Genome-Wide Association Study for Age-Related Hearing Loss (AHL) in the Mouse: A Meta-Analysis

被引:0
|
作者
Jeffrey Ohmen
Eun Yong Kang
Xin Li
Jong Wha Joo
Farhad Hormozdiari
Qing Yin Zheng
Richard C. Davis
Aldons J. Lusis
Eleazar Eskin
Rick A. Friedman
机构
[1] House Research Institute,Department of Cell and Molecular Biology and Genetics
[2] University of California,Department of Computer Science
[3] Los Angeles,Interdepartmental Program in Bioinformatics
[4] University of California,Department of Otolaryngology
[5] Los Angeles,Department of Medicine
[6] Case Western Reserve University,Department of Human Genetics
[7] University of California,Department of Otolaryngology, Zilkha Neurogenetic Institute, Keck School of Medicine
[8] Los Angeles,undefined
[9] University of California,undefined
[10] Los Angeles,undefined
[11] University of Southern California,undefined
来源
Journal of the Association for Research in Otolaryngology | 2014年 / 15卷
关键词
genome-wide association study; age-related hearing loss (ARL); meta-analysis; random-effects model; mouse models;
D O I
暂无
中图分类号
学科分类号
摘要
Age-related hearing loss (AHL) is characterized by a symmetric sensorineural hearing loss primarily in high frequencies and individuals have different levels of susceptibility to AHL. Heritability studies have shown that the sources of this variance are both genetic and environmental, with approximately half of the variance attributable to hereditary factors as reported by Huag and Tang (Eur Arch Otorhinolaryngol 267(8):1179–1191, 2010). Only a limited number of large-scale association studies for AHL have been undertaken in humans, to date. An alternate and complementary approach to these human studies is through the use of mouse models. Advantages of mouse models include that the environment can be more carefully controlled, measurements can be replicated in genetically identical animals, and the proportion of the variability explained by genetic variation is increased. Complex traits in mouse strains have been shown to have higher heritability and genetic loci often have stronger effects on the trait compared to humans. Motivated by these advantages, we have performed the first genome-wide association study of its kind in the mouse by combining several data sets in a meta-analysis to identify loci associated with age-related hearing loss. We identified five genome-wide significant loci (<10−6). One of these loci confirmed a previously identified locus (ahl8) on distal chromosome 11 and greatly narrowed the candidate region. Specifically, the most significant associated SNP is located 450 kb upstream of Fscn2. These data confirm the utility of this approach and provide new high-resolution mapping information about variation within the mouse genome associated with hearing loss.
引用
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页码:335 / 352
页数:17
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