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A Whole-Genome Scan for 24-Hour Respiration Rate: A Major Locus at 10q26 Influences Respiration During Sleep.

机译:全基因组扫描24小时呼吸速率:10q26时的主要基因座会影响睡眠期间的呼吸。

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摘要

Identification of genes causing variation in daytime and nighttime respiration rates could advance our understanding of the basic molecular processes of human respiratory rhythmogenesis. This could also serve an important clinical purpose, because dysfunction of such processes has been identified as critically important in sleep disorders. We performed a sib-pair-based linkage analysis on ambulatory respiration rate, using the data from 270 sibling pairs who were genotyped at 374 markers on the autosomes, with an average distance of 9.65 cM. Uni- and multivariate variance-components-based multipoint linkage analyses were performed for respiration rate during three daytime periods (morning, afternoon, and evening) and during nighttime sleep. Evidence of linkage was found at chromosomal locations 3q27, 7p22, 10q26, and 22q12. The strongest evidence of linkage was found for respiration rate during sleep, with LOD scores of 2.36 at 3q27, 3.86 at 10q26, and 1.59 at 22q12. In a simultaneous analysis of these three loci, >50% of the variance in sleep respiration rate could be attributed to a quantitative-trait loci near marker D10S1248 at 10q. Genes in this area (GFRA1, ADORA2L, FGR2, EMX2, and HMX2) can be considered promising positional candidates for genetic association studies of respiratory control during sleep.
机译:鉴定引起白天和晚上呼吸频率变化的基因可以促进我们对人类呼吸节律发生的基本分子过程的了解。这也可以用于重要的临床目的,因为这种过程的功能障碍已被确定对睡眠障碍至关重要。我们使用来自270对同卵双胞胎的数据对同伴配对进行了基于同胞对的连锁分析,这些同胞对在常染色体上以374个标记进行基因分型,平均距离为9.65 cM。在三个白天时段(早晨,下午和晚上)和夜间睡眠期间,对呼吸速率进行了基于单变量和多变量方差成分的多点链接分析。在染色体位置3q27、7p22、10q26和22q12发现了连锁的证据。在睡眠期间发现呼吸速率有最强的联系证据,LOD得分在27年3季度为2.36,26年10季度为3.86,22年12月为1.59。在对这三个基因座的同时分析中,睡眠呼吸率变异的> 50%可以归因于10q处标记D10S1248附近的定量特征基因座。该区域的基因(GFRA1,ADORA2L,FGR2,EMX2和HMX2)被认为是有希望的位置候选物,可用于睡眠期间呼吸控制的遗传关联研究。

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