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UKPDS 19: heterogeneity in NIDDM: separate contributions of IRS-1 and b3-adrenergic-receptor mutations to insulin resistance and obesity respectively with no evidence for glycogen synthase gene mutations

UKPDS 19: heterogeneity in NIDDM: separate contributions of IRS-1 and b3-adrenergic-receptor mutations to insulin resistance and obesity respectively with no evidence for glycogen synthase gene mutations
UKPDS 19: heterogeneity in NIDDM: separate contributions of IRS-1 and b3-adrenergic-receptor mutations to insulin resistance and obesity respectively with no evidence for glycogen synthase gene mutations

Insulin receptor substrate-1 (IRS-1), β3-adrenergic-receptor (β3-AR) and glycogen synthase (GS) genes are candidate genes for non-insulin-dependent diabetes mellitus (NIDDM), insulin resistance, dyslipidaemia and obesity. We studied white Caucasian subjects with NIDDM, 227 being randomly selected, 49 NIDDM within the top two percentiles of insulin resistance; 54 with dyslipidaemia in the top quintile of triglyceride/insulin and the bottom quintile of HDL, and 166 non-diabetic control subjects. We examined the association of the simple tandem repeat DNA polymorphisms (STRPs) near the IRS-1 and GS genes, and the prevalence of mutations at codons of IRS-1 513 and 972, β3-AR 64 and GS 464 using restriction fragment length polymorphism (RFLP). The STRP alleles in IRS-1 were significantly different between NIDDM and control subjects (p = 0.015). The IRS-1 972 mutation was significantly different between the four groups with increased prevalence in the insulin resistant and dyslipidaemia subjects (18 and 26% compared with 11% in control subjects; p < 0.0005). Thoese with or without IRS-1 mutations had similar clinical characteristics and impaired insulin sensitivity. β3-AR 64 mutation was not significantly different between the four groups but those with the mutation were more obese, with a test for linear association between number of alleles and degree of obesity in an analysis of variance showing a significant association (p = 0.029). The GS 464 mutation was not detected in any of the diabetic or control subjects and the population association study using GS STRP showed no difference in allelic frequencies between NIDDM patients and control subjects. A mutation in lipoprotein lipase at codon 291, associated in the general population with low HDL cholesterol, was not at increased prevalence in the NIDDM patients with dyslipidaemia. In conclusion, IRS-1 972 had an increased prevalence in subjects with insulin resistance, with or without dyslipidaemia. β3-AR 64 was associated with increased obesity but not with insulin resistance or dyslipidaemia. These separate contributions to different features of NIDDM are an example of the polygenic inheritance of this heterogeneous disorder.

β3-adrenergic-receptor, dyslipidaemia, glycogen synthase, insulin receptor substrate-1, insulin resistance, lipoprotein lipase
0012-186X
1505-1511
Zhang, Y.
f812509d-2a3c-41aa-8ba1-68210952d5a6
Wat, N.
3b3bf82f-c5d6-47a4-9d17-a830479bf3f9
Stratton, I.M.
772f25b9-23c0-4240-a3f6-1e76b03b172f
Warren-Perry, M.G.
5e2b05c6-5c32-4e17-9e66-3dab28d1e589
Orho, M.
b8b479a6-52cb-4010-a1cb-717f1d8b095a
Groop, L.
5f0d3a41-aaf8-41f6-aa9e-472f56fceab7
Turner, R.C.
d04d8425-6d8d-4042-a5e6-ca25b4d2d894
Zhang, Y.
f812509d-2a3c-41aa-8ba1-68210952d5a6
Wat, N.
3b3bf82f-c5d6-47a4-9d17-a830479bf3f9
Stratton, I.M.
772f25b9-23c0-4240-a3f6-1e76b03b172f
Warren-Perry, M.G.
5e2b05c6-5c32-4e17-9e66-3dab28d1e589
Orho, M.
b8b479a6-52cb-4010-a1cb-717f1d8b095a
Groop, L.
5f0d3a41-aaf8-41f6-aa9e-472f56fceab7
Turner, R.C.
d04d8425-6d8d-4042-a5e6-ca25b4d2d894

Zhang, Y., Wat, N., Stratton, I.M., Warren-Perry, M.G., Orho, M., Groop, L. and Turner, R.C. (1996) UKPDS 19: heterogeneity in NIDDM: separate contributions of IRS-1 and b3-adrenergic-receptor mutations to insulin resistance and obesity respectively with no evidence for glycogen synthase gene mutations. Diabetologia, 39 (12), 1505-1511. (doi:10.1007/s001250050605).

Record type: Article

Abstract

Insulin receptor substrate-1 (IRS-1), β3-adrenergic-receptor (β3-AR) and glycogen synthase (GS) genes are candidate genes for non-insulin-dependent diabetes mellitus (NIDDM), insulin resistance, dyslipidaemia and obesity. We studied white Caucasian subjects with NIDDM, 227 being randomly selected, 49 NIDDM within the top two percentiles of insulin resistance; 54 with dyslipidaemia in the top quintile of triglyceride/insulin and the bottom quintile of HDL, and 166 non-diabetic control subjects. We examined the association of the simple tandem repeat DNA polymorphisms (STRPs) near the IRS-1 and GS genes, and the prevalence of mutations at codons of IRS-1 513 and 972, β3-AR 64 and GS 464 using restriction fragment length polymorphism (RFLP). The STRP alleles in IRS-1 were significantly different between NIDDM and control subjects (p = 0.015). The IRS-1 972 mutation was significantly different between the four groups with increased prevalence in the insulin resistant and dyslipidaemia subjects (18 and 26% compared with 11% in control subjects; p < 0.0005). Thoese with or without IRS-1 mutations had similar clinical characteristics and impaired insulin sensitivity. β3-AR 64 mutation was not significantly different between the four groups but those with the mutation were more obese, with a test for linear association between number of alleles and degree of obesity in an analysis of variance showing a significant association (p = 0.029). The GS 464 mutation was not detected in any of the diabetic or control subjects and the population association study using GS STRP showed no difference in allelic frequencies between NIDDM patients and control subjects. A mutation in lipoprotein lipase at codon 291, associated in the general population with low HDL cholesterol, was not at increased prevalence in the NIDDM patients with dyslipidaemia. In conclusion, IRS-1 972 had an increased prevalence in subjects with insulin resistance, with or without dyslipidaemia. β3-AR 64 was associated with increased obesity but not with insulin resistance or dyslipidaemia. These separate contributions to different features of NIDDM are an example of the polygenic inheritance of this heterogeneous disorder.

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More information

Published date: November 1996
Keywords: β3-adrenergic-receptor, dyslipidaemia, glycogen synthase, insulin receptor substrate-1, insulin resistance, lipoprotein lipase

Identifiers

Local EPrints ID: 487085
URI: http://eprints.soton.ac.uk/id/eprint/487085
DOI: doi:10.1007/s001250050605
ISSN: 0012-186X
PURE UUID: edb701db-b5fb-486d-912d-80317b47f6c4
ORCID for I.M. Stratton: ORCID iD orcid.org/0000-0003-1172-7865

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Date deposited: 13 Feb 2024 17:31
Last modified: 12 Nov 2024 03:06

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Contributors

Author: Y. Zhang
Author: N. Wat
Author: I.M. Stratton ORCID iD
Author: M.G. Warren-Perry
Author: M. Orho
Author: L. Groop
Author: R.C. Turner

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