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A defined synthetic substrate for serum-free culture of human stem cell derived cardiomyocytes with improved functional maturity identified using combinatorial materials microarrays

机译:使用组合材料微阵列鉴定的用于人干细胞衍生的心肌细胞无血清培养且功能成熟度提高的确定的合成底物

摘要

Cardiomyocytes from human stem cells have applications in regenerative medicine and can provide models for heart disease and toxicity screening. Soluble components of the culture system such as growth factors within serum and insoluble components such as the substrate on which cells adhere to are important variables controlling the biological activity of cells. Using a combinatorial materials approach we develop a synthetic, chemically defined cellular niche for the support of functional cardiomyocytes derived from human embryonic stem cells (hESC-CMs) in a serum-free fully defined culture system. Almost 700 polymers were synthesized and evaluated for their utility as growth substrates. From this group, 20 polymers were identified that supported cardiomyocyte adhesion and spreading. The most promising 3 polymers were scaled up for extended culture of hESC-CMs for 15 days and were characterized using patch clamp electrophysiology and myofibril analysis to find that functional and structural phenotype was maintained on these synthetic substrates without the need for coating with extracellular matrix protein. In addition, we found that hESC-CMs cultured on a co-polymer of isobornyl methacrylate and tert-butylamino-ethyl methacrylate exhibited significantly longer sarcomeres relative to gelatin control. The potential utility of increased structural integrity was demonstrated in an in vitro toxicity assay that found an increase in detection sensitivity of myofibril disruption by the anti-cancer drug doxorubicin at a concentration of 0.05 μM in cardiomyocytes cultured on the co-polymer compared to 0.5 μM on gelatin. The chemical moieties identified in this large-scale screen provide chemically defined conditions for the culture and manipulation of hESC-CMs, as well as a framework for the rational design of superior biomaterials.
机译:来自人类干细胞的心肌细胞已应用于再生医学,可为心脏病和毒性筛查提供模型。培养系统的可溶性成分(例如血清中的生长因子)和不溶成分(例如细胞粘附于其上的底物)是控制细胞生物学活性的重要变量。使用组合材料方法,我们开发了合成的,化学定义的细胞生境,以在无血清的完全定义的培养系统中支持源自人胚胎干细胞(hESC-CMs)的功能性心肌细胞。合成了近700种聚合物,并评估了它们作为生长底物的用途。从这一组中,鉴定出支持心肌细胞粘附和扩散的20种聚合物。将最有前途的3种聚合物按比例放大以用于hESC-CM的延长培养15天,并使用膜片钳电生理学和肌原纤维分析对其进行表征,以发现在这些合成底物上可以保持功能和结构表型,而无需用细胞外基质蛋白包被。另外,我们发现,在异丁烯酸异冰片酯和异丁烯酸叔丁氨基乙酯的共聚物上培养的hESC-CMs相对于明胶对照具有更长的肉瘤。在体外毒性试验中证明了提高结构完整性的潜在效用,该试验发现,在共聚物上培养的心肌细胞中浓度为0.05μM的抗癌药阿霉素对肌原纤维干扰的检测敏感性提高了,而0.5μM在明胶上。在大规模筛选中鉴定出的化学部分为hESC-CM的培养和操作提供了化学定义的条件,并为合理设计优质生物材料提供了框架。

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