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‘Above all do no harm’: safeguarding pluripotent stem cell therapy against iatrogenic tumorigenesis

机译:万无一失:维护多能干细胞疗法防止医源性肿瘤发生

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摘要

Human pluripotent stem cells are the foundations of regenerative medicine. However, the worst possible complication of using pluripotent stem cells in therapy could be iatrogenic cancerogenesis. Nevertheless, despite the rapid progress in the development of new techniques for induction of pluripotency and for directed differentiation, risks of cancerogenic transformation of therapeutically implanted pluripotent stem cells still persist. 'Above all, do no harm', as quoted from the Hippocratic Oath, is our ultimate creed. Therefore, the primary goal in designing any therapeutic regimes involving stem cells should be the elimination of any possibilities of their neoplasmic transformation. I review here the basic strategies that have been designed to attain this goal: sorting out undifferentiated, pluripotent stem cells with antibodies targeting surface-displayed biomarkers; sorting in differentiating cells, which express recombinant proteins as reporters; killing undifferentiated stem cells with toxic antibodies or antibody-guided toxins; eliminating undifferentiated stem cells with cytotoxic drugs; making potentially tumorigenic stem cells sensitive to pro-drugs by transformation with suicide-inducing genes; eradication of differentiation-refractive stem cells by self-triggered transgenic expression of human recombinant DNases. Every pluripotent undifferentiated stem cell poses a risk of neoplasmic transformation. Therefore, the aforementioned or other novel strategies that would safeguard against iatrogenic transformation of these stem cells should be considered for incorporation into every stem cell therapy trial.
机译:人多能干细胞是再生医学的基础。然而,在治疗中使用多能干细胞的最严重的并发症可能是医源性致癌作用。然而,尽管在诱导多能性和定向分化的新技术的开发中取得了迅速的进展,但是治疗植入的多能干细胞的致癌转化风险仍然存在。希波克拉底誓言中提到的“首先,不要伤害”是我们的最终信条。因此,设计涉及干细胞的任何治疗方案的主要目标应该是消除其赘生物转化的任何可能性。我在这里回顾了为实现该目标而设计的基本策略:用针对表面展示的生物标记物的抗体筛选出未分化的多能干细胞;在分化细胞中分选,这些细胞表达重组蛋白作为报告基因;用毒性抗体或抗体指​​导的毒素杀死未分化的干细胞;用细胞毒性药物消除未分化的干细胞;通过诱导自杀的基因转化,使潜在致癌干细胞对前药敏感;通过人类重组DNase的自触发转基因表达根除分化难治性干细胞。每个多能未分化的干细胞都具有肿瘤转化的风险。因此,应该考虑将前述或其他新颖的策略防止这些干细胞的医源性转化,并纳入每个干细胞治疗试验中。

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