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利用肌成纤维细胞构建基于纤维蛋白的组织工程构建体,并施加约束和应变以诱导细胞和胶原蛋白重组。

Engineering fibrin-based tissue constructs from myofibroblasts and application of constraints and strain to induce cell and collagen reorganization.

作者信息

de Jonge Nicky, Baaijens Frank P T, Bouten Carlijn V C

机构信息

Department of Biomedical Engineering, Eindhoven University of Technology.

出版信息

J Vis Exp. 2013 Oct 28(80):e51009. doi: 10.3791/51009.

Abstract

Collagen content and organization in developing collagenous tissues can be influenced by local tissue strains and tissue constraint. Tissue engineers aim to use these principles to create tissues with predefined collagen architectures. A full understanding of the exact underlying processes of collagen remodeling to control the final tissue architecture, however, is lacking. In particular, little is known about the (re)orientation of collagen fibers in response to changes in tissue mechanical loading conditions. We developed an in vitro model system, consisting of biaxially-constrained myofibroblast-seeded fibrin constructs, to further elucidate collagen (re)orientation in response to i) reverting biaxial to uniaxial static loading conditions and ii) cyclic uniaxial loading of the biaxially-constrained constructs before and after a change in loading direction, with use of the Flexcell FX4000T loading device. Time-lapse confocal imaging is used to visualize collagen (re)orientation in a nondestructive manner. Cell and collagen organization in the constructs can be visualized in real-time, and an internal reference system allows us to relocate cells and collagen structures for time-lapse analysis. Various aspects of the model system can be adjusted, like cell source or use of healthy and diseased cells. Additives can be used to further elucidate mechanisms underlying collagen remodeling, by for example adding MMPs or blocking integrins. Shape and size of the construct can be easily adapted to specific needs, resulting in a highly tunable model system to study cell and collagen (re)organization.

摘要

正在发育的胶原组织中的胶原蛋白含量和组织结构会受到局部组织应变和组织约束的影响。组织工程师旨在利用这些原理来创建具有预定义胶原结构的组织。然而,目前尚缺乏对胶原蛋白重塑的确切潜在过程的全面理解,以控制最终的组织结构。特别是,关于胶原纤维在组织机械负荷条件变化时的(重新)定向知之甚少。我们开发了一种体外模型系统,该系统由双轴约束的接种成肌纤维细胞的纤维蛋白构建体组成,以进一步阐明胶原在以下情况下的(重新)定向:i)将双轴静态负荷条件恢复为单轴静态负荷条件,以及ii)在负荷方向改变之前和之后对双轴约束构建体进行循环单轴负荷,使用Flexcell FX4000T负荷装置。延时共聚焦成像用于以非破坏性方式可视化胶原的(重新)定向。构建体中的细胞和胶原组织可以实时可视化,并且内部参考系统使我们能够重新定位细胞和胶原结构以进行延时分析。该模型系统的各个方面都可以调整,例如细胞来源或使用健康和患病细胞。添加剂可用于进一步阐明胶原蛋白重塑的潜在机制,例如通过添加基质金属蛋白酶或阻断整合素。构建体的形状和大小可以很容易地根据特定需求进行调整,从而形成一个高度可调的模型系统来研究细胞和胶原的(重新)组织化。

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