Triglyceride Response to an Intensive Lifestyle Intervention Is Enhanced in Carriers of the GCKR Pro446Leu Polymorphism

Publication Description
Context: Glucokinase regulatory protein (GCKR) regulates the trafficking and enzymatic activity of hepatic glucokinase, the rate-limiting enzyme in glycogen synthesis and glycolysis. The intronic single-nucleotide polymorphism (SNP) rs780094 (intron 16) and the missense SNP rs1260326 (P446L) in the GCKR gene are strongly associated with increased circulating triglyceride and C-reactive protein levels and, paradoxically, reductions in diabetes incidence, fasting glucose levels, and insulin resistance. Objective, Setting, and Patients: We sought to replicate these associations and evaluate interactions with lifestyle and metformin interventions in the multiethnic Diabetes Prevention Program (DPP). Interventions and Main Outcome Measures: We genotyped the two GCKR SNP in 3346 DPP participants and evaluated association with progression to diabetes and both baseline levels and changes in triglycerides, homeostasis model assessment of insulin resistance (HOMA-IR), oral disposition index, and inflammatory markers along with their interactions with DPP interventions. Results: GCKR variation did not predict development of type 2 diabetes. At baseline, the 446L allele was associated with higher triglyceride and C-reactive protein levels (both P > 0.0001) and lower fasting glucose (P = 0.001) and HOMA-IR (P = 0.06). The lifestyle intervention was associated with a decrease in magnitude of the effect of the 446L allele on triglyceride levels (interaction P = 0.04). Metformin was more effective in reducing HOMA-IR in carriers of the P446 allele (interaction P = 0.05). Conclusions: Intensive lifestyle intervention appears to partially mitigate the effect of the 446L allele on higher triglycerides, whereas the P446 allele appears to enhance responsiveness to the HOMA-IR-lowering effect of metformin.

Primary Author
Pollin,T. I.
Jablonski,K. A.
McAteer,J. B.
Saxena,R.
Kathiresan,S.
Kahn,S. E.
Goldberg,R. B.
Altshuler,D.
Florez,J. C.
for the Diabetes Prevention Program Research Group

Author Address
Division of Endocrinology, Diabetes, and Nutrition (T.I.P.), Department of Medicine, and Program in Genetics and Genomic Medicine, University of Maryland School of Medicine, Baltimore, Maryland 21201; The Biostatistics Center (K.A.J.), George Wa(TRUNCATED)

Volume
96

Issue
7

Start Page
E1142

Other Pages
E1147

Author Address
Division of Endocrinology, Diabetes, and Nutrition (T.I.P.), Department of Medicine, and Program in Genetics and Genomic Medicine, University of Maryland School of Medicine, Baltimore, Maryland 21201; The Biostatistics Center (K.A.J.), George Wa(TRUNCATED)

URL
http://jcem.endojournals.org/content/early/2011/04/27/jc.2010-2324

PMID
21525158

PMCID
PMC3205512



Reference Type
Journal Article

Periodical Full
The Journal of clinical endocrinology and metabolism

Publication Year
2011

Publication Date
Jul

ISSN/ISBN
1945-7197

Document Object Index
10.1210/jc.2010-2324

Accession Number
jc.2010-2324