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A 3D-bioprinted scaffold with doxycycline-controlled BMP2-expressing cells for inducing bone regeneration and inhibiting bacterial infection

机译:具有多西环素控制的BMP2表达细胞的3D-生物印刷的支架用于诱发骨再生和抑制细菌感染

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摘要

Large bone defects face a high risk of pathogen exposure due to open wounds, which leads to high infection rates and delayed bone union. To promote successful repair of infectious bone defects, fabrication of a scaffold with dual functions of osteo-induction and bacterial inhibition is required. This study describes creation of an engineered progenitor cell line (C3H10T1/2) capable of doxycycline (DOX)-mediated release of bone morphogenetic protein-2 (BMP2). Three-dimensional bioprinting technology enabled creation of scaffolds, comprising polycaprolactone/mesoporous bioactive glass/DOX and bioink, containing these engineered cells. In vivo and in vitro experiments confirmed that the scaffold could actively secrete BMP2 to significantly promote osteoblast differentiation and induce ectopic bone formation. Additionally, the scaffold exhibited broad-spectrum antibacterial capacity, thereby ensuring the survival of embedded engineered cells when facing high risk of infection. These findings demonstrated the efficacy of this bioprinted scaffold to release BMP2 in a controlled manner and prevent the occurrence of infection; thus, showing its potential for repairing infectious bone defects.
机译:由于开放的伤口,大骨缺损面临高风险的病原体暴露,这导致高感染率和延迟骨内联合。为了促进传染性骨缺损的成功修复,需要使用骨肉诱导和细菌抑制的双函数的支架的制造。本研究描述了能够产生能够进行强霉素(DOX)介导的骨形态发生蛋白-2(BMP2)的工程化祖细胞系(C3H10T1 / 2)的创建。三维生物监测技术使得构成支架,包括聚己内酯/中孔生物活性玻璃/ DOX和生物链,含有这些工程细胞。体内和体外实验证实,支架可以积极分泌BMP2以显着促进成骨细胞分化并诱导异位骨形成。另外,支架表现出广谱抗菌容量,从而确保面对感染风险高时嵌入式工程细胞的存活。这些研究结果证明了这种生物印刷的支架以受控方式释放BMP2的功效,并防止感染的发生;因此,表明其适用于修复传染性骨缺陷。

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