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胶原低聚物调节三维自组装基质的物理和生物学特性。

Collagen oligomers modulate physical and biological properties of three-dimensional self-assembled matrices.

机构信息

Weldon School of Biomedical Engineering, College of Engineering, Purdue University, West Lafayette, IN 47907, USA.

出版信息

Biopolymers. 2011 Feb;95(2):77-93. doi: 10.1002/bip.21537. Epub 2010 Aug 24.

Abstract

Elucidation of mechanisms underlying collagen fibril assembly and matrix-induced guidance of cell fate will contribute to the design and expanded use of this biopolymer for research and clinical applications. Here, we define how Type I collagen oligomers affect in-vitro polymerization kinetics as well as fibril microstructure and mechanical properties of formed matrices. Monomers and oligomers were fractionated from acid-solubilized pig skin collagen and used to generate formulations varying in monomer/oligomer content or average polymer molecular weight (AMW). Polymerization half-times decreased with increasing collagen AMW and closely paralleled lag times, indicating that oligomers effectively served as nucleation sites. Furthermore, increasing AMW yielded matrices with increased interfibril branching and had no correlative effect on fibril density or diameter. These microstructure changes increased the stiffness of matrices as evidenced by increases in both shear storage and compressive moduli. Finally, the biological relevance of modulating collagen AMW was evidenced by the ability of cultured endothelial colony forming cells to sense associated changes in matrix physical properties and alter vacuole and capillary-like network formation. This work documents the importance of oligomers as another physiologically-relevant design parameter for development and standardization of polymerizable collagen formulations to be used for cell culture, regenerative medicine, and engineered tissue applications.

摘要

阐明胶原蛋白纤维组装的机制以及基质对细胞命运的引导作用,将有助于设计和扩大这种生物聚合物在研究和临床应用中的使用。在这里,我们定义了 I 型胶原蛋白低聚物如何影响体外聚合动力学以及形成的基质的纤维微观结构和机械性能。从酸溶性猪皮胶原中分离出单体和低聚物,并用于生成单体/低聚物含量或平均聚合物分子量 (AMW) 变化的配方。聚合半衰期随胶原 AMW 的增加而减小,并且与滞后时间密切平行,表明低聚物有效地充当了成核位点。此外,增加 AMW 会导致纤维间分支增加,并且对纤维密度或直径没有相关性影响。这些微观结构变化增加了基质的刚度,表现为剪切储能和压缩模量的增加。最后,通过培养的血管内皮集落形成细胞感知基质物理性质的相关变化并改变空泡和类似毛细血管的网络形成,证明了调节胶原 AMW 的生物学相关性。这项工作证明了低聚物作为可聚合胶原配方开发和标准化的另一个生理相关设计参数的重要性,可用于细胞培养、再生医学和工程组织应用。

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