在成骨细胞中敲除 Hdac4 会影响骨骼的分解代谢和合成代谢作用。
The Deletion of Hdac4 in Mouse Osteoblasts Influences Both Catabolic and Anabolic Effects in Bone.
机构信息
Department of Basic Science and Craniofacial Biology, New York University College of Dentistry, New York, NY, USA.
Department of Orthopedic Surgery, Mayo Clinic, Rochester, MN, USA.
出版信息
J Bone Miner Res. 2018 Jul;33(7):1362-1375. doi: 10.1002/jbmr.3422. Epub 2018 Apr 25.
Histone deacetylase 4 (Hdac4) is known to control chondrocyte hypertrophy and bone formation. We have previously shown that parathyroid hormone (PTH) regulates many aspects of Hdac4 function in osteoblastic cells in vitro; however, in vivo confirmation was previously precluded by preweaning lethality of the Hdac4-deficient mice. To analyze the function of Hdac4 in bone in mature animals, we generated mice with osteoblast lineage-specific knockout of Hdac4 (Hdac4 ) by crossing transgenic mice expressing Cre recombinase under the control of a 2.3-kb fragment of the Col1a1 promoter with mice bearing loxP-Hdac4. The Hdac4 mice survive to adulthood and developed a mild skeletal phenotype. At age 12 weeks, they had short, irregularly shaped and stiff tails due to smaller tail vertebrae, with almost no growth plates. The tibial growth plate zone was also thinned, and Mmp13 and Sost mRNAs were increased in the distal femurs of Hdac4 mice. Immunohistochemistry showed that sclerostin was elevated in Hdac4 mice, suggesting that Hdac4 inhibits its gene and protein expression. To determine the effect of PTH in these mice, hPTH (1-34) or saline were delivered for 14 days with subcutaneously implanted devices in 8-week-old female Hdac4 and wild-type (Hdac4 ) mice. Serum CTX, a marker of bone resorption, was increased in Hdac4 mice with or without PTH treatment. Tibial cortical bone volume/total volume (BV/TV), cortical thickness (Ct.Th), and relative cortical area (RCA) were decreased in Hdac4 mice, but PTH caused no further decrease in Hdac4 mice. Tibial trabecular BV/TV and thickness were not changed significantly in Hdac4 mice but decreased with PTH treatment. These results indicate that Hdac4 inhibits bone resorption and has anabolic effects via inhibiting Mmp13 and Sost/sclerostin expression. Hdac4 influences cortical bone mass and thickness and knockout of Hdac4 prevents the catabolic effect of PTH in cortical bone. © 2018 American Society for Bone and Mineral Research.
组蛋白去乙酰化酶 4(Hdac4)已知可控制软骨细胞肥大和骨形成。我们之前已经表明,甲状旁腺激素(PTH)在体外调节成骨细胞中 Hdac4 功能的许多方面;然而,由于 Hdac4 缺陷型小鼠在断奶前的致死性,以前无法进行体内证实。为了分析 Hdac4 在成熟动物骨骼中的功能,我们通过将表达 Cre 重组酶的转基因小鼠与携带 loxP-Hdac4 的小鼠杂交,生成了成骨细胞谱系特异性 Hdac4 敲除(Hdac4)的小鼠(Hdac4)由 Col1a1 启动子的 2.3kb 片段控制。Hdac4 小鼠存活至成年期,并表现出轻度骨骼表型。在 12 周龄时,由于较小的尾椎骨,它们的尾巴短、形状不规则且僵硬,几乎没有生长板。胫骨生长板区也变薄,并且 Hdac4 小鼠的远端股骨中 Mmp13 和 Sost mRNA 增加。免疫组织化学显示,Hdac4 小鼠的硬化素升高,表明 Hdac4 抑制其基因和蛋白表达。为了确定 PTH 在这些小鼠中的作用,在 8 周龄的雌性 Hdac4 和野生型(Hdac4)小鼠中,用皮下植入装置分别给予 hPTH(1-34)或生理盐水 14 天。有或没有 PTH 治疗的 Hdac4 小鼠的血清 CTX,骨吸收的标志物增加。Hdac4 小鼠的胫骨皮质骨体积/总体积(BV/TV)、皮质厚度(Ct.Th)和相对皮质面积(RCA)降低,但 PTH 未进一步降低 Hdac4 小鼠的皮质骨。Hdac4 小鼠的胫骨小梁 BV/TV 和厚度没有明显变化,但用 PTH 处理后减少。这些结果表明,Hdac4 通过抑制 Mmp13 和 Sost/硬化素的表达来抑制骨吸收并具有合成代谢作用。Hdac4 影响皮质骨量和厚度,并且 Hdac4 的缺失可防止 PTH 在皮质骨中的分解代谢作用。© 2018 美国骨骼与矿物质研究协会。
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