Genetic Evidence for a Normal-Weight “Metabolically Obese” Phenotype Linking Insulin Resistance, Hypertension, Coronary Artery Disease, and Type 2 Diabetes

The mechanisms that predispose to hypertension, coronary artery disease (CAD), and type 2 diabetes (T2D) in individuals of normal weight are poorly understood. In contrast, in monogenic primary lipodystrophy—a reduction in subcutaneous adipose tissue—it is clear that it is adipose dysfunction that c...

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Autores principales: Yaghootkar, Hanieh, Scott, Robert A., White, Charles C., Zhang, Weihua, Speliotes, Elizabeth, Munroe, Patricia B., Ehret, Georg B., Bis, Joshua C., Fox, Caroline S., Walker, Mark, Borecki, Ingrid B., Knowles, Joshua W., Yerges-Armstrong, Laura, Ohlsson, Claes, Perry, John R.B., Chambers, John C., Kooner, Jaspal S., Franceschini, Nora, Langenberg, Claudia, Hivert, Marie-France, Dastani, Zari, Richards, J. Brent, Semple, Robert K., Frayling, Timothy M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Diabetes Association 2014
Materias:
Genetics/Genomes/Proteomics/Metabolomics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4392920/
https://www.ncbi.nlm.nih.gov/pubmed/25048195
http://dx.doi.org/10.2337/db14-0318
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author Yaghootkar, Hanieh
Scott, Robert A.
White, Charles C.
Zhang, Weihua
Speliotes, Elizabeth
Munroe, Patricia B.
Ehret, Georg B.
Bis, Joshua C.
Fox, Caroline S.
Walker, Mark
Borecki, Ingrid B.
Knowles, Joshua W.
Yerges-Armstrong, Laura
Ohlsson, Claes
Perry, John R.B.
Chambers, John C.
Kooner, Jaspal S.
Franceschini, Nora
Langenberg, Claudia
Hivert, Marie-France
Dastani, Zari
Richards, J. Brent
Semple, Robert K.
Frayling, Timothy M.
author_facet Yaghootkar, Hanieh
Scott, Robert A.
White, Charles C.
Zhang, Weihua
Speliotes, Elizabeth
Munroe, Patricia B.
Ehret, Georg B.
Bis, Joshua C.
Fox, Caroline S.
Walker, Mark
Borecki, Ingrid B.
Knowles, Joshua W.
Yerges-Armstrong, Laura
Ohlsson, Claes
Perry, John R.B.
Chambers, John C.
Kooner, Jaspal S.
Franceschini, Nora
Langenberg, Claudia
Hivert, Marie-France
Dastani, Zari
Richards, J. Brent
Semple, Robert K.
Frayling, Timothy M.
author_sort Yaghootkar, Hanieh
collection PubMed
description The mechanisms that predispose to hypertension, coronary artery disease (CAD), and type 2 diabetes (T2D) in individuals of normal weight are poorly understood. In contrast, in monogenic primary lipodystrophy—a reduction in subcutaneous adipose tissue—it is clear that it is adipose dysfunction that causes severe insulin resistance (IR), hypertension, CAD, and T2D. We aimed to test the hypothesis that common alleles associated with IR also influence the wider clinical and biochemical profile of monogenic IR. We selected 19 common genetic variants associated with fasting insulin–based measures of IR. We used hierarchical clustering and results from genome-wide association studies of eight nondisease outcomes of monogenic IR to group these variants. We analyzed genetic risk scores against disease outcomes, including 12,171 T2D cases, 40,365 CAD cases, and 69,828 individuals with blood pressure measurements. Hierarchical clustering identified 11 variants associated with a metabolic profile consistent with a common, subtle form of lipodystrophy. A genetic risk score consisting of these 11 IR risk alleles was associated with higher triglycerides (β = 0.018; P = 4 × 10(−29)), lower HDL cholesterol (β = −0.020; P = 7 × 10(−37)), greater hepatic steatosis (β = 0.021; P = 3 × 10(−4)), higher alanine transaminase (β = 0.002; P = 3 × 10(−5)), lower sex-hormone-binding globulin (β = −0.010; P = 9 × 10(−13)), and lower adiponectin (β = −0.015; P = 2 × 10(−26)). The same risk alleles were associated with lower BMI (per-allele β = −0.008; P = 7 × 10(−8)) and increased visceral-to-subcutaneous adipose tissue ratio (β = −0.015; P = 6 × 10(−7)). Individuals carrying ≥17 fasting insulin–raising alleles (5.5% population) were slimmer (0.30 kg/m(2)) but at increased risk of T2D (odds ratio [OR] 1.46; per-allele P = 5 × 10(−13)), CAD (OR 1.12; per-allele P = 1 × 10(−5)), and increased blood pressure (systolic and diastolic blood pressure of 1.21 mmHg [per-allele P = 2 × 10(−5)] and 0.67 mmHg [per-allele P = 2 × 10(−4)], respectively) compared with individuals carrying ≤9 risk alleles (5.5% population). Our results provide genetic evidence for a link between the three diseases of the “metabolic syndrome” and point to reduced subcutaneous adiposity as a central mechanism.
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spelling pubmed-43929202015-12-01 Genetic Evidence for a Normal-Weight “Metabolically Obese” Phenotype Linking Insulin Resistance, Hypertension, Coronary Artery Disease, and Type 2 Diabetes Yaghootkar, Hanieh Scott, Robert A. White, Charles C. Zhang, Weihua Speliotes, Elizabeth Munroe, Patricia B. Ehret, Georg B. Bis, Joshua C. Fox, Caroline S. Walker, Mark Borecki, Ingrid B. Knowles, Joshua W. Yerges-Armstrong, Laura Ohlsson, Claes Perry, John R.B. Chambers, John C. Kooner, Jaspal S. Franceschini, Nora Langenberg, Claudia Hivert, Marie-France Dastani, Zari Richards, J. Brent Semple, Robert K. Frayling, Timothy M. Diabetes Genetics/Genomes/Proteomics/Metabolomics The mechanisms that predispose to hypertension, coronary artery disease (CAD), and type 2 diabetes (T2D) in individuals of normal weight are poorly understood. In contrast, in monogenic primary lipodystrophy—a reduction in subcutaneous adipose tissue—it is clear that it is adipose dysfunction that causes severe insulin resistance (IR), hypertension, CAD, and T2D. We aimed to test the hypothesis that common alleles associated with IR also influence the wider clinical and biochemical profile of monogenic IR. We selected 19 common genetic variants associated with fasting insulin–based measures of IR. We used hierarchical clustering and results from genome-wide association studies of eight nondisease outcomes of monogenic IR to group these variants. We analyzed genetic risk scores against disease outcomes, including 12,171 T2D cases, 40,365 CAD cases, and 69,828 individuals with blood pressure measurements. Hierarchical clustering identified 11 variants associated with a metabolic profile consistent with a common, subtle form of lipodystrophy. A genetic risk score consisting of these 11 IR risk alleles was associated with higher triglycerides (β = 0.018; P = 4 × 10(−29)), lower HDL cholesterol (β = −0.020; P = 7 × 10(−37)), greater hepatic steatosis (β = 0.021; P = 3 × 10(−4)), higher alanine transaminase (β = 0.002; P = 3 × 10(−5)), lower sex-hormone-binding globulin (β = −0.010; P = 9 × 10(−13)), and lower adiponectin (β = −0.015; P = 2 × 10(−26)). The same risk alleles were associated with lower BMI (per-allele β = −0.008; P = 7 × 10(−8)) and increased visceral-to-subcutaneous adipose tissue ratio (β = −0.015; P = 6 × 10(−7)). Individuals carrying ≥17 fasting insulin–raising alleles (5.5% population) were slimmer (0.30 kg/m(2)) but at increased risk of T2D (odds ratio [OR] 1.46; per-allele P = 5 × 10(−13)), CAD (OR 1.12; per-allele P = 1 × 10(−5)), and increased blood pressure (systolic and diastolic blood pressure of 1.21 mmHg [per-allele P = 2 × 10(−5)] and 0.67 mmHg [per-allele P = 2 × 10(−4)], respectively) compared with individuals carrying ≤9 risk alleles (5.5% population). Our results provide genetic evidence for a link between the three diseases of the “metabolic syndrome” and point to reduced subcutaneous adiposity as a central mechanism. American Diabetes Association 2014-12 2014-11-13 /pmc/articles/PMC4392920/ /pubmed/25048195 http://dx.doi.org/10.2337/db14-0318 Text en © 2014 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered.
spellingShingle Genetics/Genomes/Proteomics/Metabolomics
Yaghootkar, Hanieh
Scott, Robert A.
White, Charles C.
Zhang, Weihua
Speliotes, Elizabeth
Munroe, Patricia B.
Ehret, Georg B.
Bis, Joshua C.
Fox, Caroline S.
Walker, Mark
Borecki, Ingrid B.
Knowles, Joshua W.
Yerges-Armstrong, Laura
Ohlsson, Claes
Perry, John R.B.
Chambers, John C.
Kooner, Jaspal S.
Franceschini, Nora
Langenberg, Claudia
Hivert, Marie-France
Dastani, Zari
Richards, J. Brent
Semple, Robert K.
Frayling, Timothy M.
Genetic Evidence for a Normal-Weight “Metabolically Obese” Phenotype Linking Insulin Resistance, Hypertension, Coronary Artery Disease, and Type 2 Diabetes
title Genetic Evidence for a Normal-Weight “Metabolically Obese” Phenotype Linking Insulin Resistance, Hypertension, Coronary Artery Disease, and Type 2 Diabetes
title_full Genetic Evidence for a Normal-Weight “Metabolically Obese” Phenotype Linking Insulin Resistance, Hypertension, Coronary Artery Disease, and Type 2 Diabetes
title_fullStr Genetic Evidence for a Normal-Weight “Metabolically Obese” Phenotype Linking Insulin Resistance, Hypertension, Coronary Artery Disease, and Type 2 Diabetes
title_full_unstemmed Genetic Evidence for a Normal-Weight “Metabolically Obese” Phenotype Linking Insulin Resistance, Hypertension, Coronary Artery Disease, and Type 2 Diabetes
title_short Genetic Evidence for a Normal-Weight “Metabolically Obese” Phenotype Linking Insulin Resistance, Hypertension, Coronary Artery Disease, and Type 2 Diabetes
title_sort genetic evidence for a normal-weight “metabolically obese” phenotype linking insulin resistance, hypertension, coronary artery disease, and type 2 diabetes
topic Genetics/Genomes/Proteomics/Metabolomics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4392920/
https://www.ncbi.nlm.nih.gov/pubmed/25048195
http://dx.doi.org/10.2337/db14-0318
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