首页> 外文期刊>European journal of human genetics: EJHG >Multiple QTL influence the serum Lp(a) concentration: a genome-wide linkage screen in the PROCARDIS study.
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Multiple QTL influence the serum Lp(a) concentration: a genome-wide linkage screen in the PROCARDIS study.

机译:多个QTL影响血清Lp(a)浓度:PROCARDIS研究中的全基因组连锁筛选。

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摘要

The serum concentration of lipoprotein Lp (a) is known to be highly heritable and associated with cardiovascular risk. A genome-wide variance component linkage analysis was performed to localise quantitative trait loci (QTLs) influencing Lp(a) levels in a large cohort collected in the PROCARDIS coronary heart disease study. Highly significant linkage was detected at the previously described LP(a) locus on chromosome 6q27 (LOD 108). Taking into account the effect of the locus detected on chromosome 6, a highly significant LOD score was detected on chromosome 13q22-31 (LOD 7.0). Another significant region of linkage was observed on chromosomes 11p14-15 (LOD 3.5).The significant peak at 13q22-31 shows an essential overlap with a locus modulating cholesterol in familial hypercholesterolemia. If the gene underlying these loci is the same, it will be a promising candidate target for manipulating LDL-cholesterol and Lp(a). We also detected linkage at a previously identified locus influencing Lp(a) on chromosome 1q23 (LOD 1.5). Our findings provide new and confirmatory information about genomic regions involved in the quantitative variation of Lp(a) and serve as a basis for further studies of candidate genes in these regions.
机译:脂蛋白Lp(a)的血清浓度已知是高度可遗传的,并且与心血管疾病风险有关。在PROCARDIS冠心病研究中收集的一个大型队列中,进行了全基因组范围的变异成分连锁分析,以定位影响Lp(a)水平的定量性状位点(QTL)。在先前描述的染色体6q27上的LP(a)位点检测到高度重要的连锁(LOD 108)。考虑到检测到的基因座对6号染色体的影响,在13q22-31号染色体上检测到了非常显着的LOD分数(LOD 7.0)。在11p14-15号染色体上观察到另一个重要的连锁区域(LOD 3.5).13q22-31处的显着峰表明与家族性高胆固醇血症中调节胆固醇的基因座基本重叠。如果这些基因座的基因相同,那么它将成为操纵LDL-胆固醇和Lp(a)的有希望的候选靶标。我们还检测到在先前确定的影响1p23染色体Lp(a)的基因座上的连锁(LOD 1.5)。我们的发现为涉及Lp(a)定量变异的基因组区域提供了新的和确证的信息,并为进一步研究这些区域中的候选基因奠定了基础。

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