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Heritability and linkage study on heart rates in a Mongolian population

机译:蒙古族人群心率的遗传性和关联性研究

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摘要

Elevated heart rate has been proposed as an independent risk factor for cardiovascular diseases, but their interrelationships are not well understood. In this study, we performed a genome-wide linkage scan in 1,026 individuals (mean age 30.6 years, 54.5% women) from 73 extended families of Mongolia and determined quantitative trait loci that influence heart rate. The DNA samples were genotyped using deCODE 1,039 microsatellite markers for 3 cM density genome-wide linkage scan. Correlation analysis was carried out to evaluate the correlation of the covariates and the heart rate. T-tests of the heart rate were also performed on sex, smoking and alcohol intake. Consequently, this model was used in a nonparametric genome-wide linkage analysis using variance component model to create a multipoint logarithm of odds (LOD) score and a corresponding P value. In the adjusted model, the heritability of heart rate was estimated as 0.32 (P < .0001) and a maximum multipoint LOD score of 2.03 was observed in 77 cM region at chromosome 18. The second largest LOD score of 1.52 was seen on chromosome 5 at 216 cM. Genes located on the specified locations in chromosomes 5 and 18 may be involved in the regulation of heart rate.
机译:有人提出过高的心率是心血管疾病的独立危险因素,但人们对它们之间的相互关系尚不甚了解。在这项研究中,我们对来自73个蒙古大家庭的1,026名个体(平均年龄30.6岁,女性54.5%)进行了全基因组连锁扫描,并确定了影响心率的定量特征位点。使用deCODE 1,039微卫星标记对DNA样品进行基因分型,以进行3 cM密度的全基因组连锁扫描。进行相关分析以评估协变量和心率的相关性。还对性别,吸烟和饮酒进行了心率的T检验。因此,该模型被用于使用方差分量模型的非参数全基因组连锁分析中,以创建赔率(LOD)分数和相应的P值的多点对数。在调整后的模型中,心率的遗传力估计为0.32(P <.0001),在18号染色体的77 cM区域观察到最大多点LOD得分为2.03。在5号染色体上看到的第二大LOD得分为1.52。在216 cM。位于5号和18号染色体指定位置的基因可能参与心率的调节。

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