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Hydrogel crosslinking density regulates temporal contractility of human embryonic stem cell-derived cardiomyocytes in 3D cultures

机译:水凝胶的交联密度调节在3D培养人胚胎干细胞衍生的心肌细胞的收缩性颞

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摘要

Systematically tunable in vitro platforms are invaluable in gaining insight to stem cell-microenvironment interactions in three-dimensional cultures. Utilizing recombinant protein technology, we independently tune hydrogel properties to systematically isolate the effects of matrix crosslinking density on cardiomyocyte differentiation, maturation, and function. We show that contracting human embryonic stem cell-derived cardiomyocytes (hESC-CMs) remain viable within four engineered elastin-like hydrogels of varying crosslinking densities with elastic moduli ranging from 0.45 to 2.4 kPa. Cardiomyocyte phenotype and function was maintained within hESC embryoid bodies for up to 2 weeks. Interestingly, increased crosslinking density was shown to transiently suspend spontaneous contractility. While encapsulated cells began spontaneous contractions at day 1 in hydrogels of the lowest crosslinking density, onset of contraction was increasingly delayed at higher crosslinking densities up to 6 days. However, once spontaneous contraction was restored, the rate of contraction was similar within all materials (71 ± 8 beats/min). Additionally, all groups successfully responded to electrical pacing at both 1 and 2 Hz. This study demonstrates that encapsulated hESC-CMs respond to 3D matrix crosslinking density within elastin-like hydrogels and stresses the importance of investigating temporal cellular responses in 3D cultures.
机译:系统可调性的体外平台对于深入了解三维培养物中干细胞-微环境相互作用的价值无穷。利用重组蛋白技术,我们独立调整水凝胶特性,以系统隔离基质交联密度对心肌细胞分化,成熟和功能的影响。我们表明,收缩人类胚胎干细胞衍生的心肌细胞(hESC-CMs)在具有可变交联密度与弹性模量范围从0.45到2.4 kPa的四个工程弹性蛋白样水凝胶中保持活力。 hESC胚状体中的心肌细胞表型和功能可维持长达2周。有趣的是,增加的交联密度显示出暂时中止了自发收缩。当封装的细胞在交联密度最低的水凝胶中从第1天开始自发收缩时,收缩的开始在更高的交联密度下(最多6天)逐渐延迟。但是,一旦恢复自发性收缩,所有材料的收缩率都将相似(71±8次/分钟)。此外,所有组均成功响应了1 Hz和2 Hz的电起搏。这项研究表明,封装的hESC-CM对弹性蛋白样水凝胶中的3D基质交联密度有反应,并强调了研究3D培养物中时间细胞反应的重要性。

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