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具有支撑关节固定装置的仿生自组织软骨生物打印

Bioprinting of biomimetic self-organised cartilage with a supporting joint fixation device.

作者信息

Burdis Ross, Chariyev-Prinz Farhad, Kelly Daniel J

机构信息

Trinity Centre for Biomedical Engineering, Trinity Biomedical Sciences Institute, Trinity College Dublin, Dublin, Ireland.

Department of Mechanical, Manufacturing and Biomedical Engineering, School of Engineering, Trinity College Dublin, Dublin, Ireland.

出版信息

Biofabrication. 2021 Nov 25;14(1). doi: 10.1088/1758-5090/ac36be.

Abstract

Despite sustained efforts, engineering truly biomimetic articular cartilage (AC) via traditional top-down approaches remains challenging. Emerging biofabrication strategies, from 3D bioprinting to scaffold-free approaches that leverage principles of cellular self-organisation, are generating significant interest in the field of cartilage tissue engineering as a means of developing biomimetic tissue analoguesAlthough such strategies have advanced the quality of engineered cartilage, recapitulation of many key structural features of native AC, in particular a collagen network mimicking the tissue's 'Benninghoff arcade', remains elusive. Additionally, a complete solution to fixating engineered cartilageswithin damaged synovial joints has yet to be identified. This study sought to address both of these key challenges by engineering biomimetic AC within a device designed to anchor the tissue within a synovial joint defect. We first designed and fabricated a fixation device capable of anchoring engineered cartilage into the subchondral bone. Next, we developed a strategy for inkjet printing porcine mesenchymal stem/stromal cells (MSCs) into this supporting fixation device, which was also designed to provide instructive cues to direct the self-organisation of MSC condensations towards a stratified engineered AC. We found that a higher starting cell-density supported the development of a more zonally defined collagen network within the engineered tissue. Dynamic culture was implemented to further enhance the quality of this engineered tissue, resulting in an approximate 3 fold increase in glycosaminoglycan and collagen accumulation. Ultimately this strategy supported the development of AC that exhibited near-native levels of glycosaminoglycan accumulation (>5% WW), as well as a biomimetic collagen network organisation with a perpendicular to a parallel fibre arrangement (relative to the tissue surface) from the deep to superficial zones via arcading fibres within the middle zone of the engineered tissue. Collectively, this work demonstrates the successful convergence of novel biofabrication methods, bioprinting strategies and culture regimes to engineer a hybrid implant suited to resurfacing AC defects.

摘要

尽管付出了持续努力,但通过传统的自上而下方法构建真正的仿生关节软骨(AC)仍然具有挑战性。新兴的生物制造策略,从3D生物打印到利用细胞自组织原理的无支架方法,作为开发仿生组织类似物的手段,正在软骨组织工程领域引起极大关注。尽管这些策略提高了工程化软骨的质量,但原生AC的许多关键结构特征,特别是模仿组织“本宁霍夫弓”的胶原网络,仍难以重现。此外,尚未找到将工程化软骨固定在受损滑膜关节内的完整解决方案。本研究旨在通过在设计用于将组织锚定在滑膜关节缺损内的装置中构建仿生AC来解决这两个关键挑战。我们首先设计并制造了一种能够将工程化软骨锚定到软骨下骨的固定装置。接下来,我们开发了一种将猪间充质干/基质细胞(MSCs)喷墨打印到这种支持性固定装置中的策略,该装置还旨在提供指导性线索,引导MSC凝聚物自组织形成分层的工程化AC。我们发现较高的起始细胞密度有助于在工程化组织内形成更具区域定义的胶原网络。实施动态培养以进一步提高这种工程化组织的质量,导致糖胺聚糖和胶原积累增加约3倍。最终,该策略支持了AC的发育,其糖胺聚糖积累水平接近天然水平(>5%湿重),并且具有仿生胶原网络组织,从工程化组织中间区域的弧形纤维开始,从深部到浅部区域呈现垂直于平行纤维排列(相对于组织表面)。总的来说,这项工作证明了新型生物制造方法、生物打印策略和培养方案的成功结合,以构建适合修复AC缺损的混合植入物。

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