作者
Dina Mansour Aly,Om Prakash Dwivedi,Rashmi B. Prasad,Annemari Käräjämäki,Rebecka Hjort,Manonanthini Thangam,Mikael Åkerlund,Anubha Mahajan,Miriam S. Udler,José C. Florez,Mark I. McCarthy,Gonçalo R. Abecasis,Aris Baras,Michael Cantor,Giovanni Coppola,Aris N. Economides,Luca A. Lotta,John D. Overton,Jeffrey G. Reid,Alan R. Shuldiner,Christina Beechert,Caitlin Forsythe,Erin D. Fuller,Zhenhua Gu,Michael Lattari,Alexander Lopez,Thomas D. Schleicher,Maria Sotiropoulos Padilla,Louis Widom,Sarah E. Wolf,Manasi Pradhan,Kia Manoochehri,Ricardo H. Ulloa,Xiaodong Bai,Suganthi Balasubramanian,Andrew Blumenfeld,Gisu Eom,Lukas Habegger,Alicia Hawes,Shareef Khalid,Evan K. Maxwell,William Salerno,Jeffrey Staples,Marcus B. Jones,Lyndon J. Mitnaul,Julia Brosnan,Olle Melander,Sofia Carlsson,Ola Hansson,Jaakko Tuomilehto,Leif Groop,Emma Ahlqvist
摘要
Type 2 diabetes has been reproducibly clustered into five subtypes with different disease progression and risk of complications; however, etiological differences are unknown. We used genome-wide association and genetic risk score (GRS) analysis to compare the underlying genetic drivers. Individuals from the Swedish ANDIS (All New Diabetics In Scania) study were compared to individuals without diabetes; the Finnish DIREVA (Diabetes register in Vasa) and Botnia studies were used for replication. We show that subtypes differ with regard to family history of diabetes and association with GRS for diabetes-related traits. The severe insulin-resistant subtype was uniquely associated with GRS for fasting insulin but not with variants in the TCF7L2 locus or GRS reflecting insulin secretion. Further, an SNP (rs10824307) near LRMDA was uniquely associated with mild obesity-related diabetes. Therefore, we conclude that the subtypes have partially distinct genetic backgrounds indicating etiological differences.
丰盛的煎饼
西红柿炒番茄
乐乐乐乐乐乐
加菲丰丰
Hayat
kento
寻道图强
ShowMaker
YifanWang
冒险寻羊
杳鸢
互助遵法尚德
lanxinyue
spark810
景辣条
乐乐
大仙
yyymmma
斯文败类
水牛
皖公网安备34019202002308
