Variants of CDKAL1 and IGF2BP2 affect first-phase insulin secretion during hyperglycaemic clamps

M. J. Groenewoud, J. M. Dekker, A. Fritsche, E. Reiling, G. Nijpels, R. J. Heine, J. A. Maassen, F. Machicao, S. A. Schäfer and H. U. Häring, et al.

View Related Documents

Journal Article
Impaired glucagon-like peptide-1-induced insulin secretion in carriers of transcription factor 7-like 2 (TCF7L2) gene polymorphisms
S. A. Schäfer, O. Tschritter, F. Machicao, C. Thamer and N. Stefan, et al.
Diabetologia, 2007, Volume 50, Number 12, Pages 2443-2450
Journal Article
A common genetic variant in WFS1 determines impaired glucagon-like peptide-1-induced insulin secretion
S. A. Schäfer, K. Müssig, H. Staiger, F. Machicao and N. Stefan, et al.
Diabetologia, 2009, Volume 52, Number 6, Pages 1075-1082
Journal Article
Open Access
Variants in KCNQ1 are associated with susceptibility to type 2 diabetes in the population of mainland China
Y. Liu, D. Z. Zhou, D. Zhang, Z. Chen and T. Zhao, et al.
Diabetologia, 2009, Volume 52, Number 7, Pages 1315-1321
Journal Article
Newly identified loci highlight beta cell dysfunction as a key cause of type 2 diabetes: Where are the insulin resistance genes?
J. C. Florez
Diabetologia, 2008, Volume 51, Number 7, Pages 1100-1110
- Download PDF (281.8 KB)
- View HTML
Journal Article
The T allele of rs7903146 TCF7L2 is associated with impaired insulinotropic action of incretin hormones, reduced 24 h profiles of plasma insulin and glucagon, and increased hepatic glucose production in young healthy men
K. Pilgaard, C. B. Jensen, J. H. Schou, V. Lyssenko and L. Wegner, et al.
Diabetologia, 2009, Volume 52, Number 7, Pages 1298-1307
Book Chapter
Genetics of Type 2 Diabetes: From Candidate Genes to Genome-Wide Association Analysis
Kevin Brown and Alan R. Shuldiner
2010, Principles of Diabetes Mellitus, 4, Pages 147-163
- Download PDF (1.5 MB)
- View HTML
Journal Article
Beta cell glucose sensitivity is decreased by 39% in non-diabetic individuals carrying multiple diabetes-risk alleles compared with those with no risk alleles
L. Pascoe, T. M. Frayling, M. N. Weedon, A. Mari and A. Tura, et al.
Diabetologia, 2008, Volume 51, Number 11, Pages 1989-1992
Journal Article
Open Access
Implication of genetic variants near SLC30A8, HHEX, CDKAL1, CDKN2A/B, IGF2BP2, FTO, TCF2, KCNQ1, and WFS1 in Type 2 Diabetes in a Chinese population
Xueyao Han, Yingying Luo, Qian Ren, Xiuying Zhang and Fang Wang, et al.
BMC Medical Genetics, 2010, Volume 11, Number 1, 81
Journal Article
Type 2 diabetes risk alleles near ADCY5, CDKAL1 and HHEX-IDE are associated with reduced birthweight
E. A. Andersson, K. Pilgaard, C. Pisinger, M. N. Harder and N. Grarup, et al.
Diabetologia, 2010, Volume 53, Number 9, Pages 1908-1916
Journal Article
Sideways Glance: Genome wide association studies for type 2 diabetes mellitus
Yula Sambuy
Genes & Nutrition, 2007, Volume 2, Number 3, Pages 245-248
- Download PDF (117.1 KB)
- View HTML

Abstract

Aims/hypothesis

Genome-wide association studies have recently identified novel type 2 diabetes susceptibility gene regions. We assessed the effects of six of these regions on insulin secretion as determined by a hyperglycaemic clamp.

Methods

Variants of the HHEX/IDE, CDKAL1, SLC30A8, IGF2BP2 and CDKN2A/CDKN2B genes were genotyped in a cohort of 146 participants with NGT and 126 with IGT from the Netherlands and Germany, who all underwent a hyperglycaemic clamp at 10 mmol/l glucose.

Results

Variants of CDKAL1 and IGF2BP2 were associated with reductions in first-phase insulin secretion (34% and 28%, respectively). The disposition index was also significantly reduced. For gene regions near HHEX/IDE, SLC30A8 and CDKN2A/CDKN2B we did not find significant associations with first-phase insulin secretion (7–18% difference between genotypes; all p > 0.3). None of the variants showed a significant effect on second-phase insulin secretion in our cohorts (2–8% difference between genotypes, all p > 0.3). Furthermore, the gene variants were not associated with the insulin sensitivity index.

Conclusions

Variants of CDKAL1 and IGF2BP2 attenuate the first phase of glucose-stimulated insulin secretion but show no effect on the second phase of insulin secretion. Our results, based on hyperglycaemic clamps, provide further insight into the pathogenic mechanism behind the association of these gene variants with type 2 diabetes.

Keywords CDKAL1 - First phase insulin secretion - Genes - Gene variants - Hyperglycaemic clamp - IGF2BP2 - Type 2 diabetes

L. M. ’t Hart and T. W. van Haeften contributed equally to this study.

Fulltext Preview

Image of the first page of the fulltext document

Frequently asked questions General info on journals and books Send us your feedback Impressum Contact us

SpringerLink