Literature DB >> 8933005

Familial correlations in the Québec family study: cross-trait familial resemblance for body fat with plasma glucose and insulin.

T Rice1, A Nadeau, L Pérusse, C Bouchard, D C Rao.   

Abstract

This study represents one component in our investigation of the familial factors underlying the insulin resistance (or metabolic) syndrome involving obesity, hyperinsulinaemia, glucose intolerance, dyslipidaemia, and hypertension. Here we examine the cross-trait familial resemblance between four measures of body size (two assessing total fat [body mass index and sum of six skinfolds] and two assessing fat patterning [ratio of trunk skinfold sum to extremity skinfold sum, adjusted and unadjusted for total subcutaneous fat]) with fasting plasma levels of glucose, insulin, and the ratio of insulin to glucose (IGR) in non-diabetic families participating in phase 1 of the Québec Family Study. A bivariate familial correlation model assessed both intraindividual (e.g. father's body size with father's insulin) and interindividual (e.g. father's body size with son's insulin) cross-trait associations. Intraindividual correlations suggested a greater degree of cross-trait associations for body fat (rather than fat distribution) measures with insulin and the IGR (rather than with glucose) levels. While the intraindividual correlations were significant for most cross-trait comparisons, only the sum of six skinfolds evidenced any familial association (i.e. interindividual resemblance) with insulin and the IGR. Specifically, cross-trait parent-offspring (but not sibling or spouse) correlations were significant, with a bivariate familiality estimate (i.e. polygenic and/or common familial environment) of about 8%. While the lack of sibling correlations does not suggest a simple familial hypothesis, a more complex genetic effect underlying the common covariation between total body fat with insulin and IGR cannot be ruled out.

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Year:  1996        PMID: 8933005     DOI: 10.1007/s001250050583

Source DB:  PubMed          Journal:  Diabetologia        ISSN: 0012-186X            Impact factor:   10.122


  8 in total

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2.  Human resistin gene polymorphism is associated with visceral obesity and fasting and oral glucose stimulated C-peptide in the Québec Family Study.

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Review 4.  Are there genetic paths common to obesity, cardiovascular disease outcomes, and cardiovascular risk factors?

Authors:  Tuomo Rankinen; Mark A Sarzynski; Sujoy Ghosh; Claude Bouchard
Journal:  Circ Res       Date:  2015-02-27       Impact factor: 17.367

5.  Sedentary behaviour, visceral fat accumulation and cardiometabolic risk in adults: a 6-year longitudinal study from the Quebec Family Study.

Authors:  Travis J Saunders; Mark S Tremblay; Jean-Pierre Després; Claude Bouchard; Angelo Tremblay; Jean-Philippe Chaput
Journal:  PLoS One       Date:  2013-01-09       Impact factor: 3.240

6.  ZFP36: a promising candidate gene for obesity-related metabolic complications identified by converging genomics.

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7.  Estimating genetic effect sizes under joint disease-endophenotype models in presence of gene-environment interactions.

Authors:  Alexandre Bureau; Jordie Croteau; Christian Couture; Marie-Claude Vohl; Claude Bouchard; Louis Pérusse
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Review 8.  Findings from the Quebec Family Study on the Etiology of Obesity: Genetics and Environmental Highlights.

Authors:  Jean-Philippe Chaput; Louis Pérusse; Jean-Pierre Després; Angelo Tremblay; Claude Bouchard
Journal:  Curr Obes Rep       Date:  2014-01-04
  8 in total

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