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首页> 外文期刊>Journal of bone and mineral research: the official journal of the American Society for Bone and Mineral Research >Genome-wide haplotype association mapping in mice identifies a genetic variant in CER1 associated with BMD and fracture in southern Chinese women.
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Genome-wide haplotype association mapping in mice identifies a genetic variant in CER1 associated with BMD and fracture in southern Chinese women.

机译:小鼠中的全基因组单体型关联图谱鉴定了中国南方女性中与BMD和骨折相关的CER1基因变异。

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摘要

BMD is a heritable trait and risk indicator for osteoporosis. In this study, we used a genome-wide haplotype association mapping (HAM) approach to identify a haplotype block within Cer1 that partitions inbred mice strains into high and low BMD groups. A cohort of 1083 high and low BMD human subjects were studied, and a nonsynonymous SNP (rs3747532) in human CER1 was identified to be associated with increased risk of both low BMD in premenopausal women (OR: 2.2; 95% CI: 1.0-4.6; p < 0.05) and increased risk of vertebral fractures (OR: 1.82, p = 0.025) in the postmenopausal cohort. We also showed that Cer1 is expressed in mouse bone and growth plate by RT-PCR, immunohistochemistry, and in situ hybridization, consistent with polymorphisms potentially influencing BMD. Our successful identification of an association with CER1 in humans together with our mouse study suggests that CER1 may play a role in the development of bone or its metabolism. Our study highlights the use of publicly available databases for rapidly surveying the genome for quantitative trait loci.
机译:BMD是骨质疏松症的遗传特征和危险指标。在这项研究中,我们使用了全基因组单倍型关联作图(HAM)方法来识别Cer1内的单倍型模块,该模块将近交小鼠品系分为高BMD组和低BMD组。研究人员对1083名高BMD和低BMD人群进行了研究,并且发现人类CER1中的同义SNP(rs3747532)与绝经前女性低BMD风险增加相关(OR:2.2; 95%CI:1.0-4.6 ; p <0.05)和绝经后队列中椎骨骨折的风险增加(OR:1.82,p = 0.025)。我们还显示,通过RT-PCR,免疫组织化学和原位杂交,Cer1在小鼠骨骼和生长板中表达,与可能影响BMD的多态性一致。我们在人类中与CER1的关联的成功鉴定以及我们的小鼠研究表明,CER1可能在骨骼发育或其代谢中发挥作用。我们的研究强调了使用公共数据库快速调查基因组的数量性状基因座。

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