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首页> 外文期刊>Cellular and molecular life sciences: CMLS >Mechanical stimulation of polycystin-1 induces human osteoblastic gene expression via potentiation of the calcineurin/NFAT signaling axis
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Mechanical stimulation of polycystin-1 induces human osteoblastic gene expression via potentiation of the calcineurin/NFAT signaling axis

机译:机械刺激polycystin-1通过增强钙调神经磷酸酶/ NFAT信号轴来诱导人成骨细胞基因表达

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摘要

Mechanical forces trigger biological responses in bone cells that ultimately control osteoblastogenesis and bone program. Although several mechanosensors have been postulated, the precise mechanotransduction pathway remains obscure as the initial mechanosensing event has not yet been identified. Studies in kidney cells have shown that polycystin-1 (PC1), via its extracellular N-terminal part, may function as an antenna-like protein providing a linkage between environmental cues and their conversion into biochemical responses that regulate various cellular processes via the calcineurin/NFAT pathway. Here we explored the involvement of PC1 in mechanical load (stretching)-induced signaling cascades that control osteoblastogenesis/bone formation. FACS and TransAM Transcription Factor ELISA analyses employing extracts from primary human osteoblast-like, PC1 expressing cells subjected to mechanical stretching (0-6 h) revealed that unphosphorylated/DNA-binding competent NFATc1 increased at 0.5-1 h and returned to normal at 6 h. In accordance with the activation mechanism of NFATc1, stretching of cultured cells pre-treated with cyclosporin A (CsA, a specific inhibitor of the calcineurin/NFAT pathway) abrogated the observed decrease in the abundance of the cytoplasmic pNFATc1 (phosphorylated/inactive) species. Furthermore, stretching of osteoblastic cells pre-treated with an antibody against the mechanosensing N-terminal part of PC1 also abrogated the observed decrease in the cytoplasmic levels of the inactive pNFATc1 species. Importantly, under similar conditions (pre-incubation of stretched cells with the inhibitory anti-PC1 antibody), the expression of the key osteoblastic, NFATc1-target gene runx2 decreased compared to untreated cells. Therefore, PC1 acts as chief mechanosensing molecule that modulates osteoblastic gene transcription and hence bone-cell differentiation through the calcineurin/NFAT signaling cascade.
机译:机械力触发骨骼细胞中的生物学反应,最终控制成骨细胞的生成和骨骼程序。尽管已经提出了几种机械传感器,但是由于尚未识别出最初的机械传感事件,因此精确的机械转导途径仍然不清楚。对肾细胞的研究表明,多囊藻蛋白1(PC1)通过其细胞外N端部分,可以起天线样蛋白的作用,提供环境提示与其转化为通过钙调神经磷酸酶调节各种细胞过程的生化反应之间的联系。 / NFAT途径。在这里,我们探讨了PC1参与机械负荷(拉伸)诱导的控制成骨细胞生成/骨形成的信号级联反应。 FACS和TransAM转录因子ELISA分析采用了原代人成骨细胞样PC1表达细胞的提取物,这些细胞经过机械拉伸(0-6小时)后发现,未磷酸化/ DNA结合能力的NFATc1在0.5-1小时增加,并在6小时恢复正常H。根据NFATc1的激活机制,用环孢菌素A(钙调神经磷酸酶/ NFAT途径的特异性抑制剂)预处理的培养细胞的拉伸消除了所观察到的胞质pNFATc1(磷酸化/非活性)物种丰度的降低。此外,用抗PC1的机械传感N端抗体进行预处理的成骨细胞的拉伸也消除了观察到的无活性pNFATc1的胞质水平下降。重要的是,在相似的条件下(拉伸细胞与抑制性抗PC1抗体预孵育),与未处理的细胞相比,成骨细胞NFATc1靶标关键基因runx2的表达下降。因此,PC1充当主要的机械传感分子,通过钙调神经磷酸酶/ NFAT信号级联反应调节成骨细胞基因转录,从而调节骨细胞分化。

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