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抗胶原酶胶原蛋白的开发及其与成人人类真皮成纤维细胞的相互作用。

Development of collagenase-resistant collagen and its interaction with adult human dermal fibroblasts.

作者信息

Goo Hyun Chul, Hwang Yu Shik, Choi Yon Rak, Cho Hyun Nam, Suh Hwal

机构信息

Department of Medical Engineering, Yonsei University College of Medicine, 134 Shinchon-dong, Seodaemun-ku, Seoul, South Korea.

出版信息

Biomaterials. 2003 Dec;24(28):5099-113. doi: 10.1016/s0142-9612(03)00431-9.

DOI:10.1016/s0142-9612(03)00431-9
PMID:14568426
Abstract

Collagen is regarded as one of the most useful biomaterials. The excellent biocompatibility and safety due to its biological characteristics, such as biodegradability and weak antigenecity, made collagen the primary source in biomedical application. Collagen has been widely used in the crosslinked form to extend the durability of collagen. The chemical treatment influences the structural integrity of collagen molecule resulting in the loss of triple helical characteristic. The structural characteristic of collagen is importantly related to its biological function for the interaction with cell. In this study, structural stability of collagen was enhanced thought EGCG treatment, resulting in high resistance against degradation by bacterial collagenase and MMP-1, which is confirmed by collagen zymography. The triple helical structure of EGCG-treated collagen could be maintained at 37 degrees C in comparison with collagen, which confirmed by CD spectra analysis, and EGCG-treated collagen showed high free-radical scavenging activity. Also, with fibroblasts culture on EGCG-treated collagen, the structural stability of EGCG-treated collagen provided a favorable support for cell function in cell adhesion and actin filament expression. These observations underscore the need for native, triple helical collagen conformation as a prerequisite for integrin-mediated cell adhesion and functions. According to this experiment, EGCG-treated collagen assumes to provide a practical benefit to resist the degradation by collagenase retaining its structural characteristic, and can be a suitable biomaterial for biomedical application.

摘要

胶原蛋白被视为最有用的生物材料之一。由于其生物特性,如生物可降解性和弱抗原性,使其具有出色的生物相容性和安全性,这使得胶原蛋白成为生物医学应用的主要来源。胶原蛋白已被广泛用于交联形式以延长其耐久性。化学处理会影响胶原蛋白分子的结构完整性,导致三螺旋特征丧失。胶原蛋白的结构特征与其与细胞相互作用的生物学功能密切相关。在本研究中,通过表没食子儿茶素没食子酸酯(EGCG)处理增强了胶原蛋白的结构稳定性,从而使其对细菌胶原酶和基质金属蛋白酶-1的降解具有高抗性,这通过胶原酶谱法得到证实。与胶原蛋白相比,经EGCG处理的胶原蛋白的三螺旋结构在37℃时可以维持,这通过圆二色光谱分析得到证实,并且经EGCG处理的胶原蛋白表现出高自由基清除活性。此外,在经EGCG处理的胶原蛋白上培养成纤维细胞时,经EGCG处理的胶原蛋白的结构稳定性为细胞黏附和肌动蛋白丝表达中的细胞功能提供了有利支持。这些观察结果强调了天然三螺旋胶原蛋白构象作为整合素介导的细胞黏附和功能的先决条件的必要性。根据本实验,经EGCG处理的胶原蛋白假定能提供实际益处,以抵抗胶原酶的降解并保持其结构特征,并且可以成为生物医学应用的合适生物材料。

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