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首页> 外文期刊>In Vitro Cellular and Developmental Biology. Animal: Journal of the Tissues Culture Association >Novel in vitro cardiovascular constructs composed of vascular-like networks and cardiomyocytes
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Novel in vitro cardiovascular constructs composed of vascular-like networks and cardiomyocytes

机译:由血管样网络和心肌细胞组成的新型体外心血管构建体

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The interaction between different cardiac cells has shown to be important for critical biological properties including cell survival, proliferation, differentiation and function. The improvement of culture conditions with different cell types and to study their effects on cardiomyocyte viability and functionality is essential. For practical applications including general toxicity testing, drug development and tissue engineering it is important to study whether co-cultures have additional advantages over cardiomyocyte monoculture. Two multicellular in vitro cardiovascular constructs devoid of added biomaterial were developed in this study. In the first construct, neonatal rat cardiomyocytes (CM) were seeded on vascular-like network formed by human umbilical vein endothelial cells (HUVEC) and human adipose stromal cells (hASC). In the second construct, CMs were seeded on vascular-like network formed by HUVECs and human foreskin fibroblasts. The ability of these two vascular-like networks to support the viability and functionality of CMs was analyzed. Different culture media compositions were evaluated to support the development of optimal cardiovascular construct. Our results demonstrate that both vascular-like networks markedly improved CM viability and functionality. In the constructs, co-localization of CMs and vascular-like networks was seen. Multicellular constructs also allowed synchronized contractility of CMs. Serum-free medium supplemented with vascular endothelial growth factor and basic fibroblast growth factor was found to provide the most optimal conditions for cardiovascular construct as an entity. In conclusion, when combining a vascular-like network with CMs, the viability and functionality of CMs was markedly improved. The results suggest that the cardiovascular constructs developed provide a promising new tool for the assessment of toxicological and safety pharmacological effects of compounds in vitro.
机译:已显示不同心脏细胞之间的相互作用对于关键的生物学特性(包括细胞存活,增殖,分化和功能)很重要。改善不同细胞类型的培养条件并研究其对心肌细胞活力和功能的影响至关重要。对于包括一般毒性测试,药物开发和组织工程在内的实际应用,重要的是研究共培养是否比心肌单细胞培养具有更多优势。在这项研究中开发了两个没有添加生物材料的体外多细胞心血管构建体。在第一个构建体中,将新生大鼠心肌细胞(CM)播种在由人脐静脉内皮细胞(HUVEC)和人脂肪基质细胞(hASC)形成的血管样网络上。在第二个构建体中,CMs播种在HUVEC和人包皮成纤维细胞形成的血管样网络上。分析了这两个类似血管的网络支持CM的生存能力和功能的能力。评价了不同的培养基成分以支持最佳心血管构造的发展。我们的结果表明,两个类似血管的网络均显着改善了CM的生存能力和功能。在构建体中,发现了CM和类血管网络的共定位。多细胞构建体还允许CM同步收缩。发现补充了血管内皮生长因子和碱性成纤维细胞生长因子的无血清培养基可为心血管构建提供最佳条件。总之,当将类似血管的网络与CM结合使用时,CM的生存能力和功能得到了显着改善。结果表明,开发的心血管构建体为评估化合物的体外毒理学和安全药理作用提供了有希望的新工具。

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