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东亚人群的全基因组关联研究表明,UHMK1是一种新的骨密度易感基因。

Genome-wide association study in East Asians suggests UHMK1 as a novel bone mineral density susceptibility gene.

作者信息

Choi Hyung Jin, Park Hyojung, Zhang Lei, Kim Jung Hee, Kim Ye An, Yang Jae-Yeon, Pei Yu-Fang, Tian Qing, Shen Hui, Hwang Joo-Yeon, Deng Hong-Wen, Cho Nam H, Shin Chan Soo

机构信息

Department of Anatomy, Department of Biomedical Sciences, Seoul National University College of Medicine, Seoul, Republic of Korea.

Department of Internal Medicine, Seoul National University College of Medicine, Seoul, Republic of Korea.

出版信息

Bone. 2016 Oct;91:113-21. doi: 10.1016/j.bone.2016.07.008. Epub 2016 Jul 15.

Abstract

To identify genetic variants that influence bone mineral density (BMD) in East Asians, we performed a quantitative trait analysis of lumbar spine, total hip and femoral neck BMD in a Korean population-based cohort (N=2729) and follow-up replication analysis in a Chinese Han population and two Caucasian populations (N=1547, 2250 and 987, respectively). From the meta-analysis of the stage 1 discovery analysis and stage 2 replication analysis, we identified four BMD loci that reached near-genome-wide significance level (P<5×10(-7)). One locus on 1q23 (UHMK1, rs16863247, P=4.1×10(-7) for femoral neck BMD and P=3.2×10(-6) for total hip BMD) was a novel BMD signal. Interestingly, rs16863247 was very rare in Caucasians (minor allele frequency<0.01), indicating that this association could be specific to East Asians. In gender specific analysis, rs1160574 on 1q32 (KCNH1) was associated with femoral neck BMD (P=2.1×10(-7)) in female subjects. rs9371538 in the known BMD region on 6q25 ESR1 was associated with lumbar spine BMD (P=5.6×10(-9)). rs7776725 in the known BMD region on 7q31 WTN16 was associated with total hip BMD (P=8.6×10(-9)). In osteoblasts, endogenous UHMK1 expression was increased during differentiation and UHMK1 knockdown decreased its differentiation, while UHMK1 overexpression increased its differentiation. In osteoclasts, endogenous UHMK1 expression was decreased during differentiation and UHMK1 knockdown increased its differentiation, while UHMK1 overexpression decreased its differentiation. In conclusion, our genome-wide association study identified the UHMK1 gene as a novel BMD locus specific to East Asians. Functional studies suggest a role of UHMK1 on regulation of osteoblasts and osteoclasts.

摘要

为了鉴定影响东亚人骨密度(BMD)的基因变异,我们在一个基于韩国人群的队列(N = 2729)中对腰椎、全髋和股骨颈骨密度进行了定量性状分析,并在中国汉族人群和两个高加索人群(分别为N = 1547、2250和987)中进行了随访重复分析。通过对第一阶段发现分析和第二阶段重复分析的荟萃分析,我们鉴定出四个达到近全基因组显著性水平(P < 5×10⁻⁷)的骨密度位点。1q23上的一个位点(UHMK1,rs16863247,股骨颈骨密度的P = 4.1×10⁻⁷,全髋骨密度的P = 3.2×10⁻⁶)是一个新的骨密度信号。有趣的是,rs16863247在高加索人中非常罕见(次要等位基因频率<0.01),表明这种关联可能是东亚人特有的。在性别特异性分析中,1q32上的rs1160574(KCNH1)与女性受试者的股骨颈骨密度相关(P = 2.1×10⁻⁷)。6q25上已知骨密度区域的rs9371538(ESR1)与腰椎骨密度相关(P = 5.6×10⁻⁹)。7q31上已知骨密度区域的rs7776725(WTN16)与全髋骨密度相关(P = 8.6×10⁻⁹)。在成骨细胞中,内源性UHMK1表达在分化过程中增加,敲低UHMK1会降低其分化,而过表达UHMK1会增加其分化。在破骨细胞中,内源性UHMK1表达在分化过程中降低,敲低UHMK1会增加其分化,而过表达UHMK1会降低其分化。总之,我们的全基因组关联研究将UHMK1基因鉴定为东亚人特有的一个新的骨密度位点。功能研究表明UHMK1在成骨细胞和破骨细胞的调节中起作用。

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