Adiponectin polymorphisms, adiposity and insulin metabolism: HERITAGE family study and Oulu diabetic study

Olavi Ukkola; Merja Santaniemi; Tuomo Rankinen; Arthur S. Leon; James S. Skinner; Jack H. Wilmore; D. C. Rao; Richard Bergman; Y. Antero Kesäniemi; Claude Bouchard

doi:10.1080/07853890510007241

Adiponectin polymorphisms, adiposity and insulin metabolism: HERITAGE family study and Oulu diabetic study

Olavi Ukkola, Merja Santaniemi, Tuomo Rankinen, Arthur S. Leon, James S. Skinner, Jack H. Wilmore, D. C. Rao, Richard Bergman, Y. Antero Kesäniemi, Claude Bouchard

Kinesiology

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Abstract

Aims/hypothesis. Adiponectin is an adipocytokine with lowered blood levels in obesity and Type 2 diabetes mellitus. We sought to define the specific effects of different alleles of the gene encoding adiponectin. Methods. We studied the associations of adiponectin gene sequence variations with body fat distribution and insulin indices in 503 White and 276 Black subjects of the HERITAGE Family Study cohort and subjects from a Finnish population. Results. The His111 allele frequency of the Tyr111His polymorphism in Finnish Type 2 diabetic subjects (n=254) was higher (5.1%) than in control subjects (n=270) (2.6%; P=0.033). In the HERITAGE cohort, the His111 allele was associated with a lower insulin sensitivity index (P=0.018) and a higher acute insulin response to glucose (P=0.0098) in Whites. Other variants showed associations with adiposity and plasma lipid values only in Blacks. Among Blacks, the IVS2+G62T variant was associated with body fat (P=0.002) and total cholesterol values (P=0.005), and the Gly15Gly variant with cholesterol (P=0.009) and triglyceride (P=0.05) levels. The haplotype derived from these two polymorphisms was associated with total body fat, while the IVS2+G62T and Tyr111His-haplotype was associated with body fat and disposition index. Conclusions. The carriers of the His111 allele may have a higher risk of developing Type 2 diabetes mellitus. Racial differences were found between Blacks and Whites in body composition and lipids according to ACDC genotypes. Sequence variants in the adiponectin gene appear to be associated with diabetes and diabetes-related phenotypes.

Original language	English (US)
Pages (from-to)	141-150
Number of pages	10
Journal	Annals of Medicine
Volume	37
Issue number	2
DOIs	https://doi.org/10.1080/07853890510007241
State	Published - 2005

Bibliographical note

Funding Information:
The HERITAGE Family Study is supported by the National Heart, Lung, and Blood Institute through grants HL-45670 (C. Bouchard), HL-47323 (A. S. Leon), HL-47317 (D. C. Rao), HL-47327 (J. S. Skinner) and HL-47321 (J. H. Wilmore). This study was also supported by the Research Council for Health of the Academy of Finland. A.S. Leon is partially supported by the Henry L. Taylor endowed Professorship in Exercise Science and Health Enhancement. C. Bouchard is supported in part by the George A. Bray Chair in Nutrition.

Keywords

Adiponectin
Gene
Insulin sensitivity
Linkage
Type 2 diabetes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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title = "Adiponectin polymorphisms, adiposity and insulin metabolism: HERITAGE family study and Oulu diabetic study",

abstract = "Aims/hypothesis. Adiponectin is an adipocytokine with lowered blood levels in obesity and Type 2 diabetes mellitus. We sought to define the specific effects of different alleles of the gene encoding adiponectin. Methods. We studied the associations of adiponectin gene sequence variations with body fat distribution and insulin indices in 503 White and 276 Black subjects of the HERITAGE Family Study cohort and subjects from a Finnish population. Results. The His111 allele frequency of the Tyr111His polymorphism in Finnish Type 2 diabetic subjects (n=254) was higher (5.1%) than in control subjects (n=270) (2.6%; P=0.033). In the HERITAGE cohort, the His111 allele was associated with a lower insulin sensitivity index (P=0.018) and a higher acute insulin response to glucose (P=0.0098) in Whites. Other variants showed associations with adiposity and plasma lipid values only in Blacks. Among Blacks, the IVS2+G62T variant was associated with body fat (P=0.002) and total cholesterol values (P=0.005), and the Gly15Gly variant with cholesterol (P=0.009) and triglyceride (P=0.05) levels. The haplotype derived from these two polymorphisms was associated with total body fat, while the IVS2+G62T and Tyr111His-haplotype was associated with body fat and disposition index. Conclusions. The carriers of the His111 allele may have a higher risk of developing Type 2 diabetes mellitus. Racial differences were found between Blacks and Whites in body composition and lipids according to ACDC genotypes. Sequence variants in the adiponectin gene appear to be associated with diabetes and diabetes-related phenotypes.",

keywords = "Adiponectin, Gene, Insulin sensitivity, Linkage, Type 2 diabetes",

author = "Olavi Ukkola and Merja Santaniemi and Tuomo Rankinen and Leon, {Arthur S.} and Skinner, {James S.} and Wilmore, {Jack H.} and Rao, {D. C.} and Richard Bergman and Kes{\"a}niemi, {Y. Antero} and Claude Bouchard",

note = "Funding Information: The HERITAGE Family Study is supported by the National Heart, Lung, and Blood Institute through grants HL-45670 (C. Bouchard), HL-47323 (A. S. Leon), HL-47317 (D. C. Rao), HL-47327 (J. S. Skinner) and HL-47321 (J. H. Wilmore). This study was also supported by the Research Council for Health of the Academy of Finland. A.S. Leon is partially supported by the Henry L. Taylor endowed Professorship in Exercise Science and Health Enhancement. C. Bouchard is supported in part by the George A. Bray Chair in Nutrition.",

year = "2005",

doi = "10.1080/07853890510007241",

language = "English (US)",

volume = "37",

pages = "141--150",

journal = "Annals of Medicine",

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T1 - Adiponectin polymorphisms, adiposity and insulin metabolism

T2 - HERITAGE family study and Oulu diabetic study

AU - Ukkola, Olavi

AU - Santaniemi, Merja

AU - Rankinen, Tuomo

AU - Leon, Arthur S.

AU - Skinner, James S.

AU - Wilmore, Jack H.

AU - Rao, D. C.

AU - Bergman, Richard

AU - Kesäniemi, Y. Antero

AU - Bouchard, Claude

N1 - Funding Information: The HERITAGE Family Study is supported by the National Heart, Lung, and Blood Institute through grants HL-45670 (C. Bouchard), HL-47323 (A. S. Leon), HL-47317 (D. C. Rao), HL-47327 (J. S. Skinner) and HL-47321 (J. H. Wilmore). This study was also supported by the Research Council for Health of the Academy of Finland. A.S. Leon is partially supported by the Henry L. Taylor endowed Professorship in Exercise Science and Health Enhancement. C. Bouchard is supported in part by the George A. Bray Chair in Nutrition.

PY - 2005

Y1 - 2005

N2 - Aims/hypothesis. Adiponectin is an adipocytokine with lowered blood levels in obesity and Type 2 diabetes mellitus. We sought to define the specific effects of different alleles of the gene encoding adiponectin. Methods. We studied the associations of adiponectin gene sequence variations with body fat distribution and insulin indices in 503 White and 276 Black subjects of the HERITAGE Family Study cohort and subjects from a Finnish population. Results. The His111 allele frequency of the Tyr111His polymorphism in Finnish Type 2 diabetic subjects (n=254) was higher (5.1%) than in control subjects (n=270) (2.6%; P=0.033). In the HERITAGE cohort, the His111 allele was associated with a lower insulin sensitivity index (P=0.018) and a higher acute insulin response to glucose (P=0.0098) in Whites. Other variants showed associations with adiposity and plasma lipid values only in Blacks. Among Blacks, the IVS2+G62T variant was associated with body fat (P=0.002) and total cholesterol values (P=0.005), and the Gly15Gly variant with cholesterol (P=0.009) and triglyceride (P=0.05) levels. The haplotype derived from these two polymorphisms was associated with total body fat, while the IVS2+G62T and Tyr111His-haplotype was associated with body fat and disposition index. Conclusions. The carriers of the His111 allele may have a higher risk of developing Type 2 diabetes mellitus. Racial differences were found between Blacks and Whites in body composition and lipids according to ACDC genotypes. Sequence variants in the adiponectin gene appear to be associated with diabetes and diabetes-related phenotypes.

AB - Aims/hypothesis. Adiponectin is an adipocytokine with lowered blood levels in obesity and Type 2 diabetes mellitus. We sought to define the specific effects of different alleles of the gene encoding adiponectin. Methods. We studied the associations of adiponectin gene sequence variations with body fat distribution and insulin indices in 503 White and 276 Black subjects of the HERITAGE Family Study cohort and subjects from a Finnish population. Results. The His111 allele frequency of the Tyr111His polymorphism in Finnish Type 2 diabetic subjects (n=254) was higher (5.1%) than in control subjects (n=270) (2.6%; P=0.033). In the HERITAGE cohort, the His111 allele was associated with a lower insulin sensitivity index (P=0.018) and a higher acute insulin response to glucose (P=0.0098) in Whites. Other variants showed associations with adiposity and plasma lipid values only in Blacks. Among Blacks, the IVS2+G62T variant was associated with body fat (P=0.002) and total cholesterol values (P=0.005), and the Gly15Gly variant with cholesterol (P=0.009) and triglyceride (P=0.05) levels. The haplotype derived from these two polymorphisms was associated with total body fat, while the IVS2+G62T and Tyr111His-haplotype was associated with body fat and disposition index. Conclusions. The carriers of the His111 allele may have a higher risk of developing Type 2 diabetes mellitus. Racial differences were found between Blacks and Whites in body composition and lipids according to ACDC genotypes. Sequence variants in the adiponectin gene appear to be associated with diabetes and diabetes-related phenotypes.

KW - Adiponectin

KW - Gene

KW - Insulin sensitivity

KW - Linkage

KW - Type 2 diabetes

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Adiponectin polymorphisms, adiposity and insulin metabolism: HERITAGE family study and Oulu diabetic study

Abstract

Bibliographical note

Keywords

UN SDGs

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