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Pathway-based genome-wide association analysis identified the importance of regulation-of-autophagy pathway for ultradistal radius BMD

单核苷酸多态性 全基因组关联研究 骨质疏松症 手腕 遗传关联 医学 骨矿物 遗传学 内科学 生物 生物信息学 基因 解剖 基因型
作者
Lishu Zhang,Yan-Fang Guo,Yaozhong Liu,Yongjun Liu,Donghai Xiong,Xiaogang Liu,Liang Wang,Tie‐Lin Yang,Shu‐Feng Lei,Yan Guo,Han Yan,Yu‐Fang Pei,Feng Zhang,Christopher J. Papasian,Robert R. Recker,Hong‐Wen Deng
出处
期刊:Journal of Bone and Mineral Research [Wiley]
卷期号:25 (7): 1572-1580 被引量:108
标识
DOI:10.1002/jbmr.36
摘要

Wrist fracture is not only one of the most common osteoporotic fractures but also a predictor of future fractures at other sites. Wrist bone mineral density (BMD) is an important determinant of wrist fracture risk, with high heritability. Specific genes underlying wrist BMD variation are largely unknown. Most published genome-wide association studies (GWASs) have focused only on a few top-ranking single-nucleotide polymorphisms (SNPs)/genes and considered each of the identified SNPs/genes independently. To identify biologic pathways important to wrist BMD variation, we used a novel pathway-based analysis approach in our GWAS of wrist ultradistal radius (UD) BMD, examining approximately 500,000 SNPs genome-wide from 984 unrelated whites. A total of 963 biologic pathways/gene sets were analyzed. We identified the regulation-of-autophagy (ROA) pathway that achieved the most significant result (p = .005, q(fdr) = 0.043, p(fwer) = 0.016) for association with UD BMD. The ROA pathway also showed significant association with arm BMD in the Framingham Heart Study sample containing 2187 subjects, which further confirmed our findings in the discovery cohort. Earlier studies indicated that during endochondral ossification, autophagy occurs prior to apoptosis of hypertrophic chondrocytes, and it also has been shown that some genes in the ROA pathway (e.g., INFG) may play important roles in osteoblastogenesis or osteoclastogenesis. Our study supports the potential role of the ROA pathway in human wrist BMD variation and osteoporosis. Further functional evaluation of this pathway to determine the mechanism by which it regulates wrist BMD should be pursued to provide new insights into the pathogenesis of wrist osteoporosis.

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