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首页> 外文期刊>Human Molecular Genetics >Plastin 3 influences bone homeostasis through regulation of osteoclast activity
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Plastin 3 influences bone homeostasis through regulation of osteoclast activity

机译:塑料3通过调节骨壳活动来影响骨稳态

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摘要

Over 200 million people suffer from osteoporosis worldwide, one third of which will develop osteoporotic bone fractures. Unfortunately, no effective cure exists. Mutations in plastin 3 (PLS3), an F-actin binding and bundling protein, cause X-linked primary osteoporosis in men and predisposition to osteoporosis in postmenopausal women. Moreover, the strongest association so far for osteoporosis in elderly women after menopause was connected to a rare SNP in PLS3, indicating a possible role of PLS3 in complex osteoporosis as well. Interestingly, 5% of the general population are overexpressing PLS3, with yet unknown consequences. Here, we studied ubiquitous Pls3 knockout and PLS3 overexpression in mice and demonstrate that both conditions influence bone remodeling and structure: while Pls3 knockout mice exhibit osteoporosis, PLS3 overexpressing mice show thickening of cortical bone and increased bone strength. We show that unbalanced PLS3 levels affect osteoclast development and function, by misregulating the NF kappa B pathway. We found upregulation of RELA (NF kappa B subunit p65) in PLS3 overexpressing mice-known to stimulate osteoclastogenesis-but strikingly reduced osteoclast resorption. We identify NF kappa B repressing factor (NKRF) as a novel PLS3 interactor, which increasingly translocates to the nucleus when PLS3 is overexpressed. We show that NKRF binds to the NF kappa B downstream target and master regulator of osteoclastogenesis nuclear factor of activated T cells 1 (Nfatc1), thereby reducing its transcription and suppressing osteoclast function. We found the opposite in Pls3 knockout osteoclasts, where decreased nuclear NKRF augmented Nfatc1 transcription, causing osteoporosis. Regulation of osteoclastogenesis and bone remodeling via the PLS3-NKRF-NF kappa B-NFATC1 axis unveils a novel possibility to counteract osteoporosis.
机译:超过2亿人患有全球骨质疏松症,其中三分之一将发展骨质疏松骨折。不幸的是,没有有效的治愈。塑料3(PLS3),F-Actin结合和捆绑蛋白中的突变导致男性和绝经后妇女骨质疏松症的X型初级骨质疏松症。此外,迄今为止骨质女性骨质疏松症的最强烈关联与PLS3中的稀有SNP相连,表明PLS3也在复杂骨质疏松症中的可能作用。有趣的是,5%的一般人群过度表达PLS3,后果未知。在这里,我们在小鼠中研究了无处不在的PLS3敲除和PLS3过表达,并证明这两种情况都会影响骨重塑和结构:而PLS3敲除小鼠表现出骨质疏松症,PLS3过表达小鼠的皮质骨的增厚和骨强度增加。我们展示了不平衡的PLS3水平,通过误导NF Kappa B途径来影响破骨细胞开发和功能。我们发现在PLS3过表达小鼠中的rela(NF Kappa B亚基p65)的上调,以促进骨质细胞发生 - 但显着降低的破骨细胞吸收。我们将NF Kappa B抑制因子(NKRF)识别为新的PLS3互动器,当PLS3过表达时,其越来越易于​​核。我们表明NKRF与活性T细胞1(NFATC1)的骨核苷酸核因子的NF Kappa B下游靶和母稳压因子结合,从而降低其转录和抑制破骨细胞功能。我们在PLS3敲除骨核糖体中发现相反,其中核NKRF增强NFATC1转录减少,导致骨质疏松症。通过PLS3-NKRF-NF Kappa B-NFATC1轴揭示骨髓细胞发生和骨重塑的调节揭示了抵消骨质疏松症的新可能性。

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  • 来源
    《Human Molecular Genetics 》 |2018年第24期| 共14页
  • 作者

    Neugebauer Janine; Heilig Juliane; Hosseinibarkooie Seyyedmohsen; Ross Bryony C.; Mendoza-Ferreira Natalia; Nolte Franziska; Peters Miriam; Hoelker Irmgard; Hupperich Kristina; Tschanz Theresa; Grysko Vanessa; Zaucke Frank; Niehoff Anja; Wirth Brunhilde;

  • 作者单位

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    German Sport Univ Cologne Univ Cologne Cologne Ctr Musculoskeletal Biomech Inst Biomech &

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

    Orthopaed Univ Hosp Friedrichsheim Frankfurt Germany;

    German Sport Univ Cologne Univ Cologne Cologne Ctr Musculoskeletal Biomech Inst Biomech &

    Univ Cologne Inst Genet Ctr Mol Med Cologne Inst Human Genet Cologne Germany;

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  • 正文语种 eng
  • 中图分类 医学遗传学 ;
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