SUMMARY: Given the biological function of SOX6 and recent genome-wide association finding, we performed a fine-mapping association analyses to investigate the relationship between SOX6 and BMD both in Caucasian and Chinese populations. We identified many single-nucleotide polymorphisms (SNPs) within or near the SOX6 gene to be significantly associated with hip bone mineral density (BMD). INTRODUCTION: SOX6 gene is an essential transcription factor in chondrogenesis and cartilage formation. Recent genome-wide association studies (GWAS) detected a SNP (rs7117858) located at the downstream of SOX6 significantly associated with hip BMD. METHODS: Given the biological function of SOX6 and the GWAS finding, we considered SOX6 as a new candidate for BMD and osteoporosis. Therefore, in this study, we performed a fine-mapping association analyses to investigate the relationship between SNPs within and near the SOX6 gene and BMD at both hip and spine. A total of 301 SNPs were tested in two independent US Caucasian populations (2,286 and 1,000 unrelated subjects, respectively) and a Chinese population (1,627 unrelated Han subjects). RESULTS: We confirmed that the previously reported rs7117858-A was associated with reduced hip BMD, with combined P value of 2.45 x 10(-4). Besides this SNP, we identified another 19 SNPs within or near the SOX6 gene to be significantly associated with hip BMD after false discovery rate adjustment. The most significant SNP was rs1347677 located at the intron 3 (P = 3.15 x 10(-7)). Seven additional SNPs in high linkage disequilibrium with rs1347677 were also significantly associated with hip BMD. SNPs in SOX6 showed significant skeletal site specificity since no SNP was detected to be associated with spine BMD. CONCLUSION: Our study identified many SNPs in the SOX6 gene associated with hip BMD even across different ethnicities, which further highlighted the importance of the SOX6 gene influencing BMD variation and provided more information to the understanding of the genetic architecture of osteoporosis.
展开▼
机译:摘要:鉴于SOX6的生物学功能和最近的全基因组关联发现,我们进行了精细映射关联分析,以研究白种人和中国人群体中SOX6与BMD之间的关系。我们发现SOX6基因内或附近的许多单核苷酸多态性(SNP)与髋骨矿物质密度(BMD)显着相关。简介:SOX6基因是软骨形成和软骨形成中必不可少的转录因子。最近的全基因组关联研究(GWAS)检测到位于SOX6下游的SNP(rs7117858)与髋骨BMD显着相关。方法:鉴于SOX6的生物学功能和GWAS的发现,我们认为SOX6是BMD和骨质疏松症的新候选者。因此,在这项研究中,我们进行了精细映射的关联分析,以研究髋关节和脊柱SOX6基因内部和附近的SNP与BMD之间的关系。在两个独立的美国高加索人群(分别为2286和1,000个无关的受试者)和一个中国人群(1,627个无关的汉族受试者)中测试了总共301个SNP。结果:我们证实先前报道的rs7117858-A与髋部BMD降低有关,合并P值为2.45 x 10(-4)。除了这个SNP,我们还发现在错误发现率调整后,SOX6基因内或附近的另外19个SNP与髋骨BMD显着相关。最重要的SNP是位于内含子3的rs1347677(P = 3.15 x 10(-7))。 rs1347677在高连锁不平衡中另外七个SNP也与髋骨BMD显着相关。由于未检测到SNP与脊柱BMD相关,因此SOX6中的SNP显示出明显的骨骼部位特异性。结论:我们的研究甚至在不同种族中都发现了与髋部BMD相关的SOX6基因中的许多SNP,这进一步突显了SOX6基因影响BMD变异的重要性,并为了解骨质疏松症的遗传结构提供了更多信息。
展开▼
