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首页> 外文期刊>Frontiers in Cell and Developmental Biology >A Systemized Approach to Investigate Ca2+ Synchronization in Clusters of Human Induced Pluripotent Stem-Cell Derived Cardiomyocytes
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A Systemized Approach to Investigate Ca2+ Synchronization in Clusters of Human Induced Pluripotent Stem-Cell Derived Cardiomyocytes

机译:研究人类诱导的多能干细胞衍生心肌细胞簇中Ca2 +同步化的系统化方法。

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Induced pluripotent stem cell-derived cardiomyocytes (IPS-CM) are considered by many to be the cornerstone of future approaches to repair the diseased heart. However, current methods for producing IPS-CM typically yield highly variable populations with low batch-to-batch reproducibility. The underlying reasons for this are not fully understood. Here we report on a systematized approach to investigate the effect of maturation in embryoid bodies (EB) versus ‘on plate’ culture on spontaneous activity and regional Ca2+ synchronization in IPS-CM clusters. A detailed analysis of the temporal and spatial organization of Ca2+ spikes in IPS-CM clusters revealed that the disaggregation of EBs between 0.5 and 2 weeks produced IPS-CM characterized by spontaneous beating and high levels of regional Ca2+ synchronization. These phenomena were typically absent in IPS-CM obtained from older EBs (> 2 weeks). The maintenance of all spontaneously active IPS-CM clusters under ‘on plate’ culture conditions promoted the progressive reduction in regional Ca2+ synchronization and the loss of spontaneous Ca2+ spiking. Raising the extracellular [Ca2+] surrounding these quiescent IPS-CM clusters from approximately 0.4 to 1.8 mM unmasked discrete behaviours typified by either a) long-lasting Ca2+ elevation that returned to baseline or b) persistent, large-amplitude Ca2+ oscillations around an increased cytoplasmic [Ca2+]. The different responses of IPS-CM to elevated extracellular [Ca2+] could be traced back to their routes of derivation. The data point to the possibility of predictably influencing IPS-CM phenotype and response to external activation via defined interventions at early stages in their maturation.
机译:诱导多能干细胞衍生的心肌细胞(IPS-CM)被许多人认为是修复患病心脏的未来方法的基石。但是,当前生产IPS-CM的方法通常会产生高度可变的种群,并且批次间的可重复性较低。根本原因尚不完全清楚。在这里,我们报告了一种系统化的方法,以研究拟胚体(EB)与“平板”培养对IPS-CM集群中自发活动和区域Ca2 +同步化的影响。对IPS-CM簇中Ca2 +峰值的时间和空间组织的详细分析显示,在0.5和2周之间EB的分解产生了IPS-CM,其特征是自发跳动和区域Ca2 +高度同步。从较旧的EB(> 2周)获得的IPS-CM中通常不存在这些现象。在“平板”培养条件下维持所有自发活跃的IPS-CM簇促进了区域Ca2 +同步性的逐步降低和自发Ca2 +尖峰的丧失。将这些静态IPS-CM簇周围的细胞外[Ca2 +]从大约0.4 mM提高到1.8 mM,从而掩盖了离散的行为,其特征是a)持久的Ca2 +升高返回基线,或者b)胞质周围不断出现持续的大幅度Ca2 +振荡[Ca2 +]。 IPS-CM对升高的细胞外[Ca2 +]的不同反应可以追溯到它们的衍生途径。数据表明,在成熟过程的早期阶段,通过定义的干预措施可以预测地影响IPS-CM表型和对外部激活的反应。

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