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Nanoscale Coatings for Ultralow Dose BMP‐2‐Driven Regeneration of Critical‐Sized Bone Defects

机译:纳米涂料可用于关键剂量骨缺损的超低剂量BMP-2驱动再生

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摘要

While new biomaterials for regenerative therapies are being reported in the literature, clinical translation is slow. Some existing regenerative approaches rely on high doses of growth factors, such as bone morphogenetic protein‐2 (BMP‐2) in bone regeneration, which can cause serious side effects. An ultralow‐dose growth factor technology is described yielding high bioactivity based on a simple polymer, poly(ethyl acrylate) (PEA), and mechanisms to drive stem cell differentiation and bone regeneration in a critical‐sized murine defect model with translation to a clinical veterinary setting are reported. This material‐based technology triggers spontaneous fibronectin organization and stimulates growth factor signalling, enabling synergistic integrin and BMP‐2 receptor activation in mesenchymal stem cells. To translate this technology, plasma‐polymerized PEA is used on 2D and 3D substrates to enhance cell signalling in vitro, showing the complete healing of a critical‐sized bone injury in mice in vivo. Efficacy is demonstrated in a Münsterländer dog with a nonhealing humerus fracture, establishing the clinical translation of advanced ultralow‐dose growth factor treatment.
机译:尽管文献中报道了用于再生疗法的新生物材料,但临床翻译缓慢。一些现有的再生方法依赖高剂量的生长因子,例如骨骼再生中的骨形态发生蛋白-2(BMP-2),这可能会导致严重的副作用。描述了一种超低剂量生长因子技术,该技术以简单的聚合物,聚丙烯酸乙酯(PEA)为基础,具有很高的生物活性,并在关键尺寸的鼠缺陷模型中将干细胞分化和骨再生的机制驱动并转化为临床报告兽医情况。这项基于材料的技术可触发自发性纤连蛋白组织并刺激生长因子信号传导,从而使间充质干细胞中的整合素和BMP-2受体协同活化。为了实现这一技术的转化,在2D和3D基质上使用了血浆聚合的PEA来增强体外细胞信号传导,从而显示出小鼠体内临界大小的骨损伤的完全愈合。在具有未愈合的肱骨骨折的Münsterländer狗中证明了疗效,确立了先进的超低剂量生长因子治疗的临床翻译。

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