Chromosome 4q locus associated with insulin resistance in Pima Indians: Studies in three European NIDDM populations
Chromosome 4q locus associated with insulin resistance in Pima Indians: Studies in three European NIDDM populations
Markers on chromosome 4q have recently been shown to be associated with insulin resistance in Pima Indians, a population in which insulin resistance precedes and predicts the development of non-insulin-dependent diabetes mellitus (NIDDM). To examine whether genes in this region could play a major role in susceptibility to NIDDM in other populations, we have examined the allele frequencies of a trinucleotide repeat near the fatty acid-binding protein 2 (FABP2) gene on 4q28-31 in three European populations: Finnish, U.K. Caucasian, and Welsh. The U.K. NIDDM population was selected for insulin resistance by studying patients whose obesity-corrected fasting plasma insulin before treatment was above the 98th percentile. Seven alleles were detected. On cross-tabulation analysis, there were no significant associations between allele frequencies and glucose intolerance in any of the populations. Log-linear analysis of the results from all three populations suggested a moderately significant interaction of glucose tolerance status (normal versus diabetic) and the FABP2 allele (partial χ2 = 24, df 6, P = 0.027). The parameter describing the interaction of allele A3 and glucose tolerance status was the only such parameter differing significantly from zero (z-score +2.003, P = 0.046). In both the Finnish and U.K. population, the A3 allele was found approximately twice as frequently in NIDDM than in control subjects (Finnish control subjects, impaired glucose tolerance, and NIDDM: 12.2, 22.4, and 26.6%, respectively; U.K. control subjects and NIDDM: 7.8 and 14.6%, respectively). In the Finnish populations, no associations were found between FABP2 alleles and plasma insulin levels or with homeostatic model assessment (HOMA) estimates of β-cell function and insulin sensitivity. Specific comparison of those subjects with and without the A3 allele revealed no difference in fasting (47.4 [36-61.8] vs. 47.4 [39-57] pM, geometric means and 95% confidence interval, NS) and 2-h (288 [222.6-373.2] vs. 297 [252.6-349.2] pM, NS) insulin or in insulin sensitivity as assessed by HOMA (47.6 [32.3-70.3] vs. 50.5 [39.8-64.2]%, NS). Similarly, in the U.K. NIDDM population, no differences in clinical or metabolic characteristics were found between those with and those without the A3 allele. In summary, in three European Caucasian populations, there is no evidence for a major genetic influence of the FABP2 locus on the development of diabetes. The weak association of the A3 allele with diabetes does not appear to be because of an effect of this allele on insulin resistance.
800-804
Humphreys, Phillippa
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McCarthy, Mark
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Tuomilehto, Jaakko
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Tuomilehto-Wolf, Eva
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Stratton, Irene
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Morgan, Ruth
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Rees, Alan
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Owens, David
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Stengård, Jari
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Nissinen, Aulikki
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Hitman, Graham
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Turner, Robert C.
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O'Rahilly, Stephen
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1994
Humphreys, Phillippa
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McCarthy, Mark
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Tuomilehto, Jaakko
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Tuomilehto-Wolf, Eva
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Stratton, Irene
772f25b9-23c0-4240-a3f6-1e76b03b172f
Morgan, Ruth
fb10246b-58ac-471a-adbf-048ac04e4d91
Rees, Alan
44638bbf-10f0-4bc0-9bb9-8c4ca90ba343
Owens, David
0d0eb9da-c362-457d-841f-3094a18120ee
Stengård, Jari
de6882dd-ccfd-4826-8f6a-94dd154e4bc2
Nissinen, Aulikki
97b355e6-623d-4b23-81d9-9fa47e603d3c
Hitman, Graham
30a1c858-bc1d-48e7-b478-613cd580dcda
Turner, Robert C.
f974acc5-a17a-49c4-8bb7-84fa4d449863
O'Rahilly, Stephen
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Humphreys, Phillippa, McCarthy, Mark, Tuomilehto, Jaakko, Tuomilehto-Wolf, Eva, Stratton, Irene, Morgan, Ruth, Rees, Alan, Owens, David, Stengård, Jari, Nissinen, Aulikki, Hitman, Graham, Turner, Robert C. and O'Rahilly, Stephen
(1994)
Chromosome 4q locus associated with insulin resistance in Pima Indians: Studies in three European NIDDM populations.
Diabetes, 43 (6), .
(doi:10.2337/diab.43.6.800).
Abstract
Markers on chromosome 4q have recently been shown to be associated with insulin resistance in Pima Indians, a population in which insulin resistance precedes and predicts the development of non-insulin-dependent diabetes mellitus (NIDDM). To examine whether genes in this region could play a major role in susceptibility to NIDDM in other populations, we have examined the allele frequencies of a trinucleotide repeat near the fatty acid-binding protein 2 (FABP2) gene on 4q28-31 in three European populations: Finnish, U.K. Caucasian, and Welsh. The U.K. NIDDM population was selected for insulin resistance by studying patients whose obesity-corrected fasting plasma insulin before treatment was above the 98th percentile. Seven alleles were detected. On cross-tabulation analysis, there were no significant associations between allele frequencies and glucose intolerance in any of the populations. Log-linear analysis of the results from all three populations suggested a moderately significant interaction of glucose tolerance status (normal versus diabetic) and the FABP2 allele (partial χ2 = 24, df 6, P = 0.027). The parameter describing the interaction of allele A3 and glucose tolerance status was the only such parameter differing significantly from zero (z-score +2.003, P = 0.046). In both the Finnish and U.K. population, the A3 allele was found approximately twice as frequently in NIDDM than in control subjects (Finnish control subjects, impaired glucose tolerance, and NIDDM: 12.2, 22.4, and 26.6%, respectively; U.K. control subjects and NIDDM: 7.8 and 14.6%, respectively). In the Finnish populations, no associations were found between FABP2 alleles and plasma insulin levels or with homeostatic model assessment (HOMA) estimates of β-cell function and insulin sensitivity. Specific comparison of those subjects with and without the A3 allele revealed no difference in fasting (47.4 [36-61.8] vs. 47.4 [39-57] pM, geometric means and 95% confidence interval, NS) and 2-h (288 [222.6-373.2] vs. 297 [252.6-349.2] pM, NS) insulin or in insulin sensitivity as assessed by HOMA (47.6 [32.3-70.3] vs. 50.5 [39.8-64.2]%, NS). Similarly, in the U.K. NIDDM population, no differences in clinical or metabolic characteristics were found between those with and those without the A3 allele. In summary, in three European Caucasian populations, there is no evidence for a major genetic influence of the FABP2 locus on the development of diabetes. The weak association of the A3 allele with diabetes does not appear to be because of an effect of this allele on insulin resistance.
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Published date: 1994
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Local EPrints ID: 486943
URI: http://eprints.soton.ac.uk/id/eprint/486943
ISSN: 0012-1797
PURE UUID: 8472d7f2-3ba2-4e03-aece-6a83c71f96b0
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Date deposited: 08 Feb 2024 17:45
Last modified: 18 Mar 2024 04:01
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Author:
Phillippa Humphreys
Author:
Mark McCarthy
Author:
Jaakko Tuomilehto
Author:
Eva Tuomilehto-Wolf
Author:
Irene Stratton
Author:
Ruth Morgan
Author:
Alan Rees
Author:
David Owens
Author:
Jari Stengård
Author:
Aulikki Nissinen
Author:
Graham Hitman
Author:
Robert C. Turner
Author:
Stephen O'Rahilly
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