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通过内皮样间充质基质细胞在可注射葡聚糖-透明质酸水凝胶中促进血管生成和功能血管化。

Boosting angiogenesis and functional vascularization in injectable dextran-hyaluronic acid hydrogels by endothelial-like mesenchymal stromal cells.

机构信息

1 Department of Tissue Regeneration, MIRA Institute for Biomedical Technology and Technical Medicine, University of Twente , Enschede, the Netherlands .

出版信息

Tissue Eng Part A. 2014 Feb;20(3-4):819-29. doi: 10.1089/ten.TEA.2013.0280. Epub 2013 Nov 12.

DOI:10.1089/ten.TEA.2013.0280
PMID:24070233
Abstract

Angiogenesis and neovascularization are fundamental for the success of clinically relevant-sized tissue-engineered (TE) constructs. The next generation of TE constructs relies on providing instructive materials combined with the delivery of angiogenic growth factors and cells to avoid tissue ischemia. However, the majority of materials and cell types screened so far show limited clinical relevance, either due to insufficient number of cells or due to the use of animal-derived matrixes. Here, we investigated whether endothelial-like cells derived from mesenchymal stromal cells (EL-MSCs) can be used for vascular TE in combination with injectable dextran-hyaluronic acid (Dex-g-HA) hydrogels. These hydrogels can be easily modified, as demonstrated by the incorporation of vascular endothelial growth factor (VEGF). We examined in vitro the reciprocal influences between cells and matrix. Dex-g-HA enabled higher EL-MSC metabolic rates associated with optimal cell sprouting in vitro compared to human umbilical vein endothelial cells. In vivo evaluation demonstrated the absence of an acute inflammatory response, and EL-MSCs incorporated within Dex-g-HA formed a functional vascular network integrated with the host vascular system. This work demonstrates that Dex-g-HA is an efficient delivery method of VEGF to induce angiogenesis. Additionally, functional neovascularization can be achieved in vitro and in vivo by the combination of Dex-g-HA with EL-MSC.

摘要

血管生成和新血管形成对于临床相关大小的组织工程(TE)构建体的成功至关重要。下一代 TE 构建体依赖于提供有指导意义的材料,结合血管生成生长因子和细胞的递送,以避免组织缺血。然而,迄今为止筛选出的大多数材料和细胞类型显示出有限的临床相关性,要么是因为细胞数量不足,要么是因为使用了动物来源的基质。在这里,我们研究了是否可以将间充质基质细胞(EL-MSC)衍生的内皮样细胞与可注射的葡聚糖-透明质酸(Dex-g-HA)水凝胶结合用于血管 TE。这些水凝胶可以很容易地进行修饰,如通过加入血管内皮生长因子(VEGF)来证明。我们在体外检查了细胞和基质之间的相互影响。与体外人脐静脉内皮细胞相比,Dex-g-HA 使 EL-MSC 的代谢率更高,细胞发芽更加优化。体内评估表明不存在急性炎症反应,并且 Dex-g-HA 内的 EL-MSC 形成了与宿主血管系统集成的功能性血管网络。这项工作表明 Dex-g-HA 是一种有效的 VEGF 递送方法,可诱导血管生成。此外,通过 Dex-g-HA 与 EL-MSC 的组合可以在体外和体内实现功能性新血管形成。

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