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Identification of PIEZO1 polymorphisms for human bone mineral density

机译:人骨矿物密度压电1多态性的鉴定

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摘要

Bone mineral density (BMD) is a key indicator for diagnosis and treatment for osteoporosis; the reduction of BMD could increase the risk of osteoporotic fracture. It was very recently found that Piezo1 mediated mechanically evoked responses in bone and further participated in bone formation in mice. Here, we performed cross phenotype meta-analysis for human BMD at lumbar spine (LS), femoral neck (FN), distal radius/forearm (FA) and heel and screened out 14 top SNPs for PIEZO1, these SNPs were overlapped with putative enhancers, DNase-I hypersensitive sites and active promoter flanking regions. We found that the signal of the best SNP rs62048221 was mainly from heel ultrasound estimated BMD (-0.02 SD per T allele, P = 8.50E-09), where calcaneus supported most of the mechanical force of body when standing, walking and doing physical exercises. Each copy of the effect allele T of SNP rs62048221 was associated with a decrease of 0.0035 g/cm(2) BMD (P = 4.6E-27, SE = 0.0003) in UK Biobank data within 477,760 samples. SNP rs62048221 was located at the enhancer region (HEDD enhancer ID 2331049) of gene PIEZO1, site-directed ChIP assays in human mesenchymal stem cells (hMSCs) showed significant enrichment of H3K4me1 and H3K27ac in this region, luciferase assays showed that rs62048221 could significantly affect the activity of the enhancer where it resides. Our results first suggested that SNP rs62048221 might mediate the PIEZO1 expression level via modulating the activity of cis-regulatory elements and then further affect the BMD.
机译:骨矿物密度(BMD)是骨质疏松症诊断和治疗的关键指标; BMD的减少可以增加骨质疏松骨折的风险。最近发现压电1介导的机械诱发反应在骨中并进一步参与小鼠的骨形成。在这里,我们对腰椎(LS),股骨颈(Fn),远端半径/前臂(FA)和鞋跟进行了交叉表型元分析,并筛选出用于压电1的14个顶部SNP,这些SNP与推定的增强剂重叠,DNase-I过敏位点和活性启动子侧翼区域。我们发现,最好的SNP RS62048221的信号主要来自脚后跟超声估计BMD(每吨-0.02 SD,P = 8.50E-09),其中Callaneus在站立时支撑了大部分机身的机械力量练习。 SNP RS62048221的效果等位基因T的每个拷贝与英国Bioband数据中的0.0035g / cm(2)BMD(P = 4.6e-27,SE = 0.0003)的副本相关联。 SNP RS62048221位于基因压电的增强区(HEDD增强子ID 2331049),人间充质干细胞(HMSCs)中的部位导向芯片测定显示出该区域中H3K4ME1和H3K27Ac的显着富集,荧光素酶测定显示RS62048221可能会显着影响它居住的增强剂的活动。我们的结果首先提出了SNP RS62048221可以通过调节顺式调节元件的活性来介导压电1表达水平,然后进一步影响BMD。

著录项

  • 来源
    《Bone》 |2020年第1期|共7页
  • 作者单位

    Westlake Univ Sch Life Sci Dis &

    Populat DaP Geninfo Lab 18 Shilongshan Rd Hangzhou 310024;

    Univ Chinese Acad Sci Chinese Acad Sci Shanghai Inst Biochem &

    Cell Biol CAS Ctr Excellence Mol;

    Zhejiang Univ Sch Med Affiliated Hosp 2 Dept Orthoped Surg Hangzhou 310009 Peoples R China;

    Zhejiang Univ Sch Med Affiliated Hosp 2 Dept Orthoped Surg Hangzhou 310009 Peoples R China;

    Binzhou Med Univ Affiliated Yantai Hosp Dept Orthoped Yantai 264000 Peoples R China;

    Westlake Univ Sch Life Sci Dis &

    Populat DaP Geninfo Lab 18 Shilongshan Rd Hangzhou 310024;

    Westlake Univ Sch Life Sci Dis &

    Populat DaP Geninfo Lab 18 Shilongshan Rd Hangzhou 310024;

    Case Western Reserve Univ Dept Populat &

    Quantitat Hlth Sci Cleveland OH 44106 USA;

    Univ Chinese Acad Sci Chinese Acad Sci Shanghai Inst Biochem &

    Cell Biol CAS Ctr Excellence Mol;

    Westlake Univ Sch Life Sci Dis &

    Populat DaP Geninfo Lab 18 Shilongshan Rd Hangzhou 310024;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 骨科学(运动系疾病、矫形外科学);
  • 关键词

    Bone mineral density; PIEZO1; Polymorphism; Mechanical force; Regulation;

    机译:骨密度;piezo1;多态性;机械力;调节;

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