TiO2纳米管通过Kindlin-2/Integrin β1/YAP途径介导的机械传导促进成骨。

Qing Deng, Quanzhou Yao, Anhang Wu, Jinsheng Li, Yingying Li, Lingling Tang, Huanghe Zeng, Song Chen, Tailin Guo
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引用次数: 0

摘要

钛因其卓越的机械和生物特性,已被广泛应用于整形外科和牙科领域。经证实,由表面改性产生的二氧化钛(TiO2)纳米管(TNTs)形态所诱导的机械刺激可增强骨髓间充质干细胞(BMSCs)的成骨分化。Kindlin-2是一种关键的局灶粘附蛋白,通过调节应力纤维丝的组装参与机械信号转导过程。要弄清Kindlin-2参与TNTs诱导成骨分化的机制还需要更多的研究。本研究系统研究了Kindlin-2对TNTs诱导成骨和机械传导的影响。采用阳极氧化法制备了直径约为30 nm(TNT-30)和100 nm(TNT-100)的TiO2纳米管,并对其进行了表征。结果表明,与抛光钛(PT)和TNT-30相比,TNT-100能显著增加Kindlin-2的表达,增强成骨分化。此外,Kindlin-2通过调节整合素β1/FAK/RhoA信号通路促进细胞骨架组装,以YAP依赖性方式影响成骨基因表达和BMSC分化。因此,这些发现有助于更全面地了解BMSCs在TNTs形态上的命运,并为开发先进的骨修复生物材料提供了新的理论基础。
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TiO2 nanotube enhance osteogenesis through Kindlin-2/Integrin β1/YAP pathway-mediated mechanotransduction.

Titanium has been widely employed in the fields of orthopaedics and dentistry, attributed to its superior mechanical and biological properties. The mechanical stimulation induced by the titanium dioxide (TiO2) nanotubes (TNTs) morphology resulting from surface modification has been demonstrated to enhance the osteogenic differentiation of bone marrow-derived mesenchymal stem cells (BMSCs). Kindlin-2, a pivotal focal adhesion protein, is involved in mechanical signaling processes through the regulation of stress fibril filament assembly. Additional research is needed to clarify the involvement of Kindlin-2 in the mechanism of TNTs-induced osteogenic differentiation. This study systematically investigated the impact of Kindlin-2 on TNTs-induced osteogenesis and mechanotransduction. TiO2 nanotubes with diameters of approximately 30 nm (TNT-30) and 100 nm (TNT-100) were fabricated and characterized using anodic oxidation. The results showed that TNT-100 significantly increased the expression of Kindlin-2 and enhanced osteogenic differentiation compared to polished titanium (PT) and TNT-30. Additionally, Kindlin-2 promotes cytoskeleton assembly by regulating the integrin β1/FAK/RhoA signaling pathway, impacting osteogenic gene expression and BMSC differentiation in a Yes-Associated Protein (YAP)-dependent manner. Therefore, these findings contribute to a more comprehensive understanding of the fate of BMSCs on TNTs morphologies and provide a novel theoretical foundation for the development of advanced bone repair biomaterials.

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