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Plasma lipidome is independently associated with variability in metabolic syndrome in Mexican American families
Authors:Hemant Kulkarni  Peter J Meikle  Manju Mamtani  Jacquelyn M Weir  Marcio Almeida  Vincent Diego  Juan Manuel Peralta  Christopher K Barlow  Claire Bellis  Thomas D Dyer  Laura Almasy  Michael C Mahaney  Anthony G Comuzzie  Harald H H G?ring  Joanne E Curran  John Blangero
Institution:*Department of Genetics, Texas Biomedical Research Institute, San Antonio, TX 78227;Baker IDI Heart and Diabetes Institute, Melbourne, Victoria, 3004, Australia
Abstract:Plasma lipidome is now increasingly recognized as a potentially important marker of chronic diseases, but the exact extent of its contribution to the interindividual phenotypic variability in family studies is unknown. Here, we used the rich data from the ongoing San Antonio Family Heart Study (SAFHS) and developed a novel statistical approach to quantify the independent and additive value of the plasma lipidome in explaining metabolic syndrome (MS) variability in Mexican American families recruited in the SAFHS. Our analytical approach included two preprocessing steps: principal components analysis of the high-resolution plasma lipidomics data and construction of a subject-subject lipidomic similarity matrix. We then used the Sequential Oligogenic Linkage Analysis Routines software to model the complex family relationships, lipidomic similarities, and other important covariates in a variance components framework. Our results suggested that even after accounting for the shared genetic influences, indicators of lipemic status (total serum cholesterol, TGs, and HDL cholesterol), and obesity, the plasma lipidome independently explained 22% of variability in the homeostatic model of assessment-insulin resistance trait and 16% to 22% variability in glucose, insulin, and waist circumference. Our results demonstrate that plasma lipidomic studies can additively contribute to an understanding of the interindividual variability in MS.
Keywords:lipidomics  obesity  lipids  genetics  insulin resistance  plasma lipidomics  variance components
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