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Linkage and association with pulmonary function measures on chromosome 6q27 in the Framingham Heart Study.

机译:在Framingham心脏研究中,染色体6q27上的肺功能测量指标具有关联性和关联性。

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Spirometric measures of pulmonary function have been shown to be highly heritable and evidence for major genes influencing forced expiratory volume in 1 s (FEV1) and forced vital capacity (FVC) have been reported. A genome scan of pulmonary traits in the Framingham Heart Study identified a region on chromosome 6qter with evidence for linkage to FEV1 and the FEV1/FVC ratio. For this study, additional markers were genotyped in the region to refine the location of linkage and test for association. Variance component linkage analysis was performed using GENEHUNTER, and family-based association tests were performed using FBAT. The chromosome 6 telomeric region provided significant evidence of linkage with the additional markers, resulting in a maximum multipoint LOD score of 5.0 for FEV1 at 184.5 cM. LOD scores for FVC and the FEV1/FVC ratio were also above 1.0 in this region. Evidence for association with FEV1 and FVC was observed with D6S281 at 190 cM. The strongest effect was seen with the 224 allele, which was associated with higher levels of FEV1 and FVC in allele carriers compared with those carrying other alleles. This study supports the presence of a gene influencing pulmonary function on the q-terminus of chromosome 6 in the region of 184 cM (D6S503) to 190 cM (D6S281).
机译:肺功能的肺活量测定法已被证明是高度可遗传的,并且已报道了影响1s内呼气量(FEV1)和强制肺活量(FVC)的主要基因的证据。在《弗雷明汉心脏研究》中对肺部性状进行基因组扫描,确定了6qter染色体上的一个区域,该区域具有与FEV1和FEV1 / FVC比值相关的证据。在本研究中,对该区域的其他标记进行了基因分型,以完善连锁位置并测试关联性。使用GENEHUNTER进行方差组件链接分析,并使用FBAT进行基于家庭的关联测试。 6号染色体的端粒区域提供了与其他标记连锁的显着证据,导致FEV1在184.5 cM时的最大多点LOD得分为5.0。在该区域,FVC的LOD分数和FEV1 / FVC比率也高于1.0。 D6S281在190 cM时观察到与FEV1和FVC相关的证据。 224个等位基因观察到最强的作用,与携带其他等位基因的那些等位基因携带者相比,FEV1和FVC的水平更高。这项研究支持在184 cM(D6S503)至190 cM(D6S281)区域的第6号染色体q端存在影响肺功能的基因。

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