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通过内在的纤维蛋白原 - 凝血酶成分和外在的细胞活性对三维纤维蛋白基质硬度进行调节。

Modulation of 3D fibrin matrix stiffness by intrinsic fibrinogen-thrombin compositions and by extrinsic cellular activity.

作者信息

Duong Haison, Wu Benjamin, Tawil Bill

机构信息

Department of Bioengineering, University of California, Los Angeles, CA 90095-1600, USA.

出版信息

Tissue Eng Part A. 2009 Jul;15(7):1865-76. doi: 10.1089/ten.tea.2008.0319.

Abstract

Fibrin is a substance formed through catalytic conversion of coagulation constituents: fibrinogen and thrombin. The kinetics of the two constituents determines the structural properties of the fibrin architecture. We have shown previously that changing the fibrinogen and thrombin concentrations in the final three-dimensional (3D) fibrin matrix influenced cell proliferation and differentiation. In this study, we further examined the effect of changing fibrinogen and thrombin concentrations in the absence or presence of fibroblasts on the structural modulus or stiffness of 3D fibrin matrices. We have prepared fibroblast-free and fibroblast-embedded 3D fibrin matrices of different fibrinogen and thrombin formulations, and tested the stiffness of these constructs using standard mechanical testing assays. Results showed that there was a corresponding increase in stiffness with increasing thrombin and fibrinogen concentrations; the increase was more notable with fibrinogen and to a lesser degree with thrombin. The effect of fibroblasts on the stiffness of the fibrin construct was also examined. We have observed a small increase in the stiffness of the fibroblast-incorporated fibrin construct as they proliferated and exhibited spreading morphology. To our knowledge, this is the first comprehensive report detailing the relationship between fibrinogen and thrombin concentrations, cell proliferation, and stiffness in 3D fibrin matrices. The data obtained may lead to optimally design suitable bioscaffolds where we can control both cell proliferation and structural integrity for a variety of tissue engineering applications.

摘要

纤维蛋白是通过凝血成分(纤维蛋白原和凝血酶)的催化转化而形成的一种物质。这两种成分的动力学决定了纤维蛋白结构的结构特性。我们之前已经表明,改变最终三维(3D)纤维蛋白基质中的纤维蛋白原和凝血酶浓度会影响细胞增殖和分化。在本研究中,我们进一步研究了在不存在或存在成纤维细胞的情况下,改变纤维蛋白原和凝血酶浓度对3D纤维蛋白基质的结构模量或硬度的影响。我们制备了不同纤维蛋白原和凝血酶配方的无成纤维细胞和嵌入成纤维细胞的3D纤维蛋白基质,并使用标准机械测试方法测试了这些构建体的硬度。结果表明,随着凝血酶和纤维蛋白原浓度的增加,硬度相应增加;纤维蛋白原的增加更显著,凝血酶的增加程度较小。还研究了成纤维细胞对纤维蛋白构建体硬度的影响。我们观察到,随着成纤维细胞的增殖并呈现出铺展形态,掺入成纤维细胞的纤维蛋白构建体的硬度略有增加。据我们所知,这是第一份详细阐述3D纤维蛋白基质中纤维蛋白原和凝血酶浓度、细胞增殖与硬度之间关系的综合报告。所获得的数据可能有助于优化设计合适的生物支架,在各种组织工程应用中,我们可以同时控制细胞增殖和结构完整性。

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