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通过掺入控释碱性成纤维细胞生长因子微球增强三维多孔藻酸盐支架的血管化。

Enhancing the vascularization of three-dimensional porous alginate scaffolds by incorporating controlled release basic fibroblast growth factor microspheres.

作者信息

Perets Anat, Baruch Yaacov, Weisbuch Felix, Shoshany Gideon, Neufeld Gera, Cohen Smadar

机构信息

Department of Biomedical Engineering, Ben-Gurion University of the Negev, Beer Sheva, Israel.

出版信息

J Biomed Mater Res A. 2003 Jun 15;65(4):489-97. doi: 10.1002/jbm.a.10542.

DOI:10.1002/jbm.a.10542
PMID:12761840
Abstract

Site-specific delivery of angiogenic growth factors from tissue-engineered devices should provide an efficient means of stimulating localized vessel recruitment to the cell transplants and would ensure cell survival and function. In the present article, we describe the construction of a novel porous alginate scaffold that incorporates tiny poly (lactic-co-glycolic acid) microspheres capable of controlling the release of angiogenic factors, such as basic fibroblast growth factor (bFGF). The microspheres are an integral part of the solid alginate matrix, and their incorporation does not affect the scaffold porosity or pore size. In vitro, bFGF was released from the porous composite scaffolds in a controlled manner and it was biologically active as assessed by its ability to induce the proliferation of cardiac fibroblasts. The controlled delivery of bFGF from the three-dimensional scaffolds accelerated the matrix vascularization after implantation on the mesenteric membrane in rat peritoneum. The number of penetrating capillaries into the bFGF-releasing scaffolds was nearly fourfold higher than into the control scaffolds (those incorporating microspheric BSA and heparin but not bFGF). At day 10 posttransplantation, capillary density in the composite scaffolds was 45 +/- 3/mm(2) and it increased to 70 +/- 7/mm(2) by day 21. The released bFGF induced the formation of large and matured blood vessels, as judged by the massive layer of mural cells surrounding the endothelial cells. The control over bFGF delivery and localizing its effects to areas of need, may aid in the wider application of bFGF in therapeutic angiogenesis as well as in tissue engineering.

摘要

从组织工程装置中进行血管生成生长因子的位点特异性递送应提供一种有效的方法来刺激局部血管向细胞移植部位募集,并确保细胞存活和功能。在本文中,我们描述了一种新型多孔藻酸盐支架的构建,该支架包含能够控制血管生成因子(如碱性成纤维细胞生长因子,bFGF)释放的微小聚(乳酸-乙醇酸)微球。微球是固体藻酸盐基质的一个组成部分,它们的加入不会影响支架的孔隙率或孔径。在体外,bFGF以可控方式从多孔复合支架中释放出来,并且通过其诱导心脏成纤维细胞增殖的能力评估,它具有生物活性。从三维支架中可控递送bFGF加速了植入大鼠腹膜肠系膜膜后的基质血管化。进入释放bFGF支架的穿透性毛细血管数量比进入对照支架(那些包含微球牛血清白蛋白和肝素但不包含bFGF的支架)的数量高出近四倍。移植后第10天,复合支架中的毛细血管密度为45±3/mm²,到第21天增加到70±7/mm²。释放的bFGF诱导形成大而成熟的血管,这可通过围绕内皮细胞的大量壁细胞层来判断。对bFGF递送的控制及其作用定位于需要的区域,可能有助于bFGF在治疗性血管生成以及组织工程中的更广泛应用。

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