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A simple, cost-effective but highly efficient system for deriving ventricular cardiomyocytes from human pluripotent stem cells

机译:一种简单,经济高效的高效系统,用于从人多能干细胞中提取心室心肌细胞

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Self-renewable human pluripotent stem cells (hPSCs) serve as a potential unlimited ex vivo source of human cardiomyocytes (CMs) for cell-based disease modeling and therapies. Although recent advances in directed differentiation protocols have enabled more efficient derivation of hPSC-derived CMs with an efficiency of ~50%-80% CMs and a final yield of ~1-20 CMs per starting undifferentiated hPSC, these protocols are often not readily transferrable across lines without first optimizing multiple parameters. Further, the resultant populations are undefined for chamber specificity or heterogeneous containing mixtures of atrial, ventricular (V), and pacemaker derivatives. Here we report a highly cost-effective and reproducibly efficient system for deriving hPSC-ventricular cardiomyocytes (VCMs) from all five human embryonic stem cell (HES2, H7, and H9) and human induced PSC (hiPSC) (reprogrammed from human adult peripheral blood CD34+ cells using nonintegrating episomal vectors) lines tested. Cardiogenic embryoid bodies could be formed by the sequential addition of BMP4, Rho kinase inhibitor, activin-A, and IWR-1. Spontaneously contracting clusters appeared as early as day 8. At day 16, up to 95% of cells were cTnT+. Of which, 93%, 94%, 100%, 92%, and 92% of cardiac derivatives from HES2, H7, H9, and two iPSC lines, respectively, were VCMs as gauged by signature ventricular action potential and ionic currents (I Na +/ICa,L +/IKr +/IKATP +); Ca2+ transients showed positive chronotropic responses to β-adrenergic stimulation. Our simple, cost-effective protocol required the least amounts of reagents and time compared with others. While the purity and percentage of PSC-VCMs were comparable to a recently published protocol, the present yield and efficiency with a final output of up to 70 hPSC-VCMs per hPSC was up to 5-fold higher and without the need of performing line-specific optimization. These differences were discussed. The results may lead to mass production of hPSC-VCMs in bioreactors.
机译:自我更新的人多能干细胞(hPSC)可以作为潜在的无限量的体外心肌细胞(CMs)体外来源,用于基于细胞的疾病建模和治疗。尽管定向分化方案的最新进展使hPSC衍生的CM的衍生效率更高,每个未分化的hPSC的转化效率约为50%-80%CM,最终产量约为1-20 CM,但这些方案通常不易转让无需先优化多个参数即可跨线运行。此外,对于心室特异性或心房,心室(V)和起搏器衍生物的异质混合物,不确定所得的总体。在这里,我们报告了一种从所有五个人类胚胎干细胞(HES2,H7和H9)和人类诱导的PSC(hiPSC)(从人类成年外周血中重新编程)衍生的hPSC心室心肌细胞(VCM)的高成本效益和可重复生产的高效系统使用非整合型附加型载体(CD34 +细胞)进行了测试。可以通过顺序添加BMP4,Rho激酶抑制剂,激活素A和IWR-1来形成心源性胚状体。自发收缩的簇最早出现在第8天。在第16天,多达95%的细胞是cTnT +。通过特征性心室动作电位和离子电流测量,来自HES2,H7,H9和两条iPSC系的心脏衍生物分别有93%,94%,100%,92%和92%是VCM。 + / ICa,L + / IKr + / IKATP +); Ca2 +瞬变对β-肾上腺素刺激表现出正的变时性反应。与其他方法相比,我们简单,经济高效的方案所需的试剂和时间最少。虽然PSC-VCM的纯度和百分比可与最近发布的方案相提并论,但目前的产量和效率最高可达每hPSC 70 hPSC-VCMs 5倍,而且无需执行生产线。具体优化。讨论了这些差异。结果可能导致在生物反应器中大量生产hPSC-VCM。

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