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Perivascular-like cells contribute to the stability of the vascular network of osteogenic tissue formed from cell sheet-based constructs

机译:类血管周围细胞有助于由基于细胞片的构建体形成的成骨组织的血管网络的稳定性

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摘要

In recent years several studies have been supporting the existence of a close relationship in terms of function and progeny between Mesenchymal Stem Cells (MSCs) and Pericytes. This concept has opened new perspectives for the application of MSCs in Tissue Engineering (TE), with special interest for the pre-vascularization of cell dense constructs. In this work, cell sheet technology was used to create a scaffold-free construct composed of osteogenic, endothelial and perivascular-like (CD146(+)) cells for improved in vivo vessel formation, maturation and stability. The CD146 pericyte-associated phenotype was induced from human bone marrow mesenchymal stem cells (hBMSCs) by the supplementation of standard culture medium with TGF-β1. Co-cultured cell sheets were obtained by culturing perivascular-like (CD146(+)) cells and human umbilical vein endothelial cells (HUVECs) on an hBMSCs monolayer maintained in osteogenic medium for 7 days. The perivascular-like (CD146(+)) cells and the HUVECs migrated and organized over the collagen-rich osteogenic cell sheet, suggesting the existence of cross-talk involving the co-cultured cell types. Furthermore the presence of that particular ECM produced by the osteoblastic cells was shown to be the key regulator for the singular observed organization. The osteogenic and angiogenic character of the proposed constructs was assessed in vivo. Immunohistochemistry analysis of the explants revealed the integration of HUVECs with the host vasculature as well as the osteogenic potential of the created construct, by the expression of osteocalcin. Additionally, the analysis of the diameter of human CD146 positive blood vessels showed a higher mean vessel diameter for the co-cultured cell sheet condition, reinforcing the advantage of the proposed model regarding blood vessels maturation and stability and for the in vitro pre-vascularization of TE constructs.
机译:近年来,一些研究已经支持了间充质干细胞(MSC)和周细胞之间在功能和子代方面的紧密关系。该概念为MSC在组织工程(TE)中的应用开辟了新的前景,特别关注细胞致密构建物的预血管形成。在这项工作中,细胞片技术被用于创建无支架的构建体,该构建体由成骨,内皮和血管周样(CD146(+))细胞组成,以改善体内血管的形成,成熟和稳定性。通过用标准培养基添加TGF-β1,从人骨髓间充质干细胞(hBMSC)诱导CD146周细胞相关表型。通过将血管周样(CD146(+))细胞和人脐静脉内皮细胞(HUVEC)在成骨培养基中保持的hBMSCs单层上培养7天来获得共培养的细胞片。血管周围样(CD146(+))细胞和HUVEC在富含胶原的成骨细胞片上迁移并组织,提示存在涉及共培养细胞类型的串扰。此外,由成骨细胞产生的特定ECM的存在被证明是观察到的单个组织的关键调节因子。在体内评估了所提出的构建体的成骨和血管生成特性。外植体的免疫组织化学分析显示,通过骨钙素的表达,HUVEC与宿主脉管系统整合,并产生了所构建体的成骨潜能。此外,对人CD146阳性血管直径的分析显示,对于共培养的细胞片条件,平均血管直径更高,从而增强了所提出模型在血管成熟和稳定性以及体外预血管化方面的优势。 TE构造。

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