首页> 外文期刊>Tissue engineering, Part A >Paracrine effects influenced by cell culture medium and consequences on microvessel-like structures in cocultures of mesenchymal stem cells and outgrowth endothelial cells.
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Paracrine effects influenced by cell culture medium and consequences on microvessel-like structures in cocultures of mesenchymal stem cells and outgrowth endothelial cells.

机译:细胞培养基受细胞培养基影响的帕拉卡碱作用及其在间充质干细胞的共培养物中微血管样结构和产卵内皮细胞的后果。

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摘要

Mesenchymal stem cells (MSC) from bone marrow and outgrowth endothelial cells (OEC) from peripheral blood are considered as attractive cell types for applications in regenerative medicine aiming to build up complex vascularized tissue-engineered constructs. MSC provide several advantages such as the potential to differentiate to osteoblasts and to support the neovascularization process by release of proangiogenic factors. On the other hand, the neovascularization process can be actively supported by OEC forming perfused vascular structures after co-implantation with other cell types. In this study the formation of angiogenic structures in vitro was investigated in cocultures of MSC and OEC, cultured either in the medium for osteogenic differentiation of MSC (ODM) or in the medium for OEC cultivation endothelial cell growth medium-2 (EGM2 Bullet Kit). After 2 weeks, cocultures in EGM2 formed more microvessel-like structures compared to cocultures in ODM as demonstrated by immunofluorescence staining for the endothelial marker CD31. Increased expression of CD31 and CD146 in quantitative real-time polymerase chain reaction as well as a higher percentage of CD31- and CD146-positive cells in flow cytometry indicated a beneficial influence of EGM2 on endothelial cell growth and function. In addition, the improved formation of vascular structures in EGM2 correlates with higher levels of the proangiogenic factor vascular endothelial growth factor and platelet-derived growth factor in the supernatant of cocultures as well as in monocultures of MSC when cultivated in EGM-2. Nevertheless, ODM was more suitable for the differentiation of MSC to osteoblastic lineages in the cocultures, whereas EGM2 favored factors involved in vessel stabilization by pericytes. In conclusion, this study highlights the importance of medium components for cell interaction triggering the formation of angiogenic structures.
机译:来自骨髓的间充质干细胞(MSC)来自外周血的骨髓和外周上皮细胞(OEC)被认为是可吸引的细胞类型,用于旨在积聚复合血管化组织工程构建体的再生药物。 MSC提供了几种优点,例如将与成骨细胞分化的可能性,并通过释放常规因子来支持新生血管形成过程。另一方面,可以在与其他细胞类型共植入后形成灌注血管结构的OEC形成新生血管化过程。在该研究中,在MSC和OEC的培养物中研究了体外血管生成结构的形成,在培养基中培养MSC(ODM)或在培养内皮细胞生长培养基-2(EGM2子弹试剂盒)中的培养基中。 2周后,与通过用于内皮标记CD31的免疫荧光染色证明,EGM2中的共gM2中的共gULLULE形成更多的微血管样结构。在定量实时聚合酶链反应中增加CD31和CD146的表达以及流式细胞术中的CD31和CD146阳性细胞的较高百分比表明EGM2对内皮细胞生长和功能的有益影响。此外,EGM2中的血管结构的改善形成与培养物上清液中的血管内皮内皮生长因子和血小板衍生的生长因子相关,以及在EGM-2中培养时的MSC的单篇文献中。然而,ODM更适合于将MSC的分化为植物细胞中的骨细胞谱系,而EGM2有利于血管血管稳定的因素。总之,该研究突出了介质组分对细胞相互作用引发血管生成结构的形成的重要性。

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