2010
DOI: 10.1194/jlr.m003897
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Association analysis of 33 lipoprotein candidate genes in multi-generational families of African ancestry

Abstract: Lipoprotein abnormalities, characterized by elevated levels of LDL cholesterol (LDL-C) and triglycerides (TRIG) and low levels of HDL cholesterol (HDL-C), have a central role in the development of atherosclerotic coronary heart disease (CHD). A recent meta-analysis, including 3,000 individuals with CHD-related deaths, showed that HDL-C and LDL-C are independently associated with CHD risk ( 1 ). There is also considerable evidence that high levels of TRIG are an additional, independent risk factor for CHD ( 2, … Show more

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Cited by 16 publications
(13 citation statements)
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“…LDL-C, HDL-C, and TGs all show similar results, with strong shared genetic correlations ( g ranging from 0.82 for TGs to 0.87 for HDL-C), weak and nonsignifi cant environmental correlations ( e ranging from 0.12 for HDL-C to 0.18 for TGs), and moderate phenotypic correlations ranging from 0.42 (TGs) to 0.55 (HDL-C) across time. Heritability for plasma lipids in our African American families (e.g., 0.17 for LDL-C to 0.62 for TGs and HDL-C) is also similar to the limited previous reports in African American or Caribbean populations (e.g., 0.28 in TGs to 0.55 for HDL-C) ( 6,8,44 ), none of which were recruited prior to the obesity epidemic. Some differences occur by lipid trait, for example TGs, where African American heritability was strong (0.62) in our study, but weak to moderate (0.28-0.37) and sometimes not signifi cant in others ( 6,8,44 ).…”
Section: Secular (Time) Trends In Heritability and Shared Genetic Effsupporting
confidence: 68%
See 1 more Smart Citation
“…LDL-C, HDL-C, and TGs all show similar results, with strong shared genetic correlations ( g ranging from 0.82 for TGs to 0.87 for HDL-C), weak and nonsignifi cant environmental correlations ( e ranging from 0.12 for HDL-C to 0.18 for TGs), and moderate phenotypic correlations ranging from 0.42 (TGs) to 0.55 (HDL-C) across time. Heritability for plasma lipids in our African American families (e.g., 0.17 for LDL-C to 0.62 for TGs and HDL-C) is also similar to the limited previous reports in African American or Caribbean populations (e.g., 0.28 in TGs to 0.55 for HDL-C) ( 6,8,44 ), none of which were recruited prior to the obesity epidemic. Some differences occur by lipid trait, for example TGs, where African American heritability was strong (0.62) in our study, but weak to moderate (0.28-0.37) and sometimes not signifi cant in others ( 6,8,44 ).…”
Section: Secular (Time) Trends In Heritability and Shared Genetic Effsupporting
confidence: 68%
“…Heritability for plasma lipids in our African American families (e.g., 0.17 for LDL-C to 0.62 for TGs and HDL-C) is also similar to the limited previous reports in African American or Caribbean populations (e.g., 0.28 in TGs to 0.55 for HDL-C) ( 6,8,44 ), none of which were recruited prior to the obesity epidemic. Some differences occur by lipid trait, for example TGs, where African American heritability was strong (0.62) in our study, but weak to moderate (0.28-0.37) and sometimes not signifi cant in others ( 6,8,44 ). The current study's estimates for African American families at LRC are lower for TC (0.22) and LDL-C (0.17) than those reported in an early analysis of a subset of this same cohort (0.39 and 0.54, respectively) ( 7 ), possibly due to differences in analysis techniques.…”
Section: Secular (Time) Trends In Heritability and Shared Genetic Effsupporting
confidence: 68%
“…13 LDLR rs6511720 is one of the most important LDLcholesterol-associated variants in genome-wide studies of lipid traits. [25][26][27][28][29][30][31] Importantly, a relationship between AAA and LDL-cholesterol levels is not presently established. The most complete meta-analysis of the relationship was inconclusive, and individual reports are inconsistent.…”
Section: Discussionmentioning
confidence: 99%
“…Sex-specific heritabilities of lipid traits have been previously reported [23,24]. Despite considerable advances in the identification of genetic variants influencing plasma lipid levels, few studies have examined the role of sex as a potential modifier of the effects of genetic variation on lipids.…”
Section: Introductionmentioning
confidence: 99%