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Genome-wide linkage analysis using cross-sectional and longitudinal traits for body mass index in a subsample of the Framingham Heart Study

机译:在弗雷明汉心脏研究的子样本中,使用横截面和纵向特征进行体重指数的全基因组连锁分析

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To evaluate linkage evidence for body mass index (BMI) using both cross-sectional and longitudinal data, we performed genome-wide multipoint linkage analyses on subjects who had complete data at four selected time points (initial, 8th, 12th, and 16th year following the initial visit) from the Framingham Heart Study. The cross-sectional measures included BMI at each of the four selected time points and the longitudinal measure was the within-subject mean of BMI at the above four time points.Using the variance components method, we consistently observed the maximum LOD score out of the genome scan using BMI at each time point and the mean of BMI between 049xd2 and GATA71H05 on chromosome 16. The highest LOD score (3.0) was at time point 1, while the lowest (1.9) was at time point 4. We also observed other suggestive linkages on chromosome 6, 10, and 18 at time point 1 only.The longitudinal measure we studied (mean of BMI) did not provide greater power to identify a positive linkage than some of the cross-sectional measures (e.g., time point 1). The changing of linkage evidence over time provided some insights on the variation of genetic effect on BMI with aging. There may be a QTL on chromosome 16 that contributes to BMI and this locus, and maybe others, is more likely to affect BMI during early adulthood.
机译:为了使用横截面和纵向数据评估体重指数(BMI)的连锁证据,我们对在四个选定时间点(初始,8 th ,第12 和第16 Framingham心脏研究。横截面测量包括四个选定时间点的每个BMI,而纵向测量是上述四个时间点的BMI的受试者内平均值。使用方差分量法,我们始终观察到了最大LOD得分。使用每个时间点的BMI进行基因组扫描,以及16号染色体上049xd2和GATA71H05之间的BMI平均值。最高LOD得分(3.0)在时间点1,而最低(1.9)在时间点4。仅在时间点1处暗示着染色体6、10和18上的暗示性连锁。我们研究的纵向量度(BMI的平均值)没有提供比某些横截面量度(例如时间点1)更大的识别正连锁的能力。 )。随着时间的推移,连锁证据的变化为随着年龄的增长对BMI遗传效应的变化提供了一些见识。在16号染色体上可能存在一个QTL导致BMI,这个位点,可能还有其他位点,在成年早期更可能影响BMI。

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