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牙移动起始的机械转导中 Wnt1 的表达和调节。

The expression and regulation of Wnt1 in tooth movement-initiated mechanotransduction.

机构信息

Department of Orthodontics, Graduate School of Medicine, Dentistry, and Pharmaceutical Sciences, Okayama University, Okayama, Japan.

Department of Orthodontics, Graduate School of Medicine, Dentistry, and Pharmaceutical Sciences, Okayama University, Okayama, Japan.

出版信息

Am J Orthod Dentofacial Orthop. 2020 Dec;158(6):e151-e160. doi: 10.1016/j.ajodo.2020.08.006. Epub 2020 Nov 1.

Abstract

INTRODUCTION

The Wnt signaling pathway acts as a key regulator of skeletal development and its homeostasis. However, the potential role of Wnt1 in the mechanotransduction machinery of orthodontic tooth movement-initiated bone remodeling is still unclear. Hence, this study focused on the regulatory dynamics of the Wnt1 expression in both the periodontal ligament (PDL) and osteocytes in vivo and in vitro.

METHODS

The Wnt1 expression in the orthodontically moved maxillary first molar in mice was assessed at 0, 1, and 5 days, on both the compression and tension sides. Primary isolated human PDL (hPDL) fibroblasts, as well as murine long-bone osteocyte-Y4 (MLO-Y4) cells, were exposed to continuous compressive force and static tensile force.

RESULTS

The relative quantification of immunodetection showed that orthodontic tooth movement significantly stimulated the Wnt1 expression in both the PDL and alveolar osteocytes on the tension side on day 5, whereas the expression on the compression side did not change. This increase in the Wnt1 expression, shown in vivo, was also noted after the application of 12% static tensile force in isolated hPDL fibroblasts and 20% in MLO-Y4 cells. In contrast, a compressive force led to the attenuation of the Wnt1 gene expression in both hPDL fibroblasts and MLO-Y4 cells in a force-dependent manner. In the osteocyte-PDL coculture system, recombinant sclerostin attenuated Wnt1 in PDL, whereas the antisclerostin antibody upregulated its gene expression, indicating that mechanically-driven Wnt1 signaling in PDL might be regulated by osteocytic sclerostin.

CONCLUSIONS

Our findings provide that Wnt1 signaling plays a vital role in tooth movement-initiated bone remodeling via innovative mechanotransduction approaches.

摘要

简介

Wnt 信号通路作为骨骼发育及其动态平衡的关键调节剂。然而,Wnt1 在正畸牙齿移动引发的骨重塑过程中的机械转导机制中的潜在作用尚不清楚。因此,本研究侧重于体内和体外研究牙周韧带(PDL)和破骨细胞中 Wnt1 表达的调节动态。

方法

在第 0、1 和 5 天,评估小鼠正畸上颌第一磨牙移动过程中牙周韧带(PDL)和牙槽骨骨细胞中的 Wnt1 表达情况。将原代分离的人牙周膜(hPDL)成纤维细胞和鼠长骨破骨细胞-Y4(MLO-Y4)细胞暴露于持续的压缩力和静态拉伸力下。

结果

免疫检测的相对定量显示,正畸牙齿移动在第 5 天显著刺激了张力侧 PDL 和牙槽骨骨细胞中的 Wnt1 表达,而压缩侧的表达没有变化。这种 Wnt1 表达的增加,在体内观察到,在分离的 hPDL 成纤维细胞中施加 12%的静态拉伸力和 MLO-Y4 细胞中施加 20%的静态拉伸力后也观察到。相比之下,在 hPDL 成纤维细胞和 MLO-Y4 细胞中,压缩力以力依赖性方式导致 Wnt1 基因表达的衰减。在破骨细胞-PDL 共培养系统中,重组硬化素减弱了 PDL 中的 Wnt1,而抗硬化素抗体上调了其基因表达,表明 PDL 中机械驱动的 Wnt1 信号可能受到破骨细胞硬化素的调节。

结论

我们的发现表明,Wnt1 信号在牙齿移动引发的骨重塑中通过创新的机械转导方法发挥了重要作用。

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