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A drug-inducible transgenic system for direct reprogramming of multiple somatic cell types.

机译:一种药物诱导的转基因系统,用于多种体细胞类型的直接重编程。

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The study of induced pluripotency is complicated by the need for infection with high-titer retroviral vectors, which results in genetically heterogeneous cell populations. We generated genetically homogeneous 'secondary' somatic cells that carry the reprogramming factors as defined doxycycline (dox)-inducible transgenes. These cells were produced by infecting fibroblasts with dox-inducible lentiviruses, reprogramming by dox addition, selecting induced pluripotent stem cells and producing chimeric mice. Cells derived from these chimeras reprogram upon dox exposure without the need for viral infection with efficiencies 25- to 50-fold greater than those observed using direct infection and drug selection for pluripotency marker reactivation. We demonstrate that (i) various induction levels of the reprogramming factors can induce pluripotency, (ii) the duration of transgene activity directly correlates with reprogramming efficiency, (iii) cells from many somatic tissues can be reprogrammed and (iv) different cell types require different induction levels. This system facilitates the characterization of reprogramming and provides a tool for genetic or chemical screens to enhance reprogramming.
机译:由于需要使用高滴度逆转录病毒载体进行感染,导致诱导多能性的研究变得复杂,这导致了遗传上异质的细胞群体。我们产生了遗传上均质的“次级”体细胞,这些细胞带有作为强力霉素(dox)诱导型转基因的重编程因子。这些细胞是通过用可诱导Dox的慢病毒感染成纤维细胞,通过添加Dox进行重编程,选择诱导的多能干细胞并产生嵌合小鼠而产生的。来自这些嵌合体的细胞在暴露于dox时会重新编程,而不需要病毒感染,其效率比使用直接感染和选择药物进行多能性标记物激活所观察到的效率高25至50倍。我们证明(i)重编程因子的各种诱导水平可以诱导多能性,(ii)转基因活性的持续时间与重编程效率直接相关,(iii)来自许多体细胞组织的细胞可以被重编程,并且(iv)需要不同的细胞类型不同的感应水平。该系统有助于重新编程的特性,并为遗传或化学筛选提供工具以增强重新编程。

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