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Locus for quantitative HDL-cholesterol on chromosome 10q in Finnish families with dyslipidemia
Authors:Lilja Heidi E  Suviolahti Elina  Soro-Paavonen Aino  Hiekkalinna Tero  Day Aaron  Lange Kenneth  Sobel Eric  Taskinen Marja-Riitta  Peltonen Leena  Perola Markus  Pajukanta Päivi
Institution:Department of Molecular Medicine, National Public Health Institute, Helsinki, Finland.
Abstract:Decreased HDL-cholesterol (HDL-C) and familial combined hyperlipidemia (FCHL) are the two most common familial dyslipidemias predisposing to premature coronary heart disease (CHD). These dyslipidemias share many phenotypic features, suggesting a partially overlapping molecular pathogenesis. This was supported by our previous pooled data analysis of the genome scans for low HDL-C and FCHL, which identified three shared chromosomal regions for a qualitative HDL-C trait on 8q23.1, 16q23.3, and 20q13.32. This study further investigates these regions as well as two other loci we identified earlier for premature CHD on 2q31 and Xq24 and a locus for high serum triglycerides (TGs) on 10q11. We analyzed 67 microsatellite markers in an extended study sample of 1,109 individuals from 92 low HDL-C or FCHL families using both qualitative and quantitative lipid phenotypes. These analyses provided evidence for linkage (a logarithm of odds score of 3.2) on 10q11 using a quantitative HDL-C trait. Importantly, this region, previously linked to TGs, body mass index, and obesity, provided evidence for association for quantitative TGs (P = 0.0006) and for a combined trait of HDL-C and TGs (P = 0.008) with marker D10S546. Suggestive evidence for linkage also emerged for HDL-C on 2q31 and for TGs on 20q13.32. Finnish families ascertained for dyslipidemias thus suggest that 10q11, 2q31, and 20q13.32 harbor loci for HDL-C and TGs.
Keywords:low high density lipoprotein-cholesterol  familial combined hyperlipidemia  coronary heart disease  atherosclerosis  quantitative traits  variance component analyses  quantitative trait locus  triglycerides  type 2 diabetes  metabolic syndrome
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