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首页> 外文期刊>European journal of epidemiology >Heritabilities, apolipoprotein E, and effects of inbreeding on plasma lipids in a genetically isolated population: the Erasmus Rucphen Family Study.
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Heritabilities, apolipoprotein E, and effects of inbreeding on plasma lipids in a genetically isolated population: the Erasmus Rucphen Family Study.

机译:遗传力,载脂蛋白E和近交对遗传分离人群血浆脂质的影响:伊拉斯ras(Erasmus Rucphen)家庭研究。

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Despite considerable progress in unravelling the genetic basis of dyslipidemias, most findings are based on families with extreme phenotypes. We studied lipid levels in an extended pedigree ascertained irrespective of phenotype from the population of a recent genetic isolate in the Netherlands. Heritabilities of plasma lipid measures were examined; this analysis also included estimates of the proportion of variance attributable to ApoE genotype. The association between inbreeding and lipids was also considered, as a substantial fraction of the population had known inbreeding. A total of 868 individuals from this pedigree, containing more than 60,000 people over 15 generations, were investigated in this study. Laboratory analysis of these subjects included the determination of fasting plasma lipids. ApoE epsilon2/3/4 status was ascertained using TaqMan assays. Heritabilities for plasma lipids were estimated with adjustments for multiple covariates using SOLAR. Heritabilities for total cholesterol (TC), high-density lipoprotein cholesterol (HDL), low-density lipoprotein cholesterol (LDL), triglycerides (TG), TC/HDL ratio, and TG/HDL ratio were found to be 0.35, 0.56, 0.30, 0.24, 0.49, and 0.39, respectively. The addition of ApoE genotype in the model significantly decreased these estimates (Deltah(2) = -0.030, -0.004, -0.054, and -0.006 for TC, HDL, LDL, and TG). In a further analysis, TC and LDL were positively associated with the extent of inbreeding (p (trend) = 0.02 and p (trend) = 0.05, respectively). These data provide estimates of lipid heritability unbiased due to selection and suggest that this population represents a good opportunity to localize novel genes influencing plasma lipid levels.
机译:尽管在阐明血脂异常的遗传学基础上取得了重大进展,但大多数发现是基于具有极端表型的家庭。我们研究了确定的血统水平中的血脂水平,而与来自荷兰最近的遗传隔离群的表型无关。检查血浆脂质测量的遗传力;该分析还包括可归因于ApoE基因型的变异比例的估计。还考虑了近亲繁殖与脂质之间的联系,因为很大一部分人口已知近亲繁殖。这项研究共调查了来自该谱系的868个人,其中包括超过15个世代的60,000多人。这些受试者的实验室分析包括测定空腹血浆脂质。使用TaqMan分析确定ApoE epsilon2 / 3/4的状态。通过使用SOLAR调整多个协变量来估计血浆脂质的遗传力。发现总胆固醇(TC),高密度脂蛋白胆固醇(HDL),低密度脂蛋白胆固醇(LDL),甘油三酸酯(TG),TC / HDL比和TG / HDL比的遗传力分别为0.35、0.56、0.30 ,0.24、0.49和0.39。在模型中添加ApoE基因型会大大降低这些估计值(对于TC,HDL,LDL和TG,Deltah(2)= -0.030,-0.004,-0.054和-0.006)。在进一步的分析中,TC和LDL与近交程度呈正相关(p(趋势)= 0.02和p(趋势)= 0.05)。这些数据提供了因选择而无偏见的脂质遗传力估计值,并表明该群体代表了定位影响血浆脂质水平的新基因的良好机会。

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