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首页> 外文期刊>Journal of Orthopaedic Translation >Three-dimensional printed multiphasic scaffolds with stratified cell-laden gelatin methacrylate hydrogels for biomimetic tendon-to-bone interface engineering
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Three-dimensional printed multiphasic scaffolds with stratified cell-laden gelatin methacrylate hydrogels for biomimetic tendon-to-bone interface engineering

机译:具有分层细胞加剧甲基丙烯酸酯水凝胶的三维印刷多相支架,用于生物纤维素对骨界面工程

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BackgroundThe anatomical properties of the enthesis of the rotator cuff are hardly regained during the process of healing. The tendon-to-bone interface is normally replaced by fibrovascular tissue instead of interposition fibrocartilage, which impairs biomechanics in the shoulder and causes dysfunction. Tissue engineering offers a promising strategy to regenerate a biomimetic interface. Here, we report heterogeneous tendon-to-bone interface engineering based on a 3D-printed multiphasic scaffold.MethodsA multiphasic poly(ε-caprolactone) (PCL)–PCL/tricalcium phosphate (TCP)–PCL/TCP porous scaffold was manufactured using 3D printing technology. The three phases of the scaffold were designed to mimic the graded tissue regions in the tendon-to-bone interface—tendon, fibrocartilage, and bone. Fibroblasts, bone marrow–derived mesenchymal stem cells, and osteoblasts were separately encapsulated in gelatin methacrylate (GelMA) and loaded seriatim on the relevant phases of the scaffold, by which a cells/GelMA-multiphasic scaffold (C/G-MS) construct, replicating the native interface, was fabricated. Cell proliferation, viability, and chondrogenic differentiation were evaluated in vitro. The C/G-MS constructs were further examined to determine the potential of regenerating a continuous interface with gradual transition of teno-, fibrocartilage- and osteo-like tissues in vivo.ResultsIn vitro tests confirmed the good cytocompatibility of the constructs. After seven days in culture, cellular microfilament staining indicated that not only could cells well proliferate in GelMA hydrogels??but also efficiently attach to and grow on scaffold fibres. Moreover, by immunolocalizing collagen type II, chondrogenesis was identified in the intermediate phase of the C/G-MS construct that had been treated with transforming growth factor β3 for 21 days. After subcutaneous implantation in mice, the C/G-MS construct exhibited a heterogeneous and graded structure up to eight weeks, with distinguished matrix distribution observed at one week. Overall, gene expression of tenogenic, chondrogenic, and osteogenic markers showed increasing patterns for eight weeks. Among them, expression of collagen type X gene was found drastically increasing during eight weeks, indicating progressive formation of calcifying cartilage within the constructs.ConclusionOur findings demonstrate that the stratified manner of fabrication based on the 3D-printed multiphasic scaffold is an effective strategy for tendon-to-bone interface engineering in terms of efficient cell seeding, chondrogenic potential, and distinct matrix deposition in varying phases.The translational potential of this articleWe fabricated a biomimetic tendon-to-bone interface by using a 3D-printed multiphasic scaffold and adopting a stratified cell-seeding manner with GelMA. The biomimetic interface might have applications in tendon-to-bone repair in the rotator cuff. It can not only be an alternative to a biological fixation device??but also offer an ex vivo living graft to replace the damaged enthesis.
机译:背景技术在愈合过程中,转子袖带的诱疮的解剖性质几乎没有重获。肌腱致骨界面通常由纤维血管组织而不是插入纤维纤维,这损害肩部的生物力学并引起功能障碍。组织工程提供了一个有希望的策略来再生仿生界面。在这里,我们报告基于3D印刷的多相型脚屑的异质肌腱到骨界面工程.方法使用3D制造磷酸钙(PCL)-PCL / TCP)-PCL / TCP多孔支架(TCP)-PCL / TCP多孔支架。印刷技术。设计支架的三个阶段以模拟肌腱与骨界面 - 肌腱,纤维纤维率和骨的分级组织区域。成纤维细胞,骨髓衍生的间充质干细胞和成骨细胞分别包封在明胶甲基丙烯酸酯(凝胶)中包封,并在支架的相关阶段加载SERIATIM,其中细胞/凝胶 - 多相支架(C / G-MS)构建体,复制本机接口,是制造的。在体外评估细胞增殖,活力和软骨内分化。进一步检查C / G-MS构建体以确定在体外转化中再生连续界面的电位,近似转变的体内,素化学试验证实了构建体的良好细胞织组种。在培养七天后,细胞微丝染色表明,细胞不仅可以在凝胶水中越来越长,但也有效地连接到支架纤维上并在支架纤维上生长。此外,通过免疫透明胶原蛋白,II型II型,在已经用转化生长因子β3处理21天的C / G-MS构建体的中间相中鉴定了软骨发生。在小鼠皮下植入后,C / G-MS构建体表现出长达八周的非均相和分级结构,在一周内观察到具有明显的基质分布。总体而言,胎生物,软骨和成骨标志物的基因表达显示出八周的速度增加。其中,在八周内发现胶原型X基因的表达急剧增加,表明构建体内的钙化软骨的逐步形成。结论ur调查结果表明,基于3D印刷的多相脚手架的制造的分层方式是肌腱的有效策略 - 在不同阶段的有效细胞播种,软骨发生潜力和不同的基质沉积方面 - 骨界面工程。该物品的平移潜力通过使用3D印刷的多相支架并采用A具有凝胶的分层细胞播种方式。仿生界面可能具有在旋转箍箍上的肌腱到骨修复中的应用。它不仅可以是生物固定装置的替代品,而且还提供了替代损坏的休息的前体内生活贪污。

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