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Method for selective ablation of undifferentiated human pluripotent stem cell populations for cell-based therapies

机译:选择性消融的方法用于未分化的人多能干细胞群用于细胞基疗法

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摘要

Human pluripotent stem cells (PSCs), which are composed of embryonic stem cells (ESCs) and induced pluripotent stem cells (iPSCs), provide an opportunity to advance cardiac cell therapy–based clinical trials. However, an important hurdle that must be overcome is the risk of teratoma formation after cell transplantation due to the proliferative capacity of residual undifferentiated PSCs in differentiation batches. To tackle this problem, we propose the use of a minimal noncardiotoxic doxorubicin dose as a purifying agent to selectively target rapidly proliferating stem cells for cell death, which will provide a purer population of terminally differentiated cardiomyocytes before cell transplantation. In this study, we determined an appropriate in vitro doxorubicin dose that (a) eliminates residual undifferentiated stem cells before cell injection to prevent teratoma formation after cell transplantation and (b) does not cause cardiotoxicity in ESC-derived cardiomyocytes (CMs) as demonstrated through contractility analysis, electrophysiology, topoisomerase activity assay, and quantification of reactive oxygen species generation. This study establishes a potentially novel method for tumorigenic-free cell therapy studies aimed at clinical applications of cardiac cell transplantation.
机译:由胚胎干细胞(ESC)和诱导多能干细胞(IPSC)组成的人多能干细胞(PSC)提供了推进基于心细胞治疗的临床试验的机会。然而,由于分化批次中残留未分化的PSC的增殖能力,必须克服必须克服的重要障碍是细胞移植后形成畸胎瘤形成的风险。为了解决这个问题,我们建议使用最小的非顽童多柔比星剂量作为净化剂,以选择性地靶向用于细胞死亡的快速增殖的干细胞,这将在细胞移植前提供液体分化的心肌细胞的纯群。在这项研究中,我们确定了适当的体外多柔比星剂量,(a)在细胞注射之前消除残留的未分化干细胞,以防止细胞移植后的畸胎瘤形成,并且(b)在ESC衍生的心肌细胞(CMS)中不会导致血管毒性,如通过收缩性分析,电生理学,拓扑异构酶活性测定和反应性氧物种的定量。本研究规划了旨在临床应用心脏细胞移植的无致致瘤性细胞治疗研究的潜在新方法。

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