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1. The interaction of GSK3B and FXR1 genotypes may influence the mania and depression dimensions in mood disorders

Author

Alexandre Bureau, Thomas Paccalet, Yvon C. Chagnon, Jean-Martin Beaulieu, and Michel Maziade

Subjects
0301 basic medicine, Adult, Male, medicine.medical_specialty, Bipolar Disorder, Genotype, Schizoaffective disorder, Lithium, behavioral disciplines and activities, 03 medical and health sciences, 0302 clinical medicine, mental disorders, medicine, Prevalence, Humans, Bipolar disorder, Age of Onset, Psychiatry, Depressive Disorder, Major, Glycogen Synthase Kinase 3 beta, Polymorphism, Genetic, Mood Disorders, RNA-Binding Proteins, Middle Aged, medicine.disease, Diagnostic and Statistical Manual of Mental Disorders, Psychiatry and Mental health, Clinical Psychology, 030104 developmental biology, Mood, Mood disorders, Schizophrenia, Endogenous depression, Female, Age of onset, medicine.symptom, Psychology, Mania, 030217 neurology & neurosurgery
Abstract

Background Previous evidence in healthy subjects suggested that functional polymorphisms GSK3B rs12630592 and FXR1 rs496250 interact in regulating mood and emotional processing. We attempted to replicate this interaction primarily on manic and depressive dimensions in mood disorder patients, and secondarily on schizophrenia patients, diagnosis itself and age of onset. Methods Symptom dimensions were derived from the Comprehensive Assessment of Symptoms and History 82 items rated lifetime in acute episodes and stabilized interepisode intervals in 384 patients from the Schizophrenia and Bipolar Disorder Eastern Quebec Kindred Study. Linear mixed effect models of symptom dimensions included rs12630592-rs496250 main and interaction fixed effects (obtained from TaqMan genotypes), and a polygenic random effect. The distribution of lifetime best-estimate DSM-IV diagnosis of 855 kindred members was studied versus genotype under a polytomous logistic model. Results In mood disorder patients, the level of mania (in both acute and stabilized periods) and depression in stabilized periods was positively associated with GSK3B rs12630592 T only in FXR1 rs496250 A-allele carriers (Bonferroni-corrected interaction p=0.024, 0.052 and 0.017 respectively). The two polymorphisms explained 11% of mania variance and 5% of interepisode depression variance. The association was observed neither in schizophrenia patients nor with the psychotic dimension in mood disorder patients. Interaction with the diagnosis distribution (p=0.03) was driven by the decreasing prevalence of recurrent major depression with rs12630592 T also only in carriers of rs496250 A. Limitations Sample size was limited, but power was sufficient to detect the tested interaction effect in this replication sample. Conclusions We replicate in affective patients an interaction between the FXR1 rs496250 and GSK3B rs12630592 polymorphisms in regulating mood dimensions.

Published
2017

2. Follow-up of a Major Psychosis Linkage Site in 13q13-q14 Reveals Significant Association in Both Case-Control and Family Samples

Author

Yvon C. Chagnon, Jordie Croteau, Michel Maziade, Chantal Mérette, Alexandre Bureau, Thomas Paccalet, Marc-André Roy, and Alain Fournier

Subjects
Male, Oncology, medicine.medical_specialty, Psychosis, Genetic Linkage, Population, Schizoaffective disorder, Single-nucleotide polymorphism, Article, Internal medicine, medicine, Humans, Family, Bipolar disorder, education, Biological Psychiatry, Genetic association, Genetics, education.field_of_study, Chromosomes, Human, Pair 13, Quebec, Odds ratio, medicine.disease, Psychotic Disorders, Case-Control Studies, Female, Age of onset, Psychology
Abstract

Background We previously reported a genome-wide significant linkage for major psychosis in chromosome 13q13-q14. Methods An association analysis was conducted in 247 unrelated DSM-IV schizophrenia (SZ) patients and 250 unrelated control subjects from the Eastern Quebec population genotyped with 2150 single nucleotide polymorphisms in 13q13-q14. We also used the kindred sample where linkage was detected (125 SZ, 120 bipolar disorder [BD] and 36 schizoaffective disorder patients vs. 467 unaffected adult relatives) for replication. Results An association of the T allele of rs1156026 found in the case-control sample (odds ratio [OR] = 1.81, p = 4×10 −6 , false discovery rate=.01) was replicated in the kindred sample (OR = 1.54, p = .01), strengthening the overall association evidence ( p = 8×10 −7 ). The effect size increased in the subset of unrelated patients with a family history (OR = 2.28) and in the 15 families where SZ was predominant (OR = 2.03). In the kindred sample, onset of either SZ or BD was, on average, 5 years earlier for T/T compared with C/C homozygotes, leading to stronger association in patients with onset before 26 years of age (SZ: OR=2.40, p = 1.3×10 −4 ; SZ, BD, and schizoaffective disorder combined: OR=1.87, p = 8×10 −5 ). Conclusions Case-control and family-based association provided evidence of a locus at 13q13-q14 related to SZ. The proximity of the associated single nucleotide polymorphism with the linkage signal and the extension of the associated phenotype to major psychosis with younger age of onset indicate congruence between the linkage and association signals. The rs1156026 association is novel and factors explaining its nondetection in previous studies are discussed.

Published
2013

3. Scientific Reports

Author

Philip L. Jackson, Catherine Mercier, Sébastien Hétu, Shirley Fecteau, Yvon C. Chagnon, Elsa Massicotte, Pierre-Emmanuel Michon, Louis De Beaumont, Vincent Taschereau-Dumouchel, Etienne Vachon-Presseau, and Judes Poirier

Subjects
Adult, Male, Candidate gene, critical-period, Genotype, motor facilitation, val66met polymorphism, Polymorphism, Single Nucleotide, stimulation, 050105 experimental psychology, Article, 03 medical and health sciences, Young Adult, visual-cortex, 0302 clinical medicine, activity-dependent secretion, Genetic variation, medicine, Humans, 0501 psychology and cognitive sciences, Allele, Evoked Potentials, Mirror Neurons, Mirror neuron, Alleles, mirror neurons, Multidisciplinary, Brain-Derived Neurotrophic Factor, 05 social sciences, Homozygote, Genetic Variation, inhibition, Associative learning, Visual cortex, medicine.anatomical_structure, plasticity, Facilitation, Female, Psychology, Motor learning, Neuroscience, 030217 neurology & neurosurgery, Simulation
Abstract

Motor representations in the human mirror neuron system are tuned to respond to specific observed actions. This ability is widely believed to be influenced by genetic factors, but no study has reported a genetic variant affecting this system so far. One possibility is that genetic variants might interact with visuomotor associative learning to configure the system to respond to novel observed actions. In this perspective, we conducted a candidate gene study on the Brain-derived neurotrophic factor (BDNF) Val(66)Met polymorphism, a genetic variant linked to motor learning in regions of the mirror neuron system, and tested the effect of this polymorphism on motor facilitation and visuomotor associative learning. In a single-pulse TMS study carried on 16 Met (Val/Met and Met/Met) and 16 Val/Val participants selected from a large pool of healthy volunteers, Met participants showed significantly less muscle-specific corticospinal sensitivity during action observation, as well as reduced visuomotor associative learning, compared to Val homozygotes. These results are the first evidence of a genetic variant tuning sensitivity to action observation and bring to light the importance of considering the intricate relation between genetics and associative learning in order to further understand the origin and function of the human mirror neuron system. National Science and Engineering Research Council (NSERC); Quebec Bio-Imaging Network (QBIN); NSERC; Centre thematique de recherche en neurosciences; Canadian Institutes of Health Research (CIHR); Fond de recherche Quebec - Sante (FRQS); New Investigator Awards from CIHR; Chercheur-Boursier Senior Awards from FRQS This work was supported by grants from the National Science and Engineering Research Council (NSERC) and from the Quebec Bio-Imaging Network (QBIN). Vincent Taschereau-Dumouchel was supported by scholarships from the NSERC, the Centre thematique de recherche en neurosciences and the Canadian Institutes of Health Research (CIHR). Sebastien Hetu was supported by scholarship from the Fond de recherche Quebec - Sante (FRQS) and CIHR. Philip L. Jackson and Catherine Mercier were supported by New Investigator Awards from the CIHR and Chercheur-Boursier Senior Awards from the FRQS. The authors declare no conflict of interest. We thank Michel-Pierre Coll, Mathieu Gregoire and professor Tim Welsh of the University of Toronto, for stimulating discussions on this topic.

Published
2016

4. BDNF Val66Met Polymorphism Is Associated with Self-Reported Empathy

Author

Sébastien Hétu, Alexandre Labrecque, Anaït Bagramian, Yvon C. Chagnon, Marion Racine, Philip L. Jackson, and Vincent Taschereau-Dumouchel

Subjects
Social Cognition, Male, Heredity, Emotions, Social Sciences, lcsh:Medicine, 0302 clinical medicine, Cognition, Emotion perception, Surveys and Questionnaires, Medicine and Health Sciences, Psychology, lcsh:Science, media_common, Multidisciplinary, 05 social sciences, Brain, Amygdala, Genetic Mapping, Interpersonal Reactivity Index, Female, Anatomy, Clinical psychology, Research Article, Adult, Genotype, media_common.quotation_subject, Empathy, Single-nucleotide polymorphism, Variant Genotypes, Polymorphism, Single Nucleotide, 050105 experimental psychology, 03 medical and health sciences, Young Adult, Social cognition, Genetics, Humans, 0501 psychology and cognitive sciences, Brain-derived neurotrophic factor, Evolutionary Biology, Behavior, Population Biology, Brain-Derived Neurotrophic Factor, lcsh:R, Cognitive Psychology, Biology and Life Sciences, Oxytocin receptor, Genetic Polymorphism, Cognitive Science, Perception, lcsh:Q, Self Report, 030217 neurology & neurosurgery, Population Genetics, Social behavior, Neuroscience
Abstract

Empathy is an important driver of human social behaviors and presents genetic roots that have been studied in neuroimaging using the intermediate phenotype approach. Notably, the Val66Met polymorphism of the Brain-derived neurotrophic factor (BDNF) gene has been identified as a potential target in neuroimaging studies based on its influence on emotion perception and social cognition, but its impact on self-reported empathy has never been documented. Using a neurogenetic approach, we investigated the association between the BDNF Val66Met polymorphism and self-reported empathy (Davis’ Interpersonal Reactivity Index; IRI) in a sample of 110 young adults. Our results indicate that the BDNF genotype is significantly associated with the linear combination of the four facets of the IRI, one of the most widely used self-reported empathy questionnaire. Crucially, the effect of BDNF Val66Met goes beyond the variance explained by two polymorphisms of the oxytocin transporter gene previously associated with empathy and its neural underpinnings (OXTR rs53576 and rs2254298). These results represent the first evidence suggesting a link between the BDNF gene and self-reported empathy and warrant further studies of this polymorphism due to its potential clinical significance. Published version

Published
2016

5. Genome-wide linkage analysis for circulating levels of adipokines and C-reactive protein in the Quebec family study (QFS)

Author

Stephanie-May Ruchat, Louis Pérusse, Yvon C. Chagnon, Claude Bouchard, S. John Weisnagel, and Jean-Pierre Després

Subjects
Adult, Genetic Markers, Male, medicine.medical_specialty, Genetic Linkage, Quantitative Trait Loci, Adipokine, Adipose tissue, Biology, Cohort Studies, Insulin resistance, Genetic linkage, Internal medicine, Genetics, medicine, Humans, Obesity, Genetics (clinical), Chromosomes, Human, Pair 15, Chromosomes, Human, Pair 12, Autosome, Adiponectin, Genome, Human, C-reactive protein, Quebec, Middle Aged, medicine.disease, C-Reactive Protein, Endocrinology, biology.protein, Female, Body mass index
Abstract

Adipose tissue synthesizes and secretes a wide range of biologically active molecules considered as inflammatory markers whose dysregulation in obesity plays a role in the development of insulin resistance and vascular disorders. Thus, finding genes that influence circulating levels of inflammatory biomarkers may provide insights into the genetic determinants of obesity-related metabolic diseases. We performed linkage analyses for fasting plasma levels of adiponectin, C-reactive protein (CRP), interleukin-6 (IL-6) and tumor-necrosis factor-alpha (TNF-alpha) in 764 subjects enrolled in the Quebec family study (QFS). A maximum of 393 pairs of siblings from 211 nuclear families were available for analyses. A total of 443 markers spanning the 22 autosomal chromosomes with an average inter-marker distance of 6.24 Mb were genotyped. Linkage was tested using both allele-sharing (SIBPAL) and variance component linkage methods (MERLIN). We showed suggestive evidence of linkage for plasma adiponectin levels on chromosome 15q21.1 [D15S659; logarithm of the odds (LOD) score = 2.23], 3q13.33 (D3S3023; LOD = 2.09), 20q13.2 (D20S197; LOD = 1.96) and 14q32.2 (D14S1426; LOD = 1.79). Evidence of linkage (SIBPAL) was also found for CRP on 12p11.23 (P = 0.001) and 12q15 (P = 0.0005) and for IL-6 on 14q12 (P = 0.002). None of these linkages remained significant after adjustment for body mass index. No evidence of linkage was found for TNF-alpha plasma levels. These results suggest that several QTLs can influence plasma levels of adiponectin and CRP, partly via their effects on adiposity.

Published
2008

6. Differential RNA expression between schizophrenic patients and controls of the dystrobrevin binding protein 1 and neuregulin 1 genes in immortalized lymphocytes

Author

Yvon C. Chagnon, Chantal Mérette, Marc-André Roy, Alexandre Bureau, and Michel Maziade

Subjects
Adult, Gene isoform, medicine.medical_specialty, Bipolar Disorder, medicine.drug_class, Neuregulin-1, Gene Expression, Atypical antipsychotic, Nerve Tissue Proteins, Stimulation, Biology, Benzodiazepines, Internal medicine, Gene expression, medicine, Humans, Protein Isoforms, Lymphocytes, Neuregulin 1, Gene, Cells, Cultured, Biological Psychiatry, Aged, Dysbindin, RNA, Middle Aged, Control Groups, Psychiatry and Mental health, Endocrinology, Olanzapine, Pharmacogenetics, Dystrophin-Associated Proteins, Schizophrenia, biology.protein, Neuregulin, Female, Carrier Proteins, Antipsychotic Agents
Abstract

The dystrobrevin binding protein 1 (DTNBP1) and neuregulin 1 (NRG1) genes have been related to schizophrenia (SZ) and bipolar disorder (BP) by several whole-genome linkage and associations studies. Few expression studies in post-mortem brains have also reported a lower or a higher expression of DTNBP1 and NRG1, respectively, in SZ. Since the difficulty to access post-mortem brains, we evaluated RNA expression of DTNBP1 and NRG1 in immortalized lymphocytes of SZ patients and unrelated-family controls. An antipsychotic stimulation was also used to challenge the genetic background of the subjects and enhance differential expression. Immortalized lymphocytes of twelve SZ and twelve controls were grown individually in the presence or not of the antipsychotic olanzapine (Zyprexa; EliLilly). RNA was extracted and pooled in four groups of three SZ and four groups of three controls, and used to probe Agilent 18K microchips. Mean gene expression values were contrasted between SZ and control groups using a T-test. For DTNBP1, RNA expression was lower in SZ than in controls before (-28%; p=0.02) and after (-30%; p=0.01) olanzapine stimulation. Similarly, NRG1 GGF2 isoform showed a lower expression in SZ before (-29%; p=0.04) and after (-33%; p=0.02) olanzapine stimulation. In contrast, NRG1 GGF isoform showed no significant difference between SZ and controls (-7%; p=0.61, +3%; p=0.86, respectively), but was slightly repressed by olanzapine in controls (-8%; p=0.008) but not in SZ (+1%; p=0.91). These results are in agreement with those observed in post-mortem brain when the isoforms involved are considered.

Published
2008

7. Evidence of Linkage and Association with Body Fatness and Abdominal Fat on Chromosome 15q26*

Author

Claude Bouchard, Luigi Bouchard, Yvon C. Chagnon, and Louis Pérusse

Subjects
Adult, Male, Candidate gene, medicine.medical_specialty, Intra-Abdominal Fat, Genetic Linkage, Endocrinology, Diabetes and Metabolism, Quantitative Trait Loci, Subcutaneous Fat, Medicine (miscellaneous), Single-nucleotide polymorphism, Quantitative trait locus, Biology, Polymerase Chain Reaction, Endocrinology, Polymorphism (computer science), Genetic linkage, Internal medicine, medicine, Humans, Obesity, Prospective Studies, Allele, Genetics, Chromosomes, Human, Pair 15, Polymorphism, Genetic, Nutrition and Dietetics, Quebec, Chromosome Mapping, Membrane Proteins, DNA, medicine.disease, Female, Microsatellite Repeats
Abstract

Objective: In the present study, we undertook a two-step fine mapping of a 20-megabase region around a quantitative trait locus previously reported on chromosome 15q26 for abdominal subcutaneous fat (ASF) in an extended sample of 707 subjects from 202 families from the Quebec Family Study. Research Methods and Procedure: First, 19 microsatellites (in addition to the 7 markers initially available on 15q24-q26; total = 26) were genotyped and tested for linkage with abdominal total fat, abdominal visceral fat, and ASF assessed by computed tomography and with fat mass (FM) using variance component-based approach on age- and sex-adjusted phenotypes. Second, 16 single nucleotide polymorphisms (SNPs) were genotyped and tested for association using family-based association tests. Results: After the fine mapping, the peak logarithm of odds ratio (LOD) score (marker D15S1004) increased from 2.79 to 3.26 for ASF and from 3.52 to 4.48 for FM, whereas for abdominal total fat, the peak linkage (marker D15S996) decreased from 2.22 to 1.53. No evidence of linkage was found for abdominal visceral fat. Overall, for genotyped SNPs, three variants located in the putative MCTP2 gene were significantly associated with FM and the three abdominal fat phenotypes (p ≤ 0.05). The major allele and genotype of rs1424695 were associated with higher adiposity values (p < 0.004). The same trend was found for the two other polymorphisms (p < 0.05). None of the other SNPs was associated with adiposity phenotypes. The linkage for FM became non-significant (LOD = 0.84) after adjustment for the MCTP2 polymorphisms, whereas the one for ASF remained unchanged. Discussion: These results suggest that the MCTP2 gene, located on chromosome 15q26, influences adiposity. Other studies will be needed to investigate the function of the MCTP2 gene and its role in obesity.

Published
2007

8. Possible association of the pro-melanin-concentrating hormone gene witha greater body mass index as a side effect of the antipsychotic olanzapine

Author

Alexandre Bureau, Chantal Mérette, Michel Maziade, D. Gendron, Yvon C. Chagnon, Roch-Hugo Bouchard, and Marc-André Roy

Subjects
Adult, Male, medicine.medical_specialty, Genotype, Genetic Linkage, medicine.drug_class, medicine.medical_treatment, Atypical antipsychotic, Single-nucleotide polymorphism, Overweight, Weight Gain, Polymorphism, Single Nucleotide, Body Mass Index, Benzodiazepines, Cellular and Molecular Neuroscience, Age Distribution, Internal medicine, medicine, Humans, Genetic Predisposition to Disease, Obesity, Protein Precursors, Sex Distribution, Antipsychotic, Genetics (clinical), Aged, Hypothalamic Hormones, business.industry, Homozygote, Case-control study, Middle Aged, medicine.disease, Psychiatry and Mental health, Endocrinology, Psychotic Disorders, Olanzapine, Case-Control Studies, Schizophrenia, Female, medicine.symptom, business, Body mass index, Pharmacogenetics, Antipsychotic Agents
Abstract

Following our report of a linkage at 12q24 with a phenotype of obesity under antipsychotics, we tested the pro-melanin-concentrating hormone (PMCH) candidate gene for a possible association in humans with the body mass index (BMI; kg/m2) in unrelated schizophrenic patients (SZ) receiving antipsychotics (N = 300) and in controls (CTL; N = 150). Subjects were classified in obese (OB) (BMI > or = 30 kg/m2), overweight (25 < or = BMI < 30 kg/m2), and normal weight (BMI < 25 kg/m2) groups. Single nucleotide polymorphisms (SNP) rs7973796 and rs11111201, located 5' at -4.5 kb and 3' at +1.8 kb, respectively, of PMCH were genotyped. Interaction effects of genotypes and antipsychotic treatment on BMI were tested in a covariance analysis with age and gender as covariates. Interaction effects on the prevalence of obesity were tested in a logistic regression analysis. For subjects under 50 years, the effect of the rs7973796 genotype on BMI differed between the SZ patients taking olanzapine and CTL group (interaction P = 0.025). Olanzapine-treated SZ patients carrying the ancestral homozygote genotype showed a higher BMI for rs7973796 (P = 0.016 with the LSMeans t-test) than the variant homozygotes. Accordingly, the ORs for obesity associated with rs7973796 genotypes differed in the SZ patients taking olanzapine compared to the CTL group (interaction P = 0.0094). The G allele was associated with an increase in the odds of obesity in SZ patients taking olanzapine. No association was observed for those over 50 years, or for rs11111201. These results suggest that the common allele of PMCH rs7973796 may be associated with a greater BMI in olanzapine-treated SZ patients.

Published
2007

9. A Quantitative Trait Locus for Body Fat on Chromosome 1q43 in French Canadians: Linkage and Association Studies*

Author

Brandon Walts, Claude Bouchard, Gilles Lapointe, Luigi Bouchard, Brahim Aissani, Yvon C. Chagnon, and Louis Pérusse

Subjects
Adult, Male, Adolescent, Genotype, Genetic Linkage, Endocrinology, Diabetes and Metabolism, Quantitative Trait Loci, Medicine (miscellaneous), Locus (genetics), Biology, Quantitative trait locus, Polymorphism, Single Nucleotide, Body Mass Index, Cohort Studies, Endocrinology, Gene Frequency, Gene mapping, Genetic linkage, Humans, Obesity, Association mapping, Aged, Genetic association, Genetics, Nutrition and Dietetics, Quebec, Transmission disequilibrium test, Middle Aged, Health Surveys, Adipose Tissue, Chromosomes, Human, Pair 1, Body Composition, Female, Body mass index, Microsatellite Repeats
Abstract

Objective: To explore a quantitative trait locus (QTL) on human chromosome 1q affecting BMI, adiposity, and fat-free mass phenotypes in the Quebec Family Study cohort. Research Methods and Procedures: Non-parametric sibpair and variance component linkage analyses and family-based association studies were performed with a dense set of chromosome 1q43 microsatellites and single-nucleotide polymorphism markers in 885 adult individuals. Results: Linkage was observed between marker D1S184 and BMI (p = 0.0004) and with body fat mass or percentage body fat (p ≤ 0.0003), but no linkage was detected with fat-free mass. Furthermore, significant linkages (p < 0.0001) were achieved with subsamples of sibpairs at both ends of phenotype distributions. Association studies with quantitative transmission disequilibrium tests refined the linkage to a region overlapping the regulator of G-protein signaling 7 (RGS7) gene and extending to immediate upstream gene loci. Discussion: The present study indicates that the QTL on chromosome 1q43 specifically affects total adiposity and provides a genetic mapping framework for the dissection of this adiposity locus.

Published
2006

10. Polymorphisms in the leptin and leptin receptor genes in relation to resting metabolic rate and respiratory quotient in the Québec Family Study

Author

Yvon C. Chagnon, André J. Tremblay, Ruth J. F. Loos, Tuomo Rankinen, Claude Bouchard, and Louis Pérusse

Subjects
Adult, Leptin, Male, medicine.medical_specialty, Genotype, Endocrinology, Diabetes and Metabolism, Medicine (miscellaneous), Receptors, Cell Surface, Biology, Energy homeostasis, Oxygen Consumption, Gene Frequency, Internal medicine, medicine, Humans, Exercise, Allele frequency, Polymorphism, Genetic, Nutrition and Dietetics, Leptin receptor, Anthropometry, Pulmonary Gas Exchange, Middle Aged, medicine.disease, Obesity, Respiratory quotient, Phenotype, Endocrinology, Basal metabolic rate, Receptors, Leptin, Female, Basal Metabolism
Abstract

Leptin (LEP) is an endocrine hormone that participates in many metabolic pathways, including those associated with the central regulation of energy homeostasis.We examined the associations between polymorphisms in the LEP and leptin receptor (LEPR) genes and resting metabolic rate (RMR) and respiratory quotient (RQ) in the Quebec Family Study.Three polymorphisms in LEPR (K109R, Q223R and K656N) and one in LEP (19AG) were genotyped in 678 subjects. RMR, RQ at rest and RQ while sitting, standing and walking at 4.5 km/h (RQ45) were adjusted for age, sex, fat mass and fat-free mass.RQ45 was associated with the LEPR-K109R (P = 0.004) and Q223R (P = 0.03) polymorphisms, and RMR showed association with the LEPR-K656N polymorphism (P = 0.006). For the LEP-19AG polymorphism, no significant associations were observed. However, LEP-A19A homozygotes who were carriers of the LEPR N656 allele had a significantly lower RQ45 compared to other genotype combinations (P for interaction=0.003).These findings suggest that DNA sequence variation in the LEPR gene contributes to human variation in RMR and in the relative rates of substrate oxidation during low-intensity exercise in steady state but not in a resting state.

Published
2005

11. Evidence of QTLs on chromosomes 13q and 14q for triglycerides before and after 20 weeks of exercise training: The HERITAGE Family Study

Author

Tuomo Rankinen, James S. Skinner, Mary F. Feitosa, Jean-Pierre Després, Michael A. Province, Yvon C. Chagnon, Claude Bouchard, Jack H. Wilmore, Arthur S. Leon, Treva Rice, Jacques Gagnon, D. C. Rao, and Ingrid B. Borecki

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, Quantitative Trait Loci, Black People, Physical exercise, Quantitative trait locus, White People, chemistry.chemical_compound, Genetic linkage, Internal medicine, Humans, Medicine, Genetic Predisposition to Disease, Risk factor, Exercise, Triglycerides, Aged, Dyslipidemias, Chromosomes, Human, Pair 14, Linkage (software), Chromosomes, Human, Pair 13, Triglyceride, medicine.diagnostic_test, business.industry, Middle Aged, Atherosclerosis, Endocrinology, chemistry, Female, lipids (amino acids, peptides, and proteins), Cardiology and Cardiovascular Medicine, business, Lipid profile, Lipoprotein
Abstract

Fasting triglyceride (TG) levels in total plasma and in lipoprotein subfractions were assessed both at baseline and after a 20-week exercise training intervention in 99 White and 101 Black families. A genome-wide multipoint variance component linkage analysis was performed separately by race, using 509 markers. The strongest evidence of linkage was for the TG subfractions of low-density lipoprotein (LDL-TG) and high-density lipoprotein (HDL-TG) rather than for overall levels of TG. For baseline levels, the maximum LOD score was 3.8 on 13q12-q14 with HDL-TG in Whites. Additional linkage evidence was found on 14q31 (LOD=3.2) and 10p14 (LOD=2.9) for baseline LDL-TG in Whites. Suggestive linkage signal at baseline in Whites was detected for HDL-TG (LOD=2.6) on 12q24 and for LDL-TG on 19p13. For training response in Whites, suggestive signal (LOD=2.2) was observed on 13q12-q14 with LDL-TG and for HDL-TG on 10q23. For Blacks, weak signals (LODs2.0) were found either for baseline and responses to training, perhaps due to small sample sizes that reduced the power of the linkage analysis. These results represent the first report of linkage for the lipoprotein subfractions and for the lipid and lipoprotein responses to exercise training. It is interesting that the strongest signals were found for the LDL-TG and HDL-TG subfractions, given their particular relationships with the atherogenic lipid profile including dense LDL and HDL particles.

Published
2005

12. Mapping of a new candidate locus for uromodulin-associated kidney disease (UAKD) to chromosome 1q41

Author

Christian-Marc Lanouette, Kateřina Hodaňová, Helena Hůlková, Yvon C. Chagnon, Blanka Stibůrková, Marie Hubalek Kalbacova, Petr Vyleťal, Anthony M. Marinaki, Gopalakrishnan Venkat-Raman, Martina Kublová, Jean-Pierre Fryns, Stanislav Kmoch, and Jacek Majewski

Subjects
Adult, Male, linkage mapping, renal failure, Candidate gene, Tamm–Horsfall protein, Adolescent, Genotype, Genetic Linkage, Locus (genetics), Hyperuricemia, Biology, Kidney, Medullary cystic kidney disease, Mucoproteins, Gene mapping, Genetic linkage, Uromodulin, medicine, Humans, Renal Insufficiency, Chronic, Child, Aged, Aged, 80 and over, Genetics, Haplotype, Chromosome Mapping, Kidney metabolism, Middle Aged, familial juvenile hyperuricemic nephropathy, medicine.disease, Pedigree, Chromosomes, Human, Pair 1, Nephrology, biology.protein, Female
Abstract

Mapping of a new candidate locus for uromodulin-associated kidney disease (UAKD) to chromosome 1q41.BackgroundAutosomal-dominant juvenile hyperuricemia, gouty arthritis, medullary cysts, and progressive renal insufficiency are features associated with familial juvenile hyperuricemic nephropathy (FJHN), medullary cystic kidney disease type 1 (MCKD1) and type 2 (MCKD2). MCKD1 has been mapped to chromosome 1q21. FJHN and MCKD2 have been mapped to chromosome 16p11.2. FJHN and MCKD2 are allelic, result from uromodulin (UMOD) mutations and the term uromodulin-associated kidney disease (UAKD) has been proposed for them. Linkage studies also reveal families that do not show linkage to any of the identified loci. To identify additional UAKD loci, we analyzed one of these families, with features suggestive of FJHN.MethodsClinical, biochemical, and immunohistochemical investigations were used for phenotype characterization. Genotyping, linkage and haplotype analyses were employed to identify the candidate disease region. Bioinformatics and sequencing were used for candidate gene selection and analyses.ResultsWe identified a new candidate UAKD locus on chromosome 1q41, bounded by markers D1S3470 and D1S1644. We analyzed and found no linkage to this region in eight additional families, who did not map to the previously established loci. We noted that affected individuals showed, in addition to the characteristic urate hypoexcretion, significant reductions in urinary excretion of calcium and UMOD. Immunohistochemical analysis showed that low UMOD excretion resulted from its reduced expression, which is a different mechanism to intracellular UMOD accumulation observed in cases with UMOD mutations.ConclusionWe have mapped a new candidate UAKD locus and shown that UAKD may be a consequence of various defects affecting uromodulin biology.

Published
2005

13. Evidence of QTLs on chromosomes 1q42 and 8q24 for LDL-cholesterol and apoB levels in the HERITAGE Family Study

Author

Tuomo Rankinen, Yvon C. Chagnon, Ingrid B. Borecki, Jean-Pierre Després, D. C. Rao, Michael A. Province, Claude Bouchard, Mary F. Feitosa, Jacques Gagnon, James S. Skinner, Arthur S. Leon, and Treva Rice

Subjects
Genetic Markers, Male, Candidate gene, Time Factors, Apolipoprotein B, Genetic Linkage, Quantitative Trait Loci, QD415-436, Quantitative trait locus, Biochemistry, Body Mass Index, lipids, Centimorgan, Endocrinology, Endurance training, Genetic linkage, Humans, Insulin, risk factors, genetics, coronary heart disease, Edetic Acid, Apolipoproteins B, Genetics, Genome, biology, Models, Genetic, exercise, Chromosome, Chromosome Mapping, Cell Biology, Cholesterol, LDL, lipoproteins, Phenotype, Chromosomes, Human, Pair 1, biology.protein, Female, lipids (amino acids, peptides, and proteins), Lod Score, Lipoprotein, Chromosomes, Human, Pair 8
Abstract

Genome-wide multipoint linkage analyses were performed to identify chromosomal regions harboring genes influencing LDL-cholesterol, total apolipoprotein B (apoB), and LDL-apoB levels using 654 markers. They were assessed in a sedentary state (baseline) and after a 20 week endurance training program. Strong evidence for two quantitative trait loci (QTLs) for baseline levels was found. There is linkage evidence in black families on chromosomes 1q41-q44 [at marker D1S2860, 238 centimorgan (cM), with a maximum log of the odds (LOD) score of 3.7 for LDL-apoB] and in white families on chromosome 8q24 (at marker D8S1774, 142 cM, with LOD scores of 3.6, 3.3, and 2.5 for baseline LDL-cholesterol, LDL-apoB, and apoB, respectively). There were no strong signals for the lipoprotein training responses (as computed as the difference in posttraining minus baseline levels). In conclusion, QTLs for baseline apoB and LDL-cholesterol levels on chromosomes 1q41-q44 (in blacks) and 8q24 (in whites) were found. As there are no known strong candidate genes in these regions for lipids, follow-up studies to determine the source of those signals are needed.

Published
2005

14. Shared and specific susceptibility loci for schizophrenia and bipolar disorder: a dense genome scan in Eastern Quebec families

Author

A. M. Ponton, N. Montgrain, J. C. Lavallee, Marc-André Roy, Fournier Jp, Nathalie Gingras, Yvon C. Chagnon, A. Pires, A. Potvin, Michel Maziade, L. Nicole, D. Cliche, C. Dion, Chantal Mérette, H. Wallot, and Y. Garneau

Subjects
Adult, Male, Psychosis, Bipolar Disorder, Genetic Linkage, Genome Scan, Biology, behavioral disciplines and activities, Genome, Genetic determinism, Cellular and Molecular Neuroscience, Genetic linkage, mental disorders, medicine, Chromosomes, Human, Humans, Family, Genetic Predisposition to Disease, Bipolar disorder, Molecular Biology, Psychiatric genetics, Genetics, Models, Genetic, Quebec, Middle Aged, medicine.disease, Psychiatry and Mental health, Schizophrenia, Female, Lod Score
Abstract

The goal of this study was to identify susceptibility loci shared by schizophrenia (SZ) and bipolar disorder (BP), or specific to each. To this end, we performed a dense genome scan in a first sample of 21 multigenerational families of Eastern Quebec affected by SZ, BP or both (N=480 family members). This probably constitutes the first genome scan of SZ and BP that used the same ascertainment, statistical and molecular methods for the concurrent study of the two disorders. We genotyped 607 microsatellite markers of which 350 were spaced by 10 cM and 257 others were follow-up markers in positive regions at the 10 cM scan. Lander and Kruglyak thresholds were conservatively adjusted for multiple testings. We maximized the lod scores (mod score) over eight combinations (2 phenotype severity levels x 2 models of transmission x 2 analyses, affected/unaffected vs affected-only). We observed five genomewide significant linkages with mod score4.0: three for BP (15q11.1, 16p12.3, 18q12-q21) and two for the shared phenotype, that is, the common locus (CL) phenotype (15q26,18q12-q21). Nine mod scores exceeded the suggestive threshold of 2.6: three for BP (3q21, 10p13, 12q23), three for SZ (6p22, 13q13, 18q21) and three for the CL phenotype (2q12.3, 13q14, 16p13). Mod scores1.9 might represent confirmatory linkages of formerly reported genomewide significant findings such as our finding in 6p22.3 for SZ. Several regions appeared to be shared by SZ and BP. One linkage signal (15q26) appeared novel, whereas others overlapped formerly reported susceptibility regions. Despite the methodological limitations we raised, our data support the following trends: (i) results from several genome scans of SZ and BP in different populations tend to converge in specific genomic regions and (ii) some of these susceptibility regions may be shared by SZ and BP, whereas others may be specific to each. The present results support the relevance of investigating concurrently SZ and BP within the same study and have implications for the modelling of genetic effects.

Published
2004

15. Genome-wide linkage scan reveals multiple susceptibility loci influencing lipid and lipoprotein levels in the Québec Family Study

Author

Yvon C. Chagnon, Marie-Claude Vohl, Yohan Bossé, Claude Bouchard, D. C. Rao, Louis Pérusse, Jean-Pierre Després, and Treva Rice

Subjects
Adult, Male, Candidate gene, Genetic Linkage, Lipoproteins, Genome Scan, genome scan, QD415-436, Biology, Quantitative trait locus, Biochemistry, chemistry.chemical_compound, quantitative trait locus, Endocrinology, Humans, Genetic Predisposition to Disease, genetics, triglyceride, Gene, Nuclear family, Family Health, Genetics, Linkage (software), Chromosomes, Human, Pair 12, blood lipids, Genome, Human, Cholesterol, Quebec, cholesterol, Chromosome, Genomics, Cell Biology, Middle Aged, Lipids, chemistry, Female, lipids (amino acids, peptides, and proteins), Lod Score
Abstract

A genome-wide linkage study was performed to identify chromosomal regions harboring genes influencing lipid and lipoprotein levels. Linkage analyses were conducted for four quantitative lipoprotein/lipid traits, i.e., total cholesterol, triglyceride, HDL-cholesterol (HDL-C), and LDL-C concentrations, in 930 subjects enrolled in the Quebec Family Study. A maximum of 534 pairs of siblings from 292 nuclear families were available. Linkage was tested using both allele-sharing and variance-component linkage methods. The strongest evidence of linkage was found on chromosome 12q14.1 at marker D12S334 for HDL-C, with a logarithm of the odds (LOD) score of 4.06. Chromosomal regions harboring quantitative trait loci (QTLs) for LDL-C included 1q43 (LOD = 2.50), 11q23.2 (LOD = 3.22), 15q26.1 (LOD = 3.11), and 19q13.32 (LOD = 3.59). In the case of triglycerides, three markers located on 2p14, 11p13, and 11q24.1 provided suggestive evidence of linkage (LOD > 1.75). Tests for total cholesterol levels yielded significant evidence of linkage at 15q26.1 and 18q22.3 with the allele-sharing linkage method, but the results were nonsignificant with the variance-component method. In conclusion, this genome scan provides evidence for several QTLs influencing lipid and lipoprotein levels. Promising candidate genes were located in the vicinity of the genomic regions showing evidence of linkage.

Published
2004

16. Evidence for a Major Quantitative Trait Locus on Chromosome 17q21 Affecting Low-Density Lipoprotein Peak Particle Diameter

Author

Yohan Bossé, Jean-Pierre Després, D. C. Rao, Yvon C. Chagnon, Treva Rice, Louis Pérusse, Marie-Claude Vohl, Claude Bouchard, and Benoît Lamarche

Subjects
Adult, Male, Genetics, Linkage (software), Quantitative Trait Loci, Chromosome, Middle Aged, Heritability, Biology, Quantitative trait locus, Linkage Disequilibrium, Genetic determinism, Lipoproteins, LDL, chemistry.chemical_compound, Phenotype, chemistry, Physiology (medical), Low-density lipoprotein, Genotype, Y linkage, Humans, Female, Particle Size, Cardiology and Cardiovascular Medicine, Chromosomes, Human, Pair 17
Abstract

Background— Several lines of evidence suggest that small dense LDL particles are associated with the risk of coronary heart disease. Heritability and segregation studies suggest that LDL particle size is characterized by a large genetic contribution and the presence of a putative major genetic locus. However, association and linkage analyses have thus far been inconclusive in identifying the underlying gene(s). Methods and Results— An autosomal genome-wide scan for LDL peak particle diameter (LDL-PPD) was performed in the Québec Family Study. A total of 442 markers were genotyped, with an average intermarker distance of 7.2 cM. LDL-PPD was measured by gradient gel electrophoresis in 681 subjects from 236 nuclear families. Linkage was tested by both sib-pair–based and variance components–based linkage methods. The strongest evidence of linkage was found on chromosome 17q21.33 at marker D17S1301, with an LOD score of 6.76 by the variance-components method for the phenotype adjusted for age, body mass index, and triglyceride levels. Similar results were obtained with the sib-pair method ( P P ≤0.0023; LOD ≥1.75) include 1p31, 2q33.2, 4p15.2, 5q12.3, and 14q31. Several candidate genes are localized under the peak linkages, including apolipoprotein H on chromosome 17q, the apolipoprotein E receptor 2, and members of the phospholipase A 2 family on chromosome 1p as well as HMG-CoA reductase on chromosome 5q. Conclusions— This genome-wide scan for LDL-PPD indicates the presence of a major quantitative trait locus located on chromosome 17q and others interesting loci influencing the phenotype.

Published
2003

17. Familial Resemblance for Plasma Leptin: Sample Homogeneity across Adiposity and Ethnic Groups

Author

Jacques Gagnon, Louis Pérusse, Treva Rice, Claude Bouchard, James S. Skinner, Dabeeru C. Rao, Greg Collier, Jack H. Wilmore, Arthur S. Leon, Yvon C. Chagnon, and Ingrid B. Borecki

Subjects
Adult, Leptin, Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Ethnic group, Black People, Medicine (miscellaneous), Adipose tissue, Biology, White People, Endocrinology, Internal medicine, medicine, Humans, Insulin, Family, Obesity, Sex Characteristics, Genetic heterogeneity, Homogeneity (statistics), Racial Groups, Public Health, Environmental and Occupational Health, Diabetes status, Fasting, Middle Aged, Heritability, Skinfold Thickness, Phenotype, Adipose Tissue, Body Composition, Female, Food Science, Demography, Sex characteristics
Abstract

Objective: Previous studies show a wide range in the percentage of variance in leptin levels attributable to genetic factors. These studies differ markedly with respect to ethnicity, study design, and statistical methodology. Therefore, the purpose of this study was to investigate heterogeneity hypotheses across ethnic groups and by adiposity level, using the same statistical methods. Research Methods and Procedures: Samples included black vs. white (HERITAGE Family Study) and random vs. obese (Quebec Family Study) individuals from 432 families (1432 individuals). Heritability for leptin, alternatively adjusted for age and sex and then for age, sex, and adiposity was estimated with the use of familial correlations. Heterogeneity in the magnitude of the familial resemblance between samples and the effect of adjusting for adiposity was explored. Results: Heritability did not vary across samples stratified by adiposity level or ethnic group or across adjustment schemes. Maximal heritability, the percentage of additive phenotypic variability due to all familial sources, was 32%. Discussion: Whereas leptin and adiposity were highly correlated within individuals, removing the effects of adiposity did not significantly alter the magnitude of the familial component for leptin. Moreover, this effect did not vary as a function of ethnicity (black vs. white) or adiposity level. Thus, no evidence for heterogeneity was detected. However, a comparison among previous studies raises questions concerning possible genetic heterogeneity in other ethnic groups in which complex interactions among leptin, adiposity, and diabetes status may be important.

Published
2002

18. Uncoupling protein 3 gene is associated with body composition changes with training in HERITAGE study

Author

Dabeeru C. Rao, Louis Pérusse, Patrick Muzzin, Jacques Gagnon, Arthur S. Leon, Jack H. Wilmore, Treva Rice, Jean Paul Giacobino, Claude Bouchard, James S. Skinner, Yvon C. Chagnon, and Christian Marc Lanouette

Subjects
Adult, Male, medicine.medical_specialty, Time Factors, Genotype, Genetic Linkage, Physiology, Black People, Biology, Ion Channels, White People, Mitochondrial Proteins, Physiology (medical), Internal medicine, medicine, Humans, Uncoupling Protein 3, Uncoupling protein, Inner mitochondrial membrane, Gene, Alleles, Ion channel, UCP3, Physical Education and Training, Polymorphism, Genetic, Skeletal muscle, Transporter, Phenotype, Endocrinology, medicine.anatomical_structure, Body Composition, Physical Endurance, Female, Carrier Proteins
Abstract

The uncoupling protein 3 (UCP3) is a mitochondrial membrane transporter mainly expressed in skeletal muscle that we have shown to be associated with obesity. We have analyzed UCP3 polymorphisms, Val102Ile, Tyr210Tyr, and a new microsatellite GAIVS6 located in the sixth intron, among 276 black and 503 white subjects from the HERITAGE Family Study. Linkage and association studies were undertaken with body composition variables measured in a sedentary state (baseline) and after 20 wk of endurance training (changes). Allele and genotype frequencies were found to be significantly different between whites and blacks. Suggestive linkages (0.009 ≤ P ≤ 0.033) with Tyr210Tyr were found in blacks and whites for baseline body mass index, fat mass, or leptin level and with GAIVS6 in whites for changes in fat mass and percent body fat. Associations were also found in whites between GAIVS6 and changes in the sum of eight skinfold thicknesses ( P = 0.0006), with a borderline result for body mass index ( P = 0.06). We concluded that UCP3 could be involved in body composition changes after regular exercise.

Published
2002

19. Evidence of LPL gene-exercise interaction for body fat and LPL activity: the HERITAGE Family Study

Author

Jean Bergeron, Louis Pérusse, Arthur S. Leon, Jacques Gagnon, Christophe Garenc, D. C. Rao, James S. Skinner, Claude Bouchard, Jack H. Wilmore, Ingrid B. Borecki, and Yvon C. Chagnon

Subjects
Adult, Male, Heterozygote, medicine.medical_specialty, Physiology, Black People, Adipose tissue, Physical exercise, White People, Endurance training, Polymorphism (computer science), Physiology (medical), Internal medicine, medicine, Humans, Allele, Exercise, Family Health, Lipoprotein lipase, Polymorphism, Genetic, business.industry, Anthropometry, Lipoprotein Lipase, Endocrinology, Body Composition, Female, business, Body mass index
Abstract

Evidence of a gene-exercise interaction for traits related to body composition is limited. Here, the association between the lipoprotein lipase (LPL) S447X polymorphism and changes in body mass index, fat mass, percent body fat, abdominal visceral fat measured by computed tomography, and post-heparin plasma LPL activity in response to 20 wk of endurance training was investigated in 741 adult white and black subjects. Changes were compared between carriers and noncarriers of the X447 allele after adjustment for the effects of age and pretraining values. No evidence of association was observed in men. However, white women carrying the X447 allele exhibited greater reductions of body mass index ( P= 0.01), fat mass ( P = 0.01), and percent body fat ( P = 0.03); in black women, the carriers exhibited a greater reduction of abdominal visceral fat ( P = 0.05) and a greater increase in post-heparin LPL activity ( P = 0.02). These results suggest that the LPL S447X polymorphism influences the training-induced changes in body fat and post-heparin LPL activity in women but not in men.

Published
2001

20. A new gene related to human obesity identified by suppression subtractive hybridization

Author

M. Larose, Yvon C. Chagnon, and Claude Bouchard

Subjects
Adult, medicine.medical_specialty, DNA, Complementary, Endocrinology, Diabetes and Metabolism, Molecular Sequence Data, Population, Gene Expression, Medicine (miscellaneous), Adipose tissue, Locus (genetics), Biology, Centimorgan, Sequence Homology, Nucleic Acid, Complementary DNA, Internal medicine, medicine, Humans, education, Gene, education.field_of_study, Nutrition and Dietetics, Reverse Transcriptase Polymerase Chain Reaction, Nucleic Acid Hybridization, Sequence Analysis, DNA, Middle Aged, Molecular biology, Obesity, Morbid, Molecular Weight, Open reading frame, Endocrinology, Adipose Tissue, Suppression subtractive hybridization, Case-Control Studies, Female, Chromosomes, Human, Pair 8
Abstract

OBJECTIVE: The aim of the research was to identify genes specially expressed in the obese state and potentially involved in the pathogenesis of obesity. DESIGN AND SUBJECTS: We used the technique of suppression subtractive hybridization (SSH), which combines subtractive hybridization with PCR, to generate a population of PCR fragments enriched for transcripts of high or low abundance from differentially expressed genes. PolyA+ mRNA was isolated from subcutaneous abdominal adipose tissue of five massively obese (>35 kg/m2) and five normal-weight (

Published
2001

21. Genomic scan for genes affecting body composition before and after training in Caucasians from HERITAGE

Author

My Anh Ho-Kim, Jacques Gagnon, Arthur S. Leon, James S. Skinner, Louis Pérusse, D. C. Rao, Michel Lacaille, Treva Rice, Luigi Bouchard, Jack H. Wilmore, Claude Bouchard, Chantal Paré, Ingrid B. Borecki, and Yvon C. Chagnon

Subjects
Adult, Genetic Markers, Leptin, Male, Canada, medicine.medical_specialty, Adolescent, Physiology, Biology, Genome, White People, Genetic determinism, Body Mass Index, Nuclear Family, Fat free mass, Physiology (medical), Internal medicine, medicine, Humans, Exercise, Gene, Aged, Genetics, Sex Characteristics, Body Weight, Chromosome Mapping, Middle Aged, Phenotype, United States, Skinfold Thickness, Endocrinology, Adipose Tissue, Receptors, LDL, Physical Fitness, Body Composition, Lean body mass, Female, Lod Score, Training program, Body mass index, Microsatellite Repeats
Abstract

An autosomal genomewide search for genes related to body composition and its changes after a 20-wk endurance-exercise training program has been completed in the HERITAGE Family Study. Phenotypes included body mass index (BMI), sum of eight skinfold thicknesses, fat mass (FM), fat-free mass, percent body fat (%Fat), and plasma leptin levels. A maximum of 364 sib-pairs from 99 Caucasian families was studied with the use of 344 markers with single-point and multipoint linkage analyses. Evidence of significant linkage was observed for changes in fat-free mass with the S100A and the insulin-like growth factor I genes ( P = 0.0001). Suggestive evidence (2.0 ≤ Lod < 3.0; 0.0001 < P ≤ 0.001) was also observed for the changes in FM and %Fat at 1q31 and 18q21-q23, in %Fat with the uncoupling protein 2 and 3 genes, and in BMI at 5q14-q21. At baseline, suggestive evidence was observed for BMI at 8q23-q24, 10p15, and 14q11; for FM at 14q11; and for plasma leptin levels with the low-density lipoprotein receptor gene. This is the first genomic scan on genes involved in exercise-training-induced changes in body composition that could provide information on the determinants of weight loss.

Published
2001

22. A Genome-Wide Scan for Abdominal Fat Assessed by Computed Tomography in the Québec Family Study

Author

D. C. Rao, Yvon C. Chagnon, Louis Pérusse, Treva Rice, Jean-Pierre Després, Claude Bouchard, Sonia Roy, Michael A. Province, Michel Lacaille, My-Ann Ho-Kim, Monique Chagnon, and Simone Lemieux

Subjects
Adult, Genetic Markers, Male, Radiography, Abdominal, medicine.medical_specialty, Genetic Linkage, Endocrinology, Diabetes and Metabolism, Adipose tissue, Locus (genetics), Biology, chemistry.chemical_compound, Genetic linkage, Internal medicine, Adipocyte, Internal Medicine, medicine, Humans, Obesity, Genome, Autosome, Chromosome Mapping, Chromosome, Middle Aged, Surgery, Phenotype, Endocrinology, Adipose Tissue, chemistry, Genetic marker, Microsatellite, Female, Lod Score
Abstract

To identify chromosomal regions harboring genes influencing the propensity to store fat in the abdominal area, a genome-wide scan for abdominal fat was performed in the Québec Family Study. Cross-sectional areas of the amount of abdominal total fat (ATF) and abdominal visceral fat (AVF) were assessed from a computed tomography scan taken at L4-L5 in 521 adult subjects. Abdominal subcutaneous fat (ASF) was obtained by computing the difference between ATF and AVF. The abdominal fat phenotypes were adjusted for age and sex effects as well as for total amount of body fat (kilogram of fat mass) measured by underwater weighing, and the adjusted phenotypes were used in linkage analyses. A total of 293 microsatellite markers spanning the 22 autosomal chromosomes were typed. The average intermarker distance was 11.9 cM. A maximum of 271 sib-pairs were available for single-point (SIBPAL) and 156 families for multipoint variance components (SEGPATH) linkage analyses. The strongest evidence of linkage was found on chromosome 12q24.3 between marker D12S2078 and ASF (logarithm of odds [LOD] = 2.88). Another marker (D12S1045) located within 2 cM of D12S2078 also provided evidence of sib-pair linkage with ASF (P = 0.019), ATF (P = 0.015), and AVF (P = 0.0007). Other regions with highly suggestive evidence (P < 0.0023 or LOD ≥1.75) of multipoint linkage and evidence (P < 0.05) of single-point linkage, all for ASF, included chromosomes 1p11.2, 4q32.1, 9q22.1, 12q22-q23, and 17q21.1. Three of these loci (1p11.2, 9q22.1, and 17q21.1) are close to genes involved in the regulation of sex steroid levels, whereas two others (4q32.1 and 17q21.1) are in the proximity of genes involved in the regulation of food intake. This first genome-wide scan for abdominal fat assessed by computed tomography indicates that there may be several loci determining the propensity to store fat in the abdominal depot and that some of these loci may influence the development of diabetes in obese subjects.

Published
2001

23. NOS3 Glu298Asp Genotype and Blood Pressure Response to Endurance Training

Author

D. C. Rao, Yvon C. Chagnon, Treva Rice, Louis Pérusse, James S. Skinner, Jack H. Wilmore, Tuomo Rankinen, Jacques Gagnon, Claude Bouchard, and Arthur S. Leon

Subjects
Adult, Male, medicine.medical_specialty, Genotype, Nitric Oxide Synthase Type III, Endothelium, Hemodynamics, Blood Pressure, Physical exercise, Vasodilation, Nitric Oxide, Endurance training, Internal medicine, Internal Medicine, medicine, Humans, Family, Polymorphism, Genetic, Base Sequence, business.industry, Phenotype, medicine.anatomical_structure, Endocrinology, Blood pressure, Circulatory system, Physical Endurance, Female, Endothelium, Vascular, Gene polymorphism, Nitric Oxide Synthase, business
Abstract

Abstract —Endothelium-dependent vasodilation is a mechanism that may affect blood pressure response to endurance training. Because NO plays a central role in this process, the endothelial NO synthase gene is a good candidate for the regulation of exercise blood pressure. We investigated the associations between an endothelial NO synthase gene polymorphism (Glu298Asp) and endurance training–induced changes in resting and submaximal exercise blood pressure in 471 white subjects of the HERITAGE Family Study. Two submaximal exercise tests at 50 W were conducted both before and after a 20-week endurance training program. Steady-state exercise blood pressure was measured twice in each test with an automated unit. The Glu298Asp polymorphism was typed with a PCR-based method and digestion with Ban II. Both systolic and diastolic blood pressure at 50 W decreased in response to the training program, whereas resting blood pressure remained unchanged. The decrease in diastolic blood pressure at 50 W was greater ( P =0.0005, adjusted for age, gender, baseline body mass index, and baseline diastolic blood pressure at 50 W) in the Glu/Glu homozygotes (4.4 [SEM 0.4] mm Hg, n=187) than in the heterozygotes (3.1 [0.4] mm Hg, n=213) and the Asp/Asp homozygotes (1.3 [0.7] mm Hg, n=71). The genotype accounted for 2.3% of the variance in diastolic blood pressure at 50 W training response. Both the Glu298 homozygotes and the heterozygotes had a greater ( P =0.013) training-induced reduction in rate-pressure product at 50 W than the Asp298 homozygotes. These data suggest that DNA sequence variation in the endothelial NO synthase gene locus is associated with the endurance training–induced decreases in submaximal exercise diastolic blood pressure and rate-pressure product in sedentary normotensive white subjects.

Published
2000

24. Genome-Wide Linkage Analysis of Systolic and Diastolic Blood Pressure

Author

Louis Pérusse, Michael A. Province, Dabeeru C. Rao, Treva Rice, Claude Bouchard, Ingrid B. Borecki, Tuomo Rankinen, and Yvon C. Chagnon

Subjects
Male, medicine.medical_specialty, Genetic Linkage, Systole, Diastole, Genome Scan, Blood Pressure, Genetic determinism, Body Mass Index, Age Distribution, Quantitative Trait, Heritable, Genetic linkage, Physiology (medical), Internal medicine, medicine, Humans, Obesity, Sex Distribution, Risk factor, Aged, Genome, Human, business.industry, Quebec, Chromosome Mapping, Genetic Variation, Middle Aged, Physical Chromosome Mapping, Blood pressure, Endocrinology, Hypertension, Regression Analysis, Female, Lod Score, Restriction fragment length polymorphism, Cardiology and Cardiovascular Medicine, business, Polymorphism, Restriction Fragment Length, Microsatellite Repeats
Abstract

Background —Blood pressure (BP), an important risk factor for coronary heart disease, is a complex trait with multiple genetic etiologies. While some loci affecting BP variation are known (eg, angiotensinogen), there are likely to be novel signals that can be detected with a genome scan approach. Methods and Results —A genome-wide scan was performed in 125 random and 81 obese families participating in the Québec Family Study. A multipoint variance-components linkage analysis of 420 markers (353 microsatellites and 67 restriction fragment length polymorphisms) revealed several signals ( P P P P P P Conclusions —Multiple linkage regions support the notion that risk for hypertension is due to multiple (ie, oligogenic) susceptibility loci. Comparisons across the complete, random, and obese samples suggest that some regions are specific to BP and others may involve obesity (eg, pleiotropy, epistasis, or gene-environment interaction). Some of these areas harbor known candidates. Others involve novel regions, some of which replicate previous reports and provide a focus for future studies to identify novel genes that influence interindividual variation in BP.

Published
2000

25. Interactions among the α2-, β2-, and β3-adrenergic receptor genes and obesity-related phenotypes in the Quebec Family Study

Author

Olavi Ukkola, Yvon C. Chagnon, Guang Sun, S. John Weisnagel, Jean-Pierre Després, Tuomo Rankinen, Louis Pérusse, and Claude Bouchard

Subjects
Adult, Male, medicine.medical_specialty, Genotype, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Biology, Body Mass Index, Cohort Studies, chemistry.chemical_compound, Endocrinology, Receptors, Adrenergic, alpha-2, Polymorphism (computer science), Internal medicine, Abdomen, Receptors, Adrenergic, beta, medicine, Humans, Obesity, Allele, Deoxyribonucleases, Type II Site-Specific, Alleles, Abdominal obesity, Family Health, Polymorphism, Genetic, Cholesterol, Insulin, Homozygote, medicine.disease, Phenotype, Adipose Tissue, chemistry, Receptors, Adrenergic, beta-3, Female, Receptors, Adrenergic, beta-2, medicine.symptom, Body mass index, Lipoprotein
Abstract

The gene-gene interactions between markers in the alpha2-, beta2-, and beta3-adrenergic receptor (ADR) genes and obesity-related phenotypes were studied in the Quebec Family Study (QFS) cohort. The prevalence of the Arg allele of the Arg16Gly polymorphism in the beta2-ADR gene was higher (49%) in males with a body mass index (BMI) of 35 kg/m2 or higher versus those with a BMI less than 35 kg/m2 (33%; P = .010). The beta2-ADR gene Arg16Gly and Gln27Glu polymorphisms were associated with plasma total and low-density lipoprotein (LDL) cholesterol concentrations. In addition, the homozygotes for the 6.3-kb allele of DraI polymorphism in the alpha2-ADR gene had the lowest mean abdominal subcutaneous fat area (P = .012) and total fat area (P = .003), as well as insulin area, under the curve during an oral glucose tolerance test ([OGTT] P = .004). Several ADR gene-gene interaction effects on abdominal fat distribution and plasma lipids were detected. First, significant interactions between alpha2- and beta3-ADR genes were observed on total (P = .015) and subcutaneous (P = .004) abdominal fat. Second, interaction effects between alpha2- and beta2-ADR gene variants influenced total, high-density lipoprotein (HDL), and LDL cholesterol concentrations. Finally, there were interactions between markers within the beta2-ADR gene affecting plasma triglyceride concentrations and subcutaneous abdominal fat. From these results, we conclude that polymorphisms in the ADR genes contribute to body fat and plasma lipid variability in men. Gene-gene interactions among the ADR genes contribute to the phenotypic variability in abdominal obesity and plasma lipid and lipoprotein, but not in visceral fat levels.

Published
2000

26. Genomic scan for maximal oxygen uptake and its response to training in the HERITAGE Family Study*

Author

James S. Skinner, Arthur S. Leon, Dabeeru C. Rao, Louis Pérusse, Jack H. Wilmore, Claude Bouchard, Jacques Gagnon, Ingrid B. Borecki, Michael A. Province, Yvon C. Chagnon, Ping An, Tuomo Rankinen, and Treva Rice

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, Genotype, Genetic Linkage, Physiology, Physical Exertion, Biology, Oxygen Consumption, Quantitative Trait, Heritable, Physiology (medical), Internal medicine, medicine, Humans, Aged, Family Health, Genetics, Genome, Human, Chromosome Mapping, VO2 max, DNA, Middle Aged, Endocrinology, Exercise Test, Physical Endurance, Regression Analysis, Female, Microsatellite Repeats
Abstract

This study aimed to identify human genomic regions that are linked to maximal oxygen uptake (V˙o 2 max) in sedentary individuals or to the responsiveness ofV˙o 2 max to a standardized endurance training program. The results of a genomic scan based on 289 polymorphic markers covering all 22 pairs of autosomes performed on the Caucasian families of the HERITAGE Family Study are presented. The mean spacing of the markers was 11 cM, and a total of 99 families and 415 pairs of siblings were available for the study.V˙o 2 max in the sedentary state was adjusted for the effects of age, sex, body mass, fat mass, and fat-free mass, whereas theV˙o 2 maxresponse was adjusted for age and baseline level of the phenotype. Two analytic strategies were used: a single-point linkage procedure using all available pairs of siblings (SIBPAL) and a multipoint variance components approach using all the family data (SEGPATH). Results indicate that linkages at P values of 0.01 and better are observed with markers on 4q, 8q, 11p, and 14q forV˙o 2 max before training and with markers on 1p, 2p, 4q, 6p, and 11p for the change inV˙o 2 max in response to a 20-wk standardized endurance training program. These chromosomal regions harbor many genes that may qualify as candidate genes for these quantitative traits. They should be investigated in this and other cohorts.

Published
2000

27. The Na+-K+-ATPase α2 gene and trainability of cardiorespiratory endurance: the HERITAGE Family Study

Author

Jacques Gagnon, James S. Skinner, Tuomo Rankinen, Arthur S. Leon, Ingrid B. Borecki, D. C. Rao, Louis Pérusse, Claude Bouchard, Jack H. Wilmore, and Yvon C. Chagnon

Subjects
Adult, Male, medicine.medical_specialty, Genotype, Genetic Linkage, Physiology, Physical exercise, White People, NA K EXCHANGING ATPASE, Cardiovascular Physiological Phenomena, Cohort Studies, Physiology (medical), Internal medicine, medicine, Humans, Exercise physiology, Na+/K+-ATPase, Muscle, Skeletal, Exercise, Genetics, Polymorphism, Genetic, business.industry, VO2 max, Cardiorespiratory fitness, Exons, Middle Aged, Adaptation, Physiological, Endocrinology, Haplotypes, Physical Fitness, Physical performance, Physical Endurance, Female, Bicycle ergometer, Sodium-Potassium-Exchanging ATPase, business
Abstract

The Na+-K+-ATPase plays an important role in the maintenance of electrolyte balance in the working muscle and thus may contribute to endurance performance. This study aimed to investigate the associations between genetic variants at the Na+-K+-ATPase α2 locus and the response (Δ) of maximal oxygen consumption (V˙o2 max) and maximal power output (W˙max) to 20 wk of endurance training in 472 sedentary Caucasian subjects from 99 families. V˙o2 maxandW˙maxwere measured during two maximal cycle ergometer exercise tests before and again after the training program, and restriction fragment length polymorphisms at the Na+-K+-ATPase α2 (exons 1 and 21–22 with Bgl II) gene were typed. Sibling-pair linkage analysis revealed marginal evidence for linkage between the α2 haplotype and ΔV˙o2 max( P= 0.054) and stronger linkages between the α2 exon 21–22 marker ( P = 0.005) and α2 haplotype ( P = 0.003) and ΔW˙max. In the whole cohort, ΔV˙o2 maxin the 3.3-kb homozygotes of the exon 1 marker ( n = 5) was 41% lower than in the 8.0/3.3-kb heterozygotes ( n = 87) and 48% lower than in the 8.0-kb homozygotes ( n = 380; P = 0.018, adjusted for age, gender, baselineV˙o2 max, and body weight). Among offspring, 10.5/10.5-kb homozygotes ( n = 14) of the exon 21–22 marker showed a 571 ± 56 (SE) ml O2/min increase inV˙o2 max, whereas the increases in the 10.5/4.3-kb ( n = 93) and 4.3/4.3-kb ( n= 187) genotypes were 442 ± 22 and 410 ± 15 ml O2/min, respectively ( P = 0.017). These data suggest that genetic variation at the Na+-K+-ATPase α2 locus influences the trainability ofV˙o2 maxin sedentary Caucasian subjects.

Published
2000

28. Linkages and associations between the leptin receptor (LEPR) gene and human body composition in the Québec Family Study

Author

Claude Bouchard, Monique Chagnon, Yvon C. Chagnon, Wendy K. Chung, Rudolph L. Leibel, and Louis Pérusse

Subjects
Adult, Male, medicine.medical_specialty, Genotype, Genetic Linkage, Endocrinology, Diabetes and Metabolism, Medicine (miscellaneous), Receptors, Cell Surface, Composition of the human body, Biology, Polymerase Chain Reaction, Body Mass Index, Polymorphism (computer science), Internal medicine, medicine, Humans, Obesity, Allele, Allele frequency, Alleles, Nutrition and Dietetics, Quebec, Exons, medicine.disease, Introns, Skinfold Thickness, Endocrinology, Adipose Tissue, Body Composition, Lean body mass, Receptors, Leptin, Female, Carrier Proteins, Body mass index, Polymorphism, Restriction Fragment Length, Microsatellite Repeats
Abstract

OBJECTIVE: To investigate linkage and association between the leptin receptor (LEPR) gene and body composition variables in the Quebec Family Study (QFS). DESIGN: Single-point linkage analysis using families, and covariance and chi-square analyses using normal weight and obese unrelated subjects from QFS. SUBJECTS: 169 nuclear families were used for linkage study. 308 unrelated subjects (146 males; 162 females) from these families were used for chi-square testing of genotype and allele distributions between subjects with body mass index (BMI) < 27 kg=m 2 (na 167) and those with BMI 27 kg=m 2 (na 141), and for a series of covariance analyses using age, plus height for fat mass (FM) and fat free mass (FFM), as covariates. A corrected P value (P*) for multiple tests has been calculated according to P*a 1-(1-P) number of phenotypes . MEASUREMENTS: Variables were BMI (in kg=m 2 ), sum of six skinfolds (SF6 in mm), FM (in kg), percent body fat (%FAT) and FFM (in kg). Polymerase chain react restricted fragment length polymorphisms PCR-RFLP) was used to identified a K109R substitution in exon 4, a Q223R in exon 6, a K656N in exon 14 and an automatic DNA sequencer for a CA microsatellite repeat in intron 3, and heteroduplex pattern on non-denaturing gel for a CTTT repeat in intron 16. RESULTS: Good evidence of linkage was observed for Q223R with FM (Pa 0.005; P*a 0.02), and for the CTTT repeat with FFM (Pa 0.007; P*a 0.03). Weaker linkages (0.02P 0.05) were also observed between Q223R and BMI, SF6 and FFM, between the CA repeat and BMI, SF6 and FM, and between the CTTT repeat and FM. Moreover, FFM values were found to be different among genotypes for the CTTT repeat polymorphism with heavier females, carriers of the 123* allele at the CTTT repeat, showing 4 kg less of FFM (43.6 1.0, na 21 vs 47.7 0.8, na 30; Pa 0.005; P*a 0.02) than non-carriers. Also, at the Q223R polymorphism, in lower BMI males, carriers of the Q223 allele were 4 kg lighter in FFM (53.4 0.6, na 47 vs 56.6 0.9, na 18; Pa 0.005; P*a 0.02) than non-carriers. No significant differences were observed between lower and higher BMI subjects in genotype and allele frequency distributions for any of the polymorphisms. CONCLUSIONS: These results indicate that the LEPR gene is involved in the regulation of the body composition in human particularly of FFM in the QFS.

Published
1999

29. DNA polymorphism in the uncoupling protein 1 (UCP1) gene has no effect on obesity related phenotypes in the Swedish Obese Subjects cohorts

Author

Claude Bouchard, Jacques Gagnon, Lars Sjöström, F Lago, Louis Pérusse, Yvon C. Chagnon, Ingmar Näslund, and Lauren Lissner

Subjects
Adult, Male, medicine.medical_specialty, Genotype, Endocrinology, Diabetes and Metabolism, Population, Medicine (miscellaneous), Weight Gain, Polymerase Chain Reaction, Ion Channels, Body Mass Index, Cohort Studies, Mitochondrial Proteins, Polymorphism (computer science), Internal medicine, medicine, Humans, Point Mutation, Uncoupling protein, Obesity, education, Alleles, Uncoupling Protein 1, Sweden, education.field_of_study, Nutrition and Dietetics, business.industry, Case-control study, Membrane Proteins, DNA, Middle Aged, medicine.disease, Phenotype, Endocrinology, Body Constitution, Female, medicine.symptom, Carrier Proteins, business, Weight gain, Body mass index, Polymorphism, Restriction Fragment Length
Abstract

To investigate the relationships between the A-G point mutation at position -3826 bp in the 5' flanking domain of the uncoupling protein 1 (UCP1 A-3826G) and some obesity phenotypes in the Swedish Obese Subjects (SOS) cohorts of obese and non-obese men and women. Previous studies have supported the hypothesis of an association between the UCP1 A-3826G polymorphism and body weight regulation in humans.Case-control study comparing obese subjects from the SOS registry and a sample of the Swedish general population (body mass index (BMI)27 kg/m2) with respect to genotype and allele frequencies of the UCP1 A-3826G polymorphism.A total of 985 Swedish subjects including 674 obese (310 Male; 364 Female) and 311 non-obese subjects (54 Male; 257 Female) from the SOS cohorts.DNA was extracted from total blood and genotyped by PCR-RFLP. Obesity-related phenotypes include weight history for SOS obese cohort and current weight, BMI, waist circumference and waist to hip ratio (WHR) for obese and normal weight subjects.No significant difference in the allelic frequencies between obese and non-obese subjects (0.25 vs 0.24; P = 0.67). In both genders, current weight, BMI, waist circumference, WHR and weight gain over time (either measures of maximal weight ever achieved minus weight at 20 y or current weight minus weight at 20 y) were similar in carriers and non-carriers of the UCP1 A-3826G mutation (P0.05). Similar results were obtained when the three genotypes were compared.In contrast to what was found in other populations, the UCP1 A-3826G sequence variation is not associated with obesity-related phenotypes and weight gain over time in subjects from the SOS cohorts.

Published
1998

30. Muscle-specific creatine kinase gene polymorphism and ??VO2max in the HERITAGE Family Study

Author

Claude Bouchard, Louis Pérusse, Yvon C. Chagnon, Jacques Gagnon, Jean-Aimé Simoneau, Monique Chagnon, Arthur S. Leon, James S. Skinner, D. C. Rao, Miguel A. Rivera, J. H. Wilmore, and F. T. Dionne

Subjects
Adult, Male, medicine.medical_specialty, Genotype, Offspring, Physical Therapy, Sports Therapy and Rehabilitation, Physical exercise, Polymerase Chain Reaction, Oxygen Consumption, Polymorphism (computer science), Endurance training, Internal medicine, medicine, Humans, Orthopedics and Sports Medicine, Allele, Muscle, Skeletal, Creatine Kinase, Alleles, Analysis of Variance, Chi-Square Distribution, Physical Education and Training, Polymorphism, Genetic, biology, Genetic Variation, VO2 max, Middle Aged, Endocrinology, Linear Models, Physical Endurance, biology.protein, Female, Creatine kinase
Abstract

This study examined the association between a DNA polymorphism in the muscle-specific creatine kinase (CKMM) gene and VO2max in the sedentary state, as well as its response (deltaVO2max) to a standardized 20-wk endurance training program. The subjects were 160 biologically unrelated Caucasian parents (80 women, 80 men) and 80 biologically unrelated adult offspring of the HERITAGE Family Study. The CKMM polymorphism was detected by PCR and digestion with the NcoI restriction enzyme. VO2max was measured during maximal cycle ergometer tests. VO2max was 2119 +/- 45 mL x min(-1) (mean +/- SE) or 26 +/- 0.4 mL x kg(-1) x min(-1). Both sexes had a significant (P0.05) increase in the deltaVO2max (women = 283 +/- 20 mL x min[-1] and men = 363 +/- 25 mL x min[-1]). Allele and genotype frequencies were not significantly different (P0.05) between sexes. Age and sex adjusted VO2max was significantly (P = 0.007) associated with the CKMM genotype in the parents, whereas no association (P0.05) was observed in the offspring. DeltaVO2max values adjusted for age, sex, VO2max, and body mass were characterized by genotype differences in both parents (P = 0.0004) and offspring (P = 0.0025). A significantly (P0.05) lower deltaVO2max to endurance training was detected in both parents and offspring homozygotes for the rare allele. The genotype accounted for at least 9% of the variance in deltaVO2max. These results indicate that the NcoI polymorphism in the 3' untranslated region of the muscle-specific creatine kinase gene is associated with the deltaVO2max to endurance training.

Published
1997

31. Genetics of obesity: advances from rodent studies

Author

Claude Bouchard and Yvon C. Chagnon

Subjects
Leptin, Male, medicine.medical_treatment, Mice, Obese, Mice, Inbred Strains, Carboxypeptidases, Quantitative trait locus, Biology, medicine.disease_cause, Mice, Insulin resistance, Diabetes mellitus, Diabetes Mellitus, Genetics, medicine, Animals, Humans, Obesity, Adaptor Proteins, Signal Transducing, Mutation, Genetics of obesity, Insulin, Carboxypeptidase H, Chromosome Mapping, Proteins, medicine.disease, Phenotype, Rats, Disease Models, Animal, Agouti Signaling Protein, Intercellular Signaling Peptides and Proteins, Female
Abstract

Maior advances have occurred over the past four years, but particularly in the past 18 months, concerning the genetic hasis of obesity in rodent models. The cloning of the five genes in which mutations are known to t.'ause obesity in mouse and rat, and the identification of the gene products of all but one of these genes, has fostered a series of innovative studies in human subjecLs. Similarly, the uncovering of se~'e:ral quantitative trait loci (QTL) infloencing body mass, body fat content or fat topography frortl cros.ses nf informative strains of mice and rats has provided a new impetus to the study of polygenic Slngle-gene-mmation models obesity in rodents and humans. These The single-gene-mutation rodent recent advances have generated a models of obesity are identified and great deal of optimism regarding the some of their genetic characteristics possibility of identil~ing the genes are summarized in Table 1. The obese responsible for the snsceptibility to (oh) and diabetes (db) mutations the common forms of obesity in huhave an almost identical phenotype marls and their co-morbidities, such when bred on the same genetic a~ ~ardiovascular diseases, insulin rebackground: juvenile onset of severe sistance and non-insuUn-dependent obesity adsing from an excess fat diabetes mellims, hypertension and in all depots, excess food intake or others. This article addresses the hyperphagia, insulin resistance, g|umajor features of the advances in cose intolerance and diabetes. A simisingle-gene-mutation rodent models, lar phenotype is observed in the QTL in mouse and rat, and their Agoutiyellow(A v) mice, except for impact on human obesity research, an adult onset of a more moderare

Published
1996

32. Relationship between cortisol level and prevalent/incident cognitive impairment and its moderating factors in older adults

Author

Michel Préville, Carol Hudon, Yvon C. Chagnon, Djamal Berbiche, Hélène Forget, and Olivier Potvin

Subjects
Male, medicine.medical_specialty, Canada, Cortisol awakening response, Hydrocortisone, Anxiety, Effect Modifier, Epidemiologic, Sex Factors, Interview, Psychological, medicine, Prevalence, Humans, Cognitive decline, Psychiatry, Saliva, Geriatric Assessment, Depression (differential diagnoses), Aged, Aged, 80 and over, Intelligence Tests, Models, Statistical, Intelligence quotient, Depression, Cognitive disorder, Cognition, Health Status Disparities, medicine.disease, Psychiatry and Mental health, Clinical Psychology, Educational Status, Female, Geriatrics and Gerontology, medicine.symptom, Psychology, Cognition Disorders, Gerontology, medicine.drug
Abstract

Background: The objectives of this study were to examine the factors modifying the relationship between cortisol level and prevalent/incident cognitive impairment in older adults and to verify whether these relationships were non-linear.Methods: Data were collected from 1,226 individuals aged 65 and older by two in-home interviews separated by 12 months. Cortisol level was measured using saliva samples taken at the beginning of the baseline interview before cognitive, mental, and physical health evaluations. Prevalent and incident cognitive impairment were defined using the Mini-Mental State Examination scores according to normative data for age, education level, and sex.Results: High morning cortisol level increased the risk of incident cognitive impairment in participants with anxiety or depressive episode while low cortisol level increased the risk in participants without anxiety or depressive episode. In high educated participants, but not in low educated participants, high morning cortisol level was associated with prevalent cognitive impairment and high afternoon cortisol level increased the risk of incident cognitive impairment. The results also suggested that lower morning cortisol values could increase the risk of incident cognitive impairment in individuals with few chronic diseases. A curvilinear relationship was observed between morning cortisol and the probability of incident cognitive impairment, but further analyses suggested that it was likely explained by anxiety and depressive episode.Conclusions: These results suggest that cognitive impairment in older adults is linked to higher or lower cortisol level depending on characteristics such as anxiety, depressive episode, education level, and physical health.

Published
2012

33. A new strategy for linkage analysis under epistasis taking into account genetic heterogeneity

Author

Jordie Croteau, Chantal Mérette, Alain Fournier, Alexandre Bureau, Yvon C. Chagnon, Michel Maziade, and Marc-André Roy

Subjects
Male, Linkage disequilibrium, Bipolar Disorder, Genetic Linkage, Pedigree chart, Locus (genetics), Penetrance, Biology, Genetic Heterogeneity, Genetic linkage, Genetics, Humans, Computer Simulation, Family, Genetics (clinical), Genes, Dominant, Models, Genetic, Genetic heterogeneity, Epistasis, Genetic, Complete linkage, Pedigree, Schizophrenia, Epistasis, Female
Abstract

Background/Aims: Epistasis, the biological interaction of multiple genes modulating their individual effects, is likely omnipresent in complex diseases, and modelling epistasis in linkage studies can help detect loci with little marginal effect and detect epistatic effects themselves. We propose a complete three-step strategy for parametric linkage analysis under epistasis and heterogeneity in extended pedigrees. Methods: (1) Loci most likely involved in epistatic interactions are pre-screened using two-locus one-marker analyses. (2) Among selected loci, linkage to each locus is evaluated conditionally on linkage information at another locus under two-locus epistatic models. Linkage statistics are maximized over a space of epistatic models to avoid misspecification of model parameters. (3) Families linked to the conditioning locus are selected to deal with heterogeneity between pairs of epistatically interacting loci and other unlinked loci. Properties of conditional linkage statistics prevent the introduction of bias. Results: Simulations reveal important gains in power to detect a locus with weak marginal effect involved in epistatic interaction. Application of our methods to schizophrenia and bipolar disorder in Eastern Quebec kindreds suggests epistasis between three locus pairs for bipolar disorder: 8p11-16p13, 15q11-16p13 and 18q12-15q11. Conclusion: These results suggest that the proposed strategy is powerful for tackling complex phenotypes involving epistasis and heterogeneity.

Published
2008

34. Evidence of a quantitative trait locus for energy and macronutrient intakes on chromosome 3q27.3: the Quebec Family Study

Author

Simone Lemieux, Anne C. Choquette, Marie-Claude Vohl, Angelo Tremblay, Louis Pérusse, Claude Bouchard, and Yvon C. Chagnon

Subjects
Adult, Male, Genotype, Genetic Linkage, Medicine (miscellaneous), Locus (genetics), Quantitative trait locus, Biology, Cohort Studies, Quantitative Trait, Heritable, Genetic linkage, Risk Factors, Dietary Carbohydrates, Humans, Obesity, Gene, Nuclear family, Genetics, Nutrition and Dietetics, Adiponectin, Genome, Human, Quebec, Chromosome Mapping, Middle Aged, Dietary Fats, Diet Records, Chromosomes, Human, Pair 1, Female, Chromosomes, Human, Pair 3, Dietary Proteins, Energy Intake, Body mass index
Abstract

BACKGROUND Little is known about the genes influencing dietary energy and nutrient intakes, despite evidence that these intakes are influenced by genetic factors. OBJECTIVE We aimed to identify, by using a genome-wide linkage analysis, chromosomal regions harboring genes that affect energy and macronutrient intakes. DESIGN Energy, carbohydrate, lipid, and protein intakes were assessed in 836 subjects from 217 families by using a 3-d dietary record. A total of 443 markers were genotyped and tested for linkage; age- and sex-adjusted energy and macronutrient intakes were expressed in grams and as percentages of total energy intake. Regression-based (Haseman-Elston) and variance-component (MERLIN) methods were applied to test for linkage with dietary data. A maximum of 454 sibpairs from 217 nuclear families were available for analysis. RESULTS The genome scan provided suggestive evidence (P < or = 0.0023) for the presence of 6 quantitative trait linkages influencing total caloric and macronutrient intakes in the Quebec Family Study. Of these, multiple linkages were found on chromosome 3q27.3, in a region harboring the adiponectin gene, at marker D3S1262 for energy [logarithm of odds (LOD): 2.24], carbohydrate (LOD: 2.00), and lipid (LOD: 1.65) intakes. The peak linkages for carbohydrate, lipid, and protein intakes were found on chromosomes 1p32.2 (LOD: 2.39), 1p35.2 (LOD: 2.41), and 10p15.3 (LOD: 2.72), respectively. The linkage results remained significant after adjustment for body mass index, which suggested that the genes underlying these quantitative trait linkages influence dietary intake independent of body size. CONCLUSION The linkage on chromosome 3q27.3 with energy, lipid, and carbohydrate intakes suggests that this region of the genome may harbor genes that influence energy and macronutrient intakes in humans.

Published
2008

35. Resting metabolic rate and respiratory quotient: results from a genome-wide scan in the Quebec Family Study

Author

Yvon C. Chagnon, Louis Pérusse, Peter Jacobson, Angelo Tremblay, Tuomo Rankinen, and Claude Bouchard

Subjects
Proband, Male, Candidate gene, Genotype, Genetic Linkage, Population, Quantitative Trait Loci, Medicine (miscellaneous), Locus (genetics), Biology, Quantitative trait locus, Oxygen Consumption, Locus heterogeneity, medicine, Humans, Family, Genetic Predisposition to Disease, Obesity, education, Genetics, Metabolic Syndrome, education.field_of_study, Nutrition and Dietetics, Genome, Human, Quebec, Chromosome Mapping, Genetic Variation, Calorimetry, Indirect, medicine.disease, Phenotype, Basal metabolic rate, Microsatellite, Female, Basal Metabolism, Lod Score
Abstract

Background: Genes influencing resting metabolic rate (RMR) and respiratoryquotient(RQ)representcandidategenesforobesity,type 2 diabetes, and the metabolic syndrome because of the involvement of these traits in energy balance and substrate oxidation. Objective:We conducted a genome-wide scan for quantitative trait loci (QTL) contributing to the variability in RMR and RQ. Design: Regression-based and variance components–based genome-wide autosomal scans on RMR and RQ phenotypes, obtained from indirect calorimetry, were performed in 169 families ascertained via an obese proband or from the general population. Results: We found evidence for linkage to RMR on chromosomes 3q26.1 (lod 2.74), 1q21.2 (2.44), and 22q12.3 (1.33). QTL influencing RQ were found on chromosomes 12q13 (1.65) and 14q22 (1.83) when the analyses were performed in all families. Considerable locus heterogeneity within this population was suggested becausemostofthefamilieswereunlinkedtoanyonequantitativetrait locus. Significant associations between traits and linked microsatellites were detected within the linked, informative subsets. Conclusions: We found several new QTL for energy metabolism, but the QTL on 1q may be a replication of the one reported in Pima Indians.All3RMRlinkagesoverlappedregionspreviouslylinkedto the metabolic syndrome or its components, and the significant association between RMR and the metabolic syndrome in the present cohort reinforces this relation. We conclude that considerable locus heterogeneityexistsevenwithinpopulations,whichshouldbetaken into account when considering candidate gene studies of energy metabolism phenotypes and other complex traits. Am J Clin Nutr 2006;84:1527–33.

Published
2006

36. Linkage Between Markers in the Vicinity of the Uncoupling Protein 2 Gene and Resting Metabolic Rate in Humans

Author

Claude Bouchard, Craig H Warden, Yvon C. Chagnon, Louis Pérusse, and Daniel Ricquier

Subjects
Adult, Male, Genetic Linkage, Locus (genetics), Biology, Ion Channels, Mitochondrial Proteins, Gene mapping, Genetic linkage, Genetics, Humans, Uncoupling protein, Uncoupling Protein 2, Resting energy expenditure, Molecular Biology, Gene, Genetics (clinical), Aged, Aged, 80 and over, Chromosomes, Human, Pair 11, Membrane Transport Proteins, Proteins, General Medicine, Middle Aged, Basal metabolic rate, Body Composition, Microsatellite, Female, Energy Metabolism, Microsatellite Repeats
Abstract

The recent cloning of a gene that codes for a novel uncoupling protein, UCP2, which is expressed in a wide range of adult human tissues, has raised the possibility that it may be involved in regulation of energy balance. To explore this concept we have investigated potential linkage relationships between three microsatellite markers which encompass the UCP2 gene location on 11q13 with resting metabolic rate (RMR), body mass index, percentage body fat (%FAT) and fat mass (FM) in 640 individuals from 155 pedigrees from the Québec Family Study. Using a linkage analysis strategy based on sibling, avuncular, grandparental and cousin pairs, strong evidence of linkage was found between the marker D11S911 (P = 0.000002) and RMR, with more moderate evidence for D11S916 (P = 0.006) and D11S1321 (P = 0.02). Suggestive evidence of linkage was also observed between D11S1321 and %FAT (P = 0.04) and FM (P = 0.02). It is concluded that the three markers encompassing the UCP2 locus and spanning a 5 cM region on 11q13 are linked to resting energy expenditure in adult humans. The evidence is strong enough to warrant a search for DNA sequence variation in the gene itself.

Published
1997

37. Melanocortin-4 receptor gene and physical activity in the Québec Family Study

Author

Claude Bouchard, Ruth J. F. Loos, André J. Tremblay, Louis Pérusse, Tuomo Rankinen, and Yvon C. Chagnon

Subjects
Male, medicine.medical_specialty, Candidate gene, Offspring, Endocrinology, Diabetes and Metabolism, Medicine (miscellaneous), Physical exercise, Biology, Internal medicine, Genotype, medicine, Humans, Genetic Predisposition to Disease, Exercise, Nutrition and Dietetics, Chi-Square Distribution, Polymorphism, Genetic, Quebec, Middle Aged, medicine.disease, Obesity, Physical activity level, Melanocortin 4 receptor, Endocrinology, Phenotype, Receptor, Melanocortin, Type 4, Female, Body mass index
Abstract

Physical inactivity is a risk factor for numerous chronic diseases. Low compliance with interventions to increase activity suggests involvement of biological systems. OBJECTIVE: To examine whether sequence variants in genes encoding neuropeptides and receptors in the arcuate and paraventricular nucleus of the hypothalamus contribute to variations in physical activity level in the Quebec Family Study. METHODS: We genotyped polymorphisms in the melanocortin-4 receptor (MC4R), melanocortin-3 receptor (MC3R), neuropeptide-Y (NPY), neuropeptide-Y Y1 receptor (NPY Y1R), cocaine- and amphetamine-regulated transcript (CART), agouti-related protein (AGRP), and pro-opiomelanocortin (POMC) genes in 669 subjects (age (X±s.d.): parents: 52±3.4 y; offspring: 28±8.7 y). Total physical activity, moderate-to-strenuous activity, and inactivity phenotypes were estimated from a three-day record. The past year's physical activity level was assessed from a questionnaire. Associations between the physical activity phenotypes and the polymorphisms were analyzed using the MIXED model (SAS). RESULTS: The MC4R-C-2745T variant showed significant associations with physical activity phenotypes. The lowest moderate-to-strenuous activity scores (P=0.005) and the highest inactivity scores (P=0.01) emerged in the T/T genotype. Exclusion of obese subjects increased the association. For inactivity, the association of the MC4R-C-2745T variant was strongest in the offspring (P=0.002). The T/T offspring had both the highest inactivity score and the lowest body mass index. The CART-A1475G variant modified the associations with MC4R-C-2745T; T/T homozygotes had the lowest activity scores when they also had the A/A CART-A1475G genotype. No significant associations were observed with polymorphisms in the other neuropeptides. CONCLUSION: These findings suggest that DNA sequence variation at the MC4R gene locus may contribute to the propensity to be sedentary.

Published
2004

38. Compendium of genome-wide scans of lipid-related phenotypes: adding a new genome-wide search of apolipoprotein levels

Author

Yohan, Bossé, Yvon C, Chagnon, Jean-Pierre, Després, Treva, Rice, D C, Rao, Claude, Bouchard, Louis, Pérusse, and Marie-Claude, Vohl

Subjects
Adult, Genetic Markers, Male, Apolipoproteins, Phenotype, Genetic Linkage, Humans, Female, Lod Score, Middle Aged
Abstract

The genetic dissection of complex inherited diseases is a major challenge. Despite limited success in finding genes, substantial data based on genome-wide scan strategies is now available for a variety of diseases and related phenotypes. This can perhaps best be appreciated in the field of lipid and lipoprotein levels, where the amount of information generated is becoming overwhelming. We have created a database containing the results from whole-genome scans of lipid-related phenotypes undertaken to date. The usefulness of this database is demonstrated by performing a new autosomal genomic scan on apolipoprotein B (apoB), LDL-apoB, and apoA-I levels, measured in 679 subjects of 243 nuclear families. Linkage was tested using both allele-sharing and variance-component methods. Only two loci provided support for linkage with both methods: a LDL-apoB locus on 18q21.32 and an apoA-I locus on 3p25.2. Adding those findings to the database highlighted the fact that the former is reported as a lipid-related locus for the first time, whereas the latter has been observed before. However, concerns arise when displaying all data on the same map, because a large portion of the genome is now covered with loci supported by at least suggestive evidence of linkage.

Published
2004

39. Leptin and leptin receptor gene polymorphisms and changes in glucose homeostasis in response to regular exercise in nondiabetic individuals: the HERITAGE family study

Author

Timo A, Lakka, Tuomo, Rankinen, S John, Weisnagel, Yvon C, Chagnon, Hanna-Maaria, Lakka, Olavi, Ukkola, Normand, Boulé, Treva, Rice, Arthur S, Leon, James S, Skinner, Jack H, Wilmore, D C, Rao, Richard, Bergman, and Claude, Bouchard

Subjects
Adult, Blood Glucose, Leptin, Male, Polymorphism, Genetic, Homozygote, Black People, Receptors, Cell Surface, Fasting, Middle Aged, White People, Glucose, Homeostasis, Humans, Insulin, Receptors, Leptin, Female, Insulin Resistance, Exercise, Alleles
Abstract

We recently reported that a genomic region close to the leptin locus was linked to fasting insulin response to exercise training in nondiabetic white subjects. We tested the hypothesis that common exonic variants in the leptin (LEP) and leptin receptor (LEPR) genes modify the effects of regular physical activity on glucose homeostasis in nondiabetic whites (n = 397) and blacks (n = 143). In whites, exercise increased insulin sensitivity index (P = 0.041) and disposition index (P = 0.046) in the LEPR 109R allele carriers but not in the K109K homozygotes, increased glucose disappearance index more in the R109R homozygotes than in the K109 allele carriers (P = 0.039), and decreased fasting glucose only in the 109R allele carriers (P = 0.018). We also found an interaction between the LEP A19G and LEPR K109R polymorphisms on the change in fasting insulin in whites (P = 0.010). The association between the LEP A19G polymorphism and the change in insulin was evident only in the LEPR 109R carriers (P = 0.019). The decrease in insulin was strongest in the LEP A19A homozygotes who carried the LEPR 109R allele. Similar interaction was observed in blacks (P = 0.046). Variations in the LEP and LEPR genes are associated with the magnitude of the effects of regular exercise on glucose homeostasis in nondiabetic individuals.

Published
2004

40. Ala67Thr polymorphism in the Agouti-related peptide gene is associated with inherited leanness in humans

Author

Daniel L, Marks, Nathalie, Boucher, Christian-Marc, Lanouette, Louis, Pérusse, Gregor, Brookhart, Anthony G, Comuzzie, Yvon C, Chagnon, and Roger D, Cone

Subjects
Adult, Leptin, Polymorphism, Genetic, Genotype, Body Weight, Homozygote, Proteins, Transfection, PC12 Cells, Body Mass Index, Rats, Immunoenzyme Techniques, Gene Frequency, Thinness, Animals, Humans, Intercellular Signaling Peptides and Proteins, Agouti-Related Protein, Female
Abstract

A role for melanocortin signaling in the regulation of body weight in humans has been clearly established. Haploinsufficiency of the type 4 melanocortin receptor is associated with early-onset obesity, implying that this receptor provides an important tonic inhibition of weight gain. Agouti-related peptide (AGRP) is an endogenous antagonist of melanocortin signaling. Therefore, loss of AGRP function could lead to the expression of a lean phenotype. We investigated the potential role of AGRP in human weight regulation by examining the association between the Ala67Thr AGRP polymorphism and indices of body composition. Significant associations were found between homozygosity for this mutation (n = 8) and body composition phenotype in 874 subjects of the Quebec family study (QFS). By PCR-RFLP analysis, we have identified eight individuals who are homozygous for the 67Thr variant allele within the QFS population, where none were observed in SAFHS. The eight QFS homozygote individuals have lower weight (-16%; P = 0.02), body mass index (-17%; P = 0.01), fat free mass (-9%; P = 0.002), fat mass (FM) (-20%; P = 0.04), and leptin (-20%; P = 0.02) when compared to those carrying at least one 67Ala allele. Individuals homozygous for the 67Thr allele had a BMI that was either at or slightly below an ideal range for their age. Thus, the Ala67Thr AGRP polymorphism is associated with lower body weight in humans, with the largest effect being observed on body FM. We did not observe any difference in the stability or cellular distribution of the mutant protein in a heterologous expression system, thus the mechanism of this effect requires further investigation.

Published
2004

41. Genome-wide linkage scan for physical activity levels in the Quebec Family study

Author

Treva Rice, Riitta L Simonen, D. C. Rao, Louis Pérusse, Quebec Family Study, Yvon C. Chagnon, Tuomo Rankinen, and Claude Bouchard

Subjects
Genetics, Adult, Male, Genome, Human, Quantitative Trait Loci, Physical activity, Quebec, Population genetics, Chromosome Mapping, Physical Therapy, Sports Therapy and Rehabilitation, Locus (genetics), Biology, Middle Aged, Motor Activity, Phenotype, Genome, Genetic determinism, Cohort Studies, Humans, Orthopedics and Sports Medicine, Family, Female, Genome wide linkage
Abstract

It is commonly recognized that there is familial aggregation for physical activity level. However, the genes and sequence variants responsible for the familial clustering have not been investigated. We performed a genome-wide linkage scan based on 432 markers typed in 767 subjects from 207 families of the Quebec Family study with the aim of identifying loci affecting physical activity levels. Four physical activity level phenotypes were used.Promising evidence of linkage (P0.0023) was found for physical inactivity on chromosome 2p22-p16. Suggestive linkages (0.0023P0.01) were found for inactivity (7p11.2, 20q13.1), total physical activity (13q22-q31), moderate to strenuous physical activity (4q28.2, 7p11.2, 9q31.1, 13q22-q31), and time spent in physical activity (11p15 and 15q13.3).This study identified several chromosomal regions harboring genes that may contribute to the propensity to be physically active or sedentary.

Published
2003

42. A quantitative trait locus on 7q31 for the changes in plasma insulin in response to exercise training: the HERITAGE Family Study

Author

Timo A, Lakka, Tuomo, Rankinen, S John, Weisnagel, Yvon C, Chagnon, Treva, Rice, Arthur S, Leon, James S, Skinner, Jack H, Wilmore, D C, Rao, and Claude, Bouchard

Subjects
Genetic Markers, Male, Canada, Genetic Linkage, Genome, Human, Quantitative Trait Loci, Black People, Chromosome Mapping, United States, White People, Cohort Studies, Diabetes Mellitus, Type 1, Physical Endurance, Humans, Insulin, Family, Female, Exercise, Chromosomes, Human, Pair 7
Abstract

Several genome-wide linkage scans have been carried out to identify quantitative trait loci for type 2 diabetes and related metabolic phenotypes. However, no previous linkage scans have focused on the response to exercise training of relevant metabolic traits. We performed a genome-wide linkage scan for baseline fasting glucose, insulin, and C-peptide and their responses to a 20-week exercise training program in nondiabetic white and black men and women from the HERITAGE Family Study. In SIBPAL linkage analyses, the maximum number of sibpairs available was 344 and 93 for baseline phenotypes and 300 and 72 for exercise training response phenotypes in whites and blacks, respectively. A total of 509 markers with an average spacing of 6.0 Mb were used. The strongest linkage was found for the changes in fasting insulin in response to exercise training with a marker in the leptin gene on 7q31 (empirical multipoint P = 0.0004) in whites. In blacks, the strongest linkage was observed for baseline fasting glucose on 12q13-q14 (empirical multipoint P = 0.0006). These regions harbor several potential candidate genes. The present findings may be important in identifying individuals at increased risk of developing type 2 diabetes and who are most likely to benefit from a physically active lifestyle.

Published
2003

43. Effects of beta2-adrenergic receptor gene variants on adiposity: the HERITAGE Family Study

Author

Jacques Gagnon, Jack H. Wilmore, Christophe Garenc, James S. Skinner, Arthur S. Leon, Ingrid B. Borecki, Yvon C. Chagnon, D. C. Rao, Tuomo Rankinen, Louis Pérusse, and Claude Bouchard

Subjects
Male, medicine.medical_specialty, Linkage disequilibrium, Genotype, Endocrinology, Diabetes and Metabolism, Medicine (miscellaneous), Adipose tissue, Black People, Linkage Disequilibrium, White People, Body Mass Index, Endocrinology, Endurance training, Polymorphism (computer science), Internal medicine, Receptors, Adrenergic, beta, medicine, Humans, Obesity, Allele, Gene, Polymorphism, Genetic, business.industry, Public Health, Environmental and Occupational Health, Skinfold Thickness, Adipose Tissue, Body Composition, Physical Endurance, Female, business, Tomography, X-Ray Computed, Body mass index, Food Science
Abstract

We investigated whether the Arg16Gly and Gln27Glu polymorphisms of the beta2-adrenergic receptor gene were associated with body-fat and fat-distribution phenotypes measured before and in response to a 20-week endurance-training program. BMI, fat mass (FAT), percentage of body fat (%FAT), sum of eight skinfolds (SF8), and abdominal fat areas assessed by computed tomography were measured in adult sedentary white and black participants of the HERITAGE Family Study. Evidence of gene-by-obesity interaction was found in whites for several adiposity phenotypes measured before training. Analyses performed separately in nonobese and obese subjects revealed that obese men carrying the Glu27 allele have lower fat accumulation (BMI, FAT, and %FAT) than noncarriers. Among white obese women, Gly16Gly homozygotes had a lower fat accumulation (BMI, FAT, and SF8) than Arg16Gly and Arg16Arg carriers. In response to endurance training, white women with the Arg16Arg genotype exhibited a greater reduction in BMI, FAT, and %FAT. Results observed in blacks were mostly negative. These results suggest that polymorphisms in the beta2-adrenergic receptor gene influence the amount of body fat in white obese men (Gln27Glu) and women (Arg16Gly), as well as the changes in adiposity in response to endurance training in white women (Arg16Gly).

Published
2003

44. Genomic scan of glucose and insulin metabolism phenotypes: the HERITAGE Family Study

Author

Jack H. Wilmore, Ping An, Yuling Hong, S. John Weisnagel, D. C. Rao, James S. Skinner, Tuomo Rankinen, Yvon C. Chagnon, Claude Bouchard, Arthur S. Leon, Treva Rice, and Richard N. Bergman

Subjects
Adult, Genetic Markers, Male, medicine.medical_specialty, Candidate gene, Adolescent, Genetic Linkage, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Quantitative Trait Loci, Black People, Biology, Quantitative trait locus, Polymorphism, Single Nucleotide, Genetic determinism, White People, Body Mass Index, Endocrinology, Insulin resistance, Genetic linkage, Internal medicine, medicine, Humans, Insulin, Genetic association, Genetics, Glucose tolerance test, medicine.diagnostic_test, Genome, Human, Glucose Tolerance Test, Middle Aged, medicine.disease, Glucose, Phenotype, Female, Lod Score, Microsatellite Repeats
Abstract

Genetic factors play a role in the regulation of glucose metabolism-related traits such as insulin sensitivity (S(I)), insulin secretion, and glucose effectiveness (S(G)). Several genomic scans have been performed to localize genes involved in glucose metabolism-related traits. However, few of these studies have been performed with phenotypes derived from the frequently sampled intravenous glucose tolerance test (IVGTT) using the minimal modeling (MINMOD) approach. Here, we report on such a scan for glucose metabolism-related traits derived from MINMOD analysis of IVGTT data in 322 sibling pairs from 95 sedentary white families and 75 sibling pairs from 49 sedentary black families from the HERITAGE Family Study. In addition to S(I) and S(G), we also considered acute insulin response to a glucose challenge (AIR(Glucose)), which is an index for insulin secretion, and disposition index (DI, product of S(I) and AIR(Glucose)), which is a measure of the activity of pancreatic beta cells corrected for insulin resistance. These traits were adjusted for age, sex, and body mass index (BMI) in each of 8 sex-by-generation-by-race groups, and then standardized residuals were used as the phenotypes in the linkage analyses. Analyses were with the multipoint variance components linkage method, as implemented in the computer program SEGPATH, using 509 markers. Several regions with promising linkages (LOD score >/= 1.75, P

Published
2003

45. Genome-wide linkage scan for exercise stroke volume and cardiac output in the HERITAGE Family Study

Author

Tuomo Rankinen, Treva Rice, Ping An, James S. Skinner, Arthur S. Leon, Jacques Gagnon, Louis Pérusse, Claude Bouchard, Yvon C. Chagnon, Dabeeru C. Rao, and Jack H. Wilmore

Subjects
Adult, Genetic Markers, Male, medicine.medical_specialty, Cardiac output, Aging, Physiology, Genetic Linkage, Physical Exertion, Black People, Submaximal exercise, Biology, White People, Cohort Studies, Genetic linkage, Internal medicine, Genetics, medicine, Humans, Cardiac Output, Exercise, Genome wide linkage, Aged, Linkage (software), Physical Education and Training, Stroke Volume, Stroke volume, Middle Aged, Cardiology, Physical Endurance, Female
Abstract

A genome-wide linkage scan was performed for genes affecting submaximal exercise cardiac output (Q) and stroke volume (SV) in the sedentary state and their responses to a standardized 20-wk endurance training program. A total of 509 polymorphic markers were used, and 328 pairs of siblings from 99 white nuclear families and 102 sibling pairs from 105 black family units were available. Q and SV were measured in relative steady state during exercise at 50 W (Q50 and SV50, respectively). Baseline phenotypes were adjusted for age, sex, and body surface area (BSA), and the training responses (post-training − baseline, Δ) were adjusted for age, sex, baseline BSA, and baseline value of the phenotype. Three analytical strategies were used: a multipoint variance components linkage analysis using all the family data, and regression-based single- and multipoint linkage analyses using pairs of siblings. In whites, baseline SV50 and ΔSV50 showed promising linkages ( P < 0.0023) with markers on chromosomes 14q31.1 and 10p11.2, respectively. Suggestive evidence of linkage (0.01 > P > 0.0023) for ΔSV50 and Δ Q50 was detected on chromosome 2q31.1 and for baseline SV50 and Q50 on chromosome 9q32-q33. In blacks, markers on 18q11.2 showed promising linkages with baseline Q50. Suggestive evidence of linkage was found in three regions for baseline SV50 (1p21.3, 3q13.3, 12q13.2) and one for baseline SV50 and Q50 (10p14). All these chromosomal regions include several potential candidate genes and therefore warrant further studies in the HERITAGE cohort and other studies.

Published
2002

46. Genomewide linkage scan of resting blood pressure: HERITAGE Family Study. Health, Risk Factors, Exercise Training, and Genetics

Author

Treva, Rice, Tuomo, Rankinen, Yvon C, Chagnon, Michael A, Province, Louis, Pérusse, Arthur S, Leon, James S, Skinner, Jack H, Wilmore, Claude, Bouchard, and Dabeeru C, Rao

Subjects
Adult, Family Health, Male, Genetic Linkage, Genome, Human, Black People, Blood Pressure, Coronary Disease, Middle Aged, White People, Risk Factors, Hypertension, Humans, Female, Genetic Predisposition to Disease, Exercise
Abstract

The purpose of this study was to search for genomic regions influencing resting systolic (SBP) and diastolic (DBP) blood pressure (BP) in sedentary families (baseline), and for resting BP responses (changes) resulting from a 20-week exercise training intervention (post-training-baseline) in the Health, Risk Factors, Exercise Training, and Genetics (HERITAGE) Family Study. A genome-wide scan was conducted on 317 black individuals from 114 families and 519 white individuals from 99 families using a multipoint variance-components linkage model and a panel of 509 markers. Promising results were primarily, but not exclusively, found in the black families. Linkage evidence (P0.0023) with baseline BP replicated other studies within a 1-logarithm of odds (LOD) interval on 2p14, 3p26.3, and 12q21.33, and provided new evidence on 3q28, 11q21, and 19p12. Results for several known hypertension genes were less compelling. For response BP, results were not very strong, although markers on 13q11 were mildly suggestive (P0.01). In conclusion, these HERITAGE data, in conjunction with results from previous genomewide scans, provide a basis for planning future investigations. The major areas warranting further study involve fine mapping to narrow down 3 regions on 2q, 3p, and 12q that may contain "novel" hypertension genes, additional typing of some biological candidate genes to determine whether they are the sources of these and other signals, multilocus investigations to understand how and to what extent some of these candidates may interact, and multivariate studies to characterize any pleiotropy.

Published
2002

47. A genomewide linkage scan for abdominal subcutaneous and visceral fat in black and white families: The HERITAGE Family Study

Author

Treva, Rice, Yvon C, Chagnon, Louis, Pérusse, Ingrid B, Borecki, Olavi, Ukkola, Tuomo, Rankinen, Jacques, Gagnon, Arthur S, Leon, James S, Skinner, Jack H, Wilmore, Claude, Bouchard, and D C, Rao

Subjects
Adult, Male, Heterozygote, Genetic Linkage, Black People, White People, Body Mass Index, Gene Frequency, Abdomen, Humans, Exercise, Alleles, Chromosomes, Human, Pair 11, Middle Aged, Viscera, Adipose Tissue, Chromosomes, Human, Pair 2, Body Composition, Physical Endurance, Female, Chromosomes, Human, Pair 4, Lod Score, Tomography, X-Ray Computed, Chromosomes, Human, Pair 7, Polymorphism, Restriction Fragment Length, Microsatellite Repeats
Abstract

Abdominal visceral fat (AVF), abdominal subcutaneous fat (ASF), and abdominal total fat (ATF) were measured using a computed tomography scan, both before (baseline) and after (post) a 20-week endurance exercise training protocol in the HERITAGE Family Study. Each of the baseline and response (post minus baseline) measures was adjusted for several covariates, including total fat mass, and responses to training were further adjusted for baseline levels. Multipoint variance components linkage analysis using a genomewide scan of 344 markers was conducted separately by race using race-specific allele frequencies. Several promising results (P0.0023) were obtained. For baseline AVF, the best evidence was on 2q22.1 and 2q33.2-q36.3 (including the IRS1 locus) in whites, with suggestive findings on 7q22.2-q31.3 (including the LEP locus) in blacks. Although several regions were indicated for baseline ASF, only 4q31.22-q32.2 and 11p15.4-p11.2 replicated the results of another study. For responses to training, promising results were limited to ASF and ATF primarily on 7q36.2 (including NOS3) in blacks, with suggestive regions (P0.01) on 1q21.2-q24.1 (S100A, ATP1A2, and ATP1B1), 10q25.2 (ADRA2A), and 11p15.5 (IGF2). In summary, the 4q and 11p regions have now been implicated in two independent studies for ASF; further research is warranted to identify the genes and mutations in these regions that are responsible for fat accumulation in the abdominal depot. Additional work in an independent sample is needed to verify the linkages for baseline AVF as well as the response measures.

Published
2002

48. The alpha 2-adrenergic receptor gene and body fat content and distribution: the HERITAGE Family Study

Author

James S. Skinner, Yvon C. Chagnon, Christophe Garenc, Jacques Gagnon, D. C. Rao, Ingrid B. Borecki, Louis Pérusse, Jack H. Wilmore, Tuomo Rankinen, Claude Bouchard, and Arthur S. Leon

Subjects
Adult, Male, medicine.medical_specialty, Canada, Adrenergic receptor, Adipose tissue, Adrenergic, Black People, Biology, White People, Body Mass Index, Fats, Gene Frequency, Receptors, Adrenergic, alpha-2, Internal medicine, Genetics, medicine, Humans, Genetic Predisposition to Disease, Allele, Receptor, Molecular Biology, Allele frequency, Genetics (clinical), chemistry.chemical_classification, Polymorphism, Genetic, Fatty acid, United States, Endocrinology, Phenotype, chemistry, Body Composition, Molecular Medicine, Female, Body mass index, Research Article
Abstract

BACKGROUND: Among adrenergic receptor subtypes that regulate lipid mobilization, the alpha2-adrenergic receptor is involved in the inhibition of fatty acid mobilization from adipose tissue. A C-1291G polymorphism is located in the alpha2-adrenergic receptor gene (ADRA2A) but no association with body fat accumulation has been reported yet. MATERIALS AND METHODS: Body mass index (BMI), fat mass (FAT), percentage body fat (%FAT), trunk-to-extremity skinfold ratio (TER), sum of eight skinfolds (SF8), and abdominal subcutaneous (ASF), visceral (AVF), and total (ATF) fat areas assessed by CT scan have been measured in adult sedentary white (n = 503) and black (n = 276) subjects participating in the HERITAGE Family Study. Association between the C-1291G polymorphism and each phenotype was tested separately in men and women of each race using ANCOVA with the effects of age as covariate in addition to the effects of BMI for TER and of FAT for AVF, ASF, and ATF. RESULTS: The allele frequencies of the ADRA2A C-1291G polymorphism differed between races. No association was observed in white subjects, except for a moderate effect of the polymorphism accounting for less than 1% of the variance in AVF and ATF in women. In black subjects, however, the G-1291 allele was found to be associated with an increase of TER in men (3.8% of variance accounted for by the polymorphism), while in black women it was associated with a decrease in TER (2.9%) and in AVF (2.5%). CONCLUSION: These results suggest a role for the ADRA2A gene in determining the propensity to store fat in the abdominal area, independently of total body fatness.

Published
2002

49. Polymorphisms in the leptin receptor gene, body composition and fat distribution in overweight and obese women

Author

Yvon C. Chagnon, Tuomo Rankinen, Robert V. Considine, Ilse Mertens, Monique Chagnon, L. Van Gaal, M. Wauters, and Claude Bouchard

Subjects
Adult, Leptin, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, Medicine (miscellaneous), Receptors, Cell Surface, Overweight, Genetic determinism, White People, Body Mass Index, Classification of obesity, Internal medicine, medicine, Humans, Obesity, Alleles, Nutrition and Dietetics, Leptin receptor, Polymorphism, Genetic, business.industry, digestive, oral, and skin physiology, nutritional and metabolic diseases, Anthropometry, Middle Aged, medicine.disease, Leptin Receptor Gene, Endocrinology, Phenotype, Adipose Tissue, Body Composition, Receptors, Leptin, Female, medicine.symptom, Menopause, business, Carrier Proteins, hormones, hormone substitutes, and hormone antagonists
Abstract

Leptin is an adipocyte-secreted hormone involved in body weight regulation, acting through the leptin receptor, localised centrally in the hypothalamus as well as peripherally, amongst others on adipose tissue. The aim of this study was to evaluate whether polymorphisms in the leptin receptor (LEPR) gene were related to obesity and body fat distribution phenotypes, such as waist and hip circumferences and the amount of visceral and subcutaneous fat.Three known LEPR polymorphisms, Lys109Arg, Gln223Arg and Lys656Asn, were typed on genomic DNA of 280 overweight and obese women (body mass index (BMI)25), aged 18-60 y. General linear model (GLM) analyses were performed in 198 pre- and 82 postmenopausal women, adjusting the data for age and menopausal state, plus fat mass for the fat distribution phenotypes.No associations were found between the LEPR polymorphisms and BMI or fat mass. In postmenopausal women, carriers of the Asn656 allele had increased hip circumference (P=0.03), total abdominal fat (P=0.03) and subcutaneous fat (P=0.04) measured by CT scan. Total abdominal fat was also higher in Gln223Gln homozygotes (P=0.04). Also in postmenopausal women, leptin levels were higher in Lys109Lys homozygotes (P=0.02).In conclusion, polymorphisms in the leptin receptor gene are associated with levels of abdominal fat in postmenopausal overweight women. Since body fat distribution variables were adjusted for fat mass, these results suggest that DNA sequence variations in the leptin receptor gene play a role in fat topography and may be involved in the predisposition to abdominal obesity.

Published
2000

50. Linkage and association studies of the lipoprotein lipase gene with postheparin plasma lipase activities, body fat, and plasma lipid and lipoprotein concentrations: the HERITAGE Family Study

Author

James S. Skinner, Arthur S. Leon, Claude Bouchard, Jean Bergeron, Jacques Gagnon, Jean-Pierre Després, Michael A. Province, Louis Pérusse, Dabeeru C. Rao, Yvon C. Chagnon, Jack H. Wilmore, and Christophe Garenc

Subjects
Adult, Male, medicine.medical_specialty, Very low-density lipoprotein, Apolipoprotein B, Genetic Linkage, Endocrinology, Diabetes and Metabolism, Lipoproteins, Blood lipids, Biology, chemistry.chemical_compound, Endocrinology, Gene Frequency, Internal medicine, medicine, Humans, Obesity, Alleles, Triglycerides, Lipoprotein lipase, Polymorphism, Genetic, Triglyceride, Cholesterol, Heparin, Osmolar Concentration, nutritional and metabolic diseases, Lipase, Middle Aged, Lipids, Lipoprotein Lipase, chemistry, Adipose Tissue, biology.protein, lipids (amino acids, peptides, and proteins), Female, Hepatic lipase, Lipoprotein
Abstract

Lipoprotein lipase (LPL) is responsible for the hydrolysis of triglyceride (TG)-rich lipoproteins. The aims of the present study were (1) to test for potential linkages (sib-pair method) between postheparin plasma lipase (lipoprotein and hepatic lipase) activities, body fatness, plasma lipid concentrations, and LPL polymorphisms (Ser447Ter and a tetranucleotide repeat) and microsatellite markers flanking the LPL locus (D8S261 and D8S258); and (2) to investigate associations between the LPL Ser447Ter (S447X) polymorphism and these phenotypes. Data on 190 parents and 312 adult offspring from 99 Caucasian families participating in the HERITAGE Family Study were available for this study. Data were adjusted for the effects of age within sex, and lipases, lipid variables, and abdominal visceral fat were further adjusted for fat mass. A suggestive linkage was observed only between the S447X polymorphism and very-low-density (VLDL)-apolipoprotein B (apo B) (332 sib-pairs, P = .013). The S447X polymorphism was not associated with body fat phenotypes or postheparin plasma LPL (PH-LPL) activity (men, P = .19; women, P = .47). In contrast, the X447 allele carriers had lower plasma TG (men and women, P = .01), VLDL-TG (men and women, P = .01), and VLDL-apo B (men and women, P = .009). The relationships between the X447 allele and plasma TG, VLDL-TG, and VLDL-apo B in both genders were observed in obese (body mass index [BMI] ⩾ 30 kg/m 2 ) but not in normal-weight (BMI 2 ) subjects. Thus, the S447X polymorphism of the LPL gene is not associated with body fatness and postheparin plasma lipase activities. However, the obese carriers of the X447 allele have plasma TG, VLDL-TG, and plasma cholesterol/high-density lipoprotein cholesterol (HDL-C) levels equivalent to those of normal-weight sedentary adults.

Published
2000

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