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首页> 外文期刊>Angiogenesis >Matrix composition regulates three-dimensional network formation by endothelial cells and mesenchymal stem cells in collagen/fibrin materials.
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Matrix composition regulates three-dimensional network formation by endothelial cells and mesenchymal stem cells in collagen/fibrin materials.

机译:基质成分调节胶原蛋白/纤维蛋白材料中内皮细胞和间充质干细胞的三维网络形成。

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Co-cultures of endothelial cells (EC) and mesenchymal stem cells (MSC) in three-dimensional (3D) protein hydrogels can be used to recapitulate aspects of vasculogenesis in vitro. MSC provide paracrine signals that stimulate EC to form vessel-like structures, which mature as the MSC transition to the role of mural cells. In this study, vessel-like network formation was studied using 3D collagen/fibrin (COL/FIB) matrices seeded with embedded EC and MSC and cultured for 7?days. The EC:MSC ratio was varied from 5:1, 3:2, 1:1, 2:3 and 1:5. The matrix composition was varied at COL/FIB compositions of 100/0 (pure COL), 60/40, 50/50, 40/60 and 0/100 (pure FIB). Vasculogenesis was markedly decreased in the highest EC:MSC ratio, relative to the other cell ratios. Network formation increased with increasing fibrin content in composite materials, although the 40/60 COL/FIB and pure fibrin materials exhibited the same degree of vasculogenesis. EC and MSC were co-localized in vessel-like structures after 7?days and total cell number increased by approximately 70%. Mechanical property measurements showed an inverse correlation between matrix stiffness and network formation. The effect of matrix stiffness was further investigated using gels made with varying total protein content and by crosslinking the matrix using the dialdehyde glyoxal. This systematic series of studies demonstrates that matrix composition regulates vasculogenesis in 3D protein hydrogels, and further suggests that this effect may be caused by matrix mechanical properties. These findings have relevance to the study of neovessel formation and the development of strategies to promote vascularization in transplanted tissues.
机译:三维(3D)蛋白水凝胶中内皮细胞(EC)和间充质干细胞(MSC)的共培养可用于概述体外血管生成的各个方面。 MSC提供旁分泌信号,刺激EC形成血管样结构,随着MSC转变成壁细胞的作用而成熟。在这项研究中,使用接种了嵌入式EC和MSC的3D胶原蛋白/纤维蛋白(COL / FIB)基质研究了血管样网络的形成,并培养了7天。 EC∶MSC的比率从5∶1、3∶2、1∶1、2∶3和1∶5变化。基质组成在100/0(纯COL),60 / 40、50 / 50、40 / 60和0/100(纯FIB)的COL / FIB组成下变化。相对于其他细胞比例,最高的EC:MSC比例显着降低了血管生成。尽管40/60 COL / FIB和纯纤维蛋白材料显示出相同程度的血管生成,但网络复合物的形成随纤维蛋白含量的增加而增加。 7天后,EC和MSC共定位在血管样结构中,总细胞数增加了约70%。力学性能测量表明,基体刚度与网络形成之间呈反比关系。使用总蛋白含量不同的凝胶和使用二醛乙二醛交联的基质进一步研究了基质刚度的影响。这一系列系统的研究表明,基质成分可调节3D蛋白水凝胶中的血管生成,并进一步表明,这种作用可能是由基质的机械性能引起的。这些发现与新血管形成的研究以及在移植组织中促进血管形成的策略的发展有关。

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