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PLGA/β-TCP composite scaffold incorporating cucurbitacin B promotes bone regeneration by inducing angiogenesis

机译:掺入CUCUBRITACIN B的PLGA /β-TCP复合支架通过诱导血管生成来促进骨再生

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ObjectivesVascularization is an essential step in successful bone tissue engineering. The induction of angiogenesis in bone tissue engineering can be enhanced through the delivery of therapeutic agents that stimulate vessel and bone formation. In this study, we show that cucurbitacin B (CuB), a tetracyclic terpene derived from Cucurbitaceae family plants, facilitates the induction of angiogenesisin vitro.MethodsWe incorporated CuB into a biodegradable poly (lactide-co-glycolide) (PLGA) and β-tricalcium phosphate (β-TCP) biomaterial scaffold (PT/CuB) Using 3D low-temperature rapid prototyping (LT-RP) technology. A rat skull defect model was used to verify whether the drug-incorporated scaffold has the effects of angiogenesis and osteogenesisin vivofor the regeneration of bone defect. Cytotoxicity assay was performed to determine the safe dose range of the CuB. Tube formation assay and western blot assay were used to analyze the angiogenesis effect of CuB.ResultsPT/CuB scaffold possessed well-designed bio-mimic structure and improved mechanical properties. CuB was linear release from the composite scaffold without affecting pH value. The results demonstrated that the PT/CuB scaffold significantly enhanced neovascularization and bone regeneration in a rat critical size calvarial defect model compared to the scaffold implants without CuB. Furthermore, CuB stimulated angiogenic signaling via up-regulating VEGFR2 and VEGFR-related signaling pathways.ConclusionCuB can serve as promising candidate compound for promoting neovascularization and osteogenesis, especially in tissue engineering for repair of bone defects.The translational potential of this articleThis study highlights the potential use of CuB as a therapeutic agent and strongly support its adoption as a component of composite scaffolds for tissue-engineering of bone repair.
机译:目标血管化是成功骨组织工程中的重要步骤。通过递送刺激血管和骨形成的治疗剂,可以增强骨组织工程中血管生成的诱导。在这项研究中,我们表明,苏布达汀B(幼崽)衍生自葫芦科家族植物的四环素萜烯,促进了血管生成素体外诱导凝聚幼崽进入可生物降解的聚(丙交酯 - 共乙酰胺)(PLGA)和β-三族磷酸盐(β-TCP)生物材料支架(PT / CUB)使用3D低温快速原型设计(LT-RP)技术。使用大鼠颅骨缺陷模型来验证药物掺入的支架是否具有血管生成和骨源性素的影响骨缺损的再生。进行细胞毒性测定以确定幼崽的安全剂量范围。管形成测定和蛋白质印迹测定用于分析CUB.Resultspt / Cum支架具有精心设计的生物模拟结构和改善的机械性能。幼崽在没有影响pH值的情况下从复合支架上线性释放。结果表明,与没有幼崽的支架植入物相比,Pt / Cum支架在大鼠临界大小颅缺陷模型中显着提高了新生血管和骨再生。此外,幼崽通过Up-Crommate VEGFR2和VEGFR相关的信号通路刺激血管生成信号传导。结论COUB可以作为促进新血管形成和骨肉发生的有前途的候选化合物,特别是在组织工程中用于修复骨缺损。这项艺术的研究的翻译潜力突出了潜在使用幼崽作为治疗剂,并强烈支持其作为骨骼修复组织工程组织工程的组成部分。

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