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通过共价结合血管内皮生长因子(VEGF)增强胶原蛋白基质中的血管生成。

Enhancing angiogenesis in collagen matrices by covalent incorporation of VEGF.

作者信息

Koch S, Yao Ch, Grieb G, Prével P, Noah E M, Steffens G C M

机构信息

Institute of Biochemistry, University Hospital, Aachen, Germany.

出版信息

J Mater Sci Mater Med. 2006 Aug;17(8):735-41. doi: 10.1007/s10856-006-9684-x.

Abstract

Since the survival of ingrowing cells in biomaterials for regenerative processes largely depends on the supply of nutrients and oxygen, angiogenesis plays an important role in the development of new materials for tissue engineering. In this study we investigated the possibility of enhancing the angiogenic properties of collagen matrices by covalent incorporation of the vascular endothelial growth factor (VEGF). In a previous paper we already reported the use of homo- and heterobifunctional cross-linking agents for modifying collagen matrices [1]. In the present work the angiogenic growth factor was linked to the collagen with the homobifunctional cross-linker disuccinimidyldisuccinatepolyethyleneglycol (SS-PEG-SS) in a two step procedure. The efficiency of the first reaction step-the reaction of SS-PEG-SS with VEGF--was evaluated by western blot analysis. After 10 minutes virtually all of the dimeric molecules VEGF were on average modified by conjugation with 1 cross-linking molecule. The biological activity of the conjugate was investigated by exposing endothelial cells to non-modified VEGF and to VEGF conjugated to the cross-linker. The conjugation only had a limited effect on the mitogenic activity of VEGF. We therefore applied the cross-linking reaction to the VEGF-collagen system. In a first approach the changes were evaluated by the in vitro exposure of HUVECs to non-modified matrices, to matrices in which the VEGF was simply admixed and to matrices in which the VEGF was covalently incorporated. The angiogenic properties were evaluated in vivo with the chorioallantois membrane model. In this assay the chorioallantois membrane of the chicken embryo was exposed to the same set of matrices. The covalent incorporation of VEGF has a small but significant effect both on the formation of microvessels in the chorioallantois membrane and the tissue ingrowth into the implant. The covalent incorporation of angiogenic growth factors may thus be considered as a promising approach for enhancing the angiogenic capabilities of collagen matrices. Also the cross-linking with the homobifunctional cross-linking agent has a positive effect on the angiogenic potential of the collagen matrices.

摘要

由于再生过程中生物材料内植入细胞的存活很大程度上取决于营养物质和氧气的供应,血管生成在组织工程新材料的开发中起着重要作用。在本研究中,我们研究了通过共价结合血管内皮生长因子(VEGF)来增强胶原基质血管生成特性的可能性。在之前的一篇论文中,我们已经报道了使用同双功能和异双功能交联剂来修饰胶原基质[1]。在本工作中,血管生成生长因子通过同双功能交联剂二琥珀酰亚胺基二琥珀酸聚乙二醇(SS-PEG-SS)以两步法与胶原相连。通过蛋白质印迹分析评估第一步反应——SS-PEG-SS与VEGF的反应——的效率。10分钟后,实际上所有的二聚体分子VEGF平均通过与1个交联分子结合而被修饰。通过将内皮细胞暴露于未修饰的VEGF和与交联剂结合的VEGF来研究偶联物的生物活性。这种偶联对VEGF的促有丝分裂活性只有有限的影响。因此,我们将交联反应应用于VEGF-胶原系统。在第一种方法中,通过将人脐静脉内皮细胞(HUVECs)体外暴露于未修饰的基质、VEGF简单混合的基质和VEGF共价结合的基质来评估变化。用尿囊膜模型在体内评估血管生成特性。在该试验中,鸡胚的尿囊膜暴露于同一组基质。VEGF的共价结合对尿囊膜中微血管的形成和组织向植入物内生长均有微小但显著的影响。因此,血管生成生长因子的共价结合可被视为增强胶原基质血管生成能力的一种有前景的方法。与同双功能交联剂的交联对胶原基质的血管生成潜力也有积极作用。

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