glucose measurements under non-standardised conditions (random glucose; RG) may capture diverse glucoregulatory processes more effectively than previous genome-wide association studies (GWAS) of fasting glycaemia or after standardised glucose loads. Through GWAS meta-analysis of RG in 493,036 individuals without diabetes of diverse ethnicities we identified 128 associated loci represented by 162 distinct signals, including 14 with sex-dimorphic effects, 9 discovered through trans-ethnic analysis, and 70 novel signals for glycaemic traits. Novel RG loci were particularly enriched in expression in the ileum and colon, indicating a prominent role for the gastrointestinal tract in the control of blood glucose. Functional studies and molecular dynamics simulations of coding variants of GLP1R, a well-established type 2 diabetes treatment target, provided a genetic framework for optimal selection of GLP-1R agonist therapy. We also provided new evidence from Mendelian randomisation that lung function is modulated by blood glucose and that pulmonary dysfunction is a diabetes complication. Thus, our approach based on RG GWAS provided wide-ranging insights into the biology of glucose regulation, diabetes complications and the potential for treatment stratification.
Publisher
Cold Spring Harbor Laboratory
Cited by
7 articles.
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