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BMP-induced Atoh8 attenuates osteoclastogenesis by suppressing Runx2 transcriptional activity and reducing the Rankl/Opg expression ratio in osteoblasts

机译:BMP诱导的Atoh8通过抑制Runx2转录活性并降低成骨细胞中的Rankl / Opg表达比来减弱破骨细胞生成

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摘要

Adult bone structural integrity is maintained by remodeling via the coupling of osteoclastic bone resorption and osteoblastic bone formation.Osteocytes or osteoblasts express receptor activator of nuclear factor k-B ligand(Rankl)or osteoprotegerin(Opg)to promote or inhibit osteoclastogenesis,respectively.Bone morphogenetic protein(BMP)is a potent bone inducer,but its major role in adult bone is to induce osteocytes to upregulate sclerostin(Sost)and increase the Rankl/Opg expression ratio,resulting in promotion of osteoclastogenesis.However,the precise effect of BMP-target gene(s)in osteoblasts on the Rankl/Opg expression ratio remains unclear.In the present study,we identified atonal homolog 8(Atoh8),which is directly upregulated by the BMPSmadl axis in osteoblasts.In vivo,Atoh8 was detected in osteoblasts but not osteocytes in adult mice.Although global Atoh8-knockout mice showed only a mild phenotype in the neonate skeleton,the bone volume was decreased and osteoclasts were increased in the adult phase.Atoh8-null marrow stroma cells were more potent than wild-type cells in inducing osteoclastogenesis in marrow cells.Atoh8 loss in osteoblasts increased Runx2 expression and the Rankl/Opg expression ratio,while Runx2 knockdown normalized the Rankl/Opg expression ratio.Moreover,Atoh8 formed a protein complex with Runx2 to inhibit Runx2 transcriptional activity and decrease the Rankl/Opg expression ratio.These results suggest that bone remodeling is regulated elaborately by BMP signaling;while BMP primarily promotes bone resorption,it simultaneously induces Atoh8 to inhibit Runx2 and reduce the Rankl/Opg expression ratio in osteoblasts,suppressing osteoclastogenesis and preventing excessive BMP-mediated bone resorption.
机译:通过骨细胞骨吸收和成骨细胞骨形成的偶联来重塑成人骨结构完整性。稳妥或骨细胞表达核因子Kb配体(RANKL)或骨蛋白酶(OPG)的受体活化剂,分别分别促进或抑制骨质细胞发生。的形态发生蛋白(BMP)是一种有效的骨诱导剂,但其在成年骨中的主要作用是诱导骨细胞来上调燃气蛋白(SOST)并提高RANKL / OPG表达比,导致骨质细胞发生促进。然而,BMP-靶的确切效果对rankl / OPG表达比的成骨细胞中的基因仍未持续。在本研究中,我们鉴定了亚核同源物8(ATOH8),其直接通过成骨细胞中的BMPSMadl轴线上调。在体内,在成骨细胞中检测到ath8但是不是成人小鼠的骨细胞。虽然全球ath8-nocketout小鼠仅在新生儿骨架中显示出一种温和的表型,但骨骼体积减少,并且疏口细胞增加在成人期间。除了在骨髓细胞中诱导骨髓细胞中野生型细胞的野生型细胞更有效。成骨细胞中的损失增加了RUNX2表达和RANKL / OPG表达比,而RUNX2敲除归一化RANKL / OPG表达。ath8,atoh8形成蛋白质复合物,runx2抑制Runx2转录活性并降低RANK1 / OPG表达比。这些结果表明骨重塑是通过BMP信号精细调节的;而BMP主要促进骨吸收,同时诱导ATOH8抑制RUNX2并降低成骨细胞中的RANKL / OPG表达比,抑制骨细胞发生并防止过量的BMP介导的骨吸收。

著录项

  • 来源
    《骨研究:英文》 |2020年第003期|P.365-378|共14页
  • 作者单位

    Department of Orthopaedic Surgery Kagoshima University Kagoshima Kagoshima 890-8520 JapanDepartment of Medical Joint Materials Kagoshima University Kagoshima Kagoshima 890-8520 Japan;

    Department of Medical Joint Materials Kagoshima University Kagoshima Kagoshima 890-8520 JapanDepartment of Bone and Joint Medicine Kagoshima University Kagoshima Kagoshima 890-8520 Japan;

    Department of Orthopaedic Surgery Kagoshima University Kagoshima Kagoshima 890-8520 Japan;

    Department of Molecular Pathology Graduate School of Medicine The University of Tokyo Bunkyo-ku Tokyo 113-0033 Japan;

    Department of Orthopaedic Surgery Kagoshima University Kagoshima Kagoshima 890-8520 JapanDepartment of Medical Joint Materials Kagoshima University Kagoshima Kagoshima 890-8520 JapanDepartment of Bone and Joint Medicine Kagoshima University Kagoshima Kagoshima 890-8520 Japan;

    Department of Orthopaedic Surgery Kagoshima University Kagoshima Kagoshima 890-8520 JapanDepartment of Medical Joint Materials Kagoshima University Kagoshima Kagoshima 890-8520 JapanDepartment of Bone and Joint Medicine Kagoshima University Kagoshima Kagoshima 890-8520 Japan;

    Department of Orthopaedic Surgery Kagoshima University Kagoshima Kagoshima 890-8520 Japan;

    Institute for Frontier Life and Medical Sciences Kyoto University Sakyo-ku Kyoto 606-8507 Japan;

    Department of Molecular Pathology Graduate School of Medicine The University of Tokyo Bunkyo-ku Tokyo 113-0033 Japan;

    Department of Orthopaedic Surgery Kagoshima University Kagoshima Kagoshima 890-8520 JapanDepartment of Medical Joint Materials Kagoshima University Kagoshima Kagoshima 890-8520 JapanDepartment of Bone and Joint Medicine Kagoshima University Kagoshima Kagoshima 890-8520 Japan;

  • 收录信息 中国科学引文数据库(CSCD);
  • 原文格式 PDF
  • 正文语种 chi
  • 中图分类 内分泌腺疾病及代谢病;
  • 关键词

    Runx2; osteoclast; BMP;

    机译:Runx2;破骨细胞;BMP;
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