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塑造用于工程硬组织的胶原蛋白:迈向打印组学方法。

Shaping collagen for engineering hard tissues: Towards a printomics approach.

机构信息

Intelligent Polymer Research Institute, ARC Centre of Excellence for Electromaterials Science, AIIM Facility, Innovation Campus, University of Wollongong, NSW 2519, Australia; Commonwealth Scientific Industrial Research Organisation, Manufacturing Clayton, VIC 3168, Australia.

Department of Orthopaedics, University Medical Centre Utrecht, Utrecht University, Utrecht, the Netherlands; Regenerative Medicine Centre, Utrecht, Utrecht University, Utrecht, the Netherlands; Department of Biomedical Engineering, Faculty of Engineering, Technical University of Eindhoven, The Netherlands.

出版信息

Acta Biomater. 2021 Sep 1;131:41-61. doi: 10.1016/j.actbio.2021.06.035. Epub 2021 Jun 27.

Abstract

Hard tissue engineering has evolved over the past decades, with multiple approaches being explored and developed. Despite the rapid development and success of advanced 3D cell culture, 3D printing technologies and material developments, a gold standard approach to engineering and regenerating hard tissue substitutes such as bone, dentin and cementum, has not yet been realised. One such strategy that differs from conventional regenerative medicine approach of other tissues, is the in vitro mineralisation of collagen templates in the absence of cells. Collagen is the most abundant protein within the human body and forms the basis of all hard tissues. Once mineralised, collagen provides important support and protection to humans, for example in the case of bone tissue. Multiple in vitro fabrication strategies and mineralisation approaches have been developed and their success in facilitating mineral deposition on collagen to achieve bone-like scaffolds evaluated. Critical to the success of such fabrication and biomineralisation approaches is the collagen template, and its chemical composition, organisation, and density. The key factors that influence such properties are the collagen processing and fabrication techniques utilised to create the template, and the mineralisation strategy employed to deposit mineral on and throughout the templates. However, despite its importance, relatively little attention has been placed on these two critical factors. Here, we critically examine the processing, fabrication and mineralisation strategies that have been used to mineralise collagen templates, and offer insights and perspectives on the most promising strategies for creating mineralised collagen scaffolds. STATEMENT OF SIGNIFICANCE: In this review, we highlight the critical need to fabricate collagen templates with advanced processing techniques, in a manner that achieves biomimicry of the hierarchical collagen structure, prior to utilising in vitro mineralisation strategies. To this end, we focus on the initial collagen that is selected, the extraction techniques used and the native fibril forming potential retained to create reconstituted collagen scaffolds. This review synthesises current best practises in material sourcing, processing, mineralisation strategies and fabrication techniques, and offers insights into how these can best be exploited in future studies to successfully mineralise collagen templates.

摘要

硬组织工程在过去几十年中不断发展,探索和开发了多种方法。尽管先进的 3D 细胞培养、3D 打印技术和材料开发取得了快速发展和成功,但尚未实现工程化和再生硬组织替代物(如骨、牙本质和牙骨质)的黄金标准方法。一种与其他组织的传统再生医学方法不同的策略是在没有细胞的情况下体外矿化胶原模板。胶原是人体内最丰富的蛋白质,构成所有硬组织的基础。一旦矿化,胶原就为人体提供了重要的支撑和保护,例如在骨组织的情况下。已经开发了多种体外制造策略和矿化方法,并评估了它们在促进胶原上矿化以实现类骨支架方面的成功。这种制造和生物矿化方法的成功的关键是胶原模板及其化学成分、组织和密度。影响这些特性的关键因素是用于创建模板的胶原处理和制造技术,以及用于在模板上和整个模板中沉积矿物质的矿化策略。然而,尽管其重要性,相对较少关注这两个关键因素。在这里,我们批判性地检查了用于矿化胶原模板的处理、制造和矿化策略,并提供了有关创建矿化胶原支架的最有前途策略的见解和观点。意义陈述:在这篇综述中,我们强调了在利用体外矿化策略之前,用先进的处理技术制造具有仿生分层胶原结构的胶原模板的迫切需要。为此,我们专注于所选的初始胶原、使用的提取技术以及保留的原生纤维形成潜力,以创建重组胶原支架。这篇综述综合了当前材料来源、处理、矿化策略和制造技术的最佳实践,并提供了有关如何在未来研究中最好地利用这些策略来成功矿化胶原模板的见解。

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