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通过将人碱性成纤维细胞生长因子(bFGF)靶向纤维蛋白来改善新生血管形成和伤口修复。

Improved neovascularization and wound repair by targeting human basic fibroblast growth factor (bFGF) to fibrin.

作者信息

Zhao Wenxue, Han Qianqian, Lin Hang, Gao Yuan, Sun Wenjie, Zhao Yannan, Wang Bin, Chen Bing, Xiao Zhifeng, Dai Jianwu

机构信息

Key Laboratory of Molecular Developmental Biology, Institute of Genetics and Developmental Biology, Chinese Academy of Sciences, Beijing, China.

出版信息

J Mol Med (Berl). 2008 Oct;86(10):1127-38. doi: 10.1007/s00109-008-0372-9. Epub 2008 Jun 11.

Abstract

Targeted therapy is a new generation of therapeutics, where two critical factors are involved. One is the particular molecular target, and the other is the specific target-binding drug. In this work, the fibrin, a main component of plasma clot at wound sites, was used as the target for human bFGF, aiming to improve therapeutic neovascularization and wound repair. To endow bFGF with fibrin-targeting ability, a fibrin-binding peptide Kringle1 (K1), derived from human plasminogen, was fused to human bFGF. The recombinant K1bFGF showed high fibrin and plasma-clot-binding ability. When applied to the wound sites with plasma clots, K1bFGF induced robust neovascularization and improved wound healing. To extend the application of K1bFGF to other cases where no plasma clots exist, we developed a fibrin-scaffold/K1bFGF system. This system could induce localized neovascularization by delivery of K1bFGF in a sustained and site-targeting manner, and provide a microenvironment promoting cell growth and tissue regeneration. In summary, we successfully used the pathologic environment fibrin clot as the target for bFGF, and based on which bFGF was designed into a targeting agent by introduction of a fibrin-binding peptide. This provides a potential approach to improve therapeutic neovascularization and wound repair.

摘要

靶向治疗是新一代的治疗方法,涉及两个关键因素。一个是特定的分子靶点,另一个是与靶点特异性结合的药物。在本研究中,伤口部位血浆凝块的主要成分纤维蛋白被用作人碱性成纤维细胞生长因子(bFGF)的靶点,旨在改善治疗性血管新生和伤口修复。为了赋予bFGF纤维蛋白靶向能力,将源自人纤溶酶原的纤维蛋白结合肽kringle1(K1)与人bFGF融合。重组K1bFGF显示出高纤维蛋白和血浆凝块结合能力。当应用于有血浆凝块的伤口部位时,K1bFGF可诱导强烈的血管新生并促进伤口愈合。为了将K1bFGF的应用扩展到不存在血浆凝块的其他情况,我们开发了一种纤维蛋白支架/K1bFGF系统。该系统可以通过持续且靶向定位的方式递送K1bFGF来诱导局部血管新生,并提供促进细胞生长和组织再生的微环境。总之,我们成功地将病理环境中的纤维蛋白凝块用作bFGF的靶点,并在此基础上通过引入纤维蛋白结合肽将bFGF设计成一种靶向剂。这为改善治疗性血管新生和伤口修复提供了一种潜在的方法。

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