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Reprogramming Committed Murine Blood Cells to Induced Hematopoietic Stem Cells with Defined Factors

机译:重定型小鼠血细胞诱导的造血干细胞具有确定的因素

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Hematopoietic stem cells (HSCs) sustain blood formation throughout life and are the functional units of bone marrow transplantation. We show that transient expression of six transcription factors Run1t1, Hlf, Lmo2, Prdm5, Pbx1, and Zfp37 imparts multilineage transplantation potential onto otherwise committed lymphoid and myeloid progenitors and myeloid effector cells. Inclusion of Mycn and Meis1 and use of polycistronic viruses increase reprogramming efficacy. The reprogrammed cells, designated induced-HSCs (iHSCs), possess clonal multilineage differentiation potential, reconstitute stem/progenitor compartments, and are serially transplantable. Single-cell analysis revealed that iHSCs derived under optimal conditions exhibit a gene expression profile that is highly similar to endogenous HSCs. These findings demonstrate that expression of a set of defined factors is sufficient to activate the gene networks governing HSC functional identity in committed blood cells. Our results raise the prospect that blood cell reprogramming may be a strategy for derivation of transplantable stem cells for clinical application.
机译:造血干细胞(HSC)终生维持血液形成,是骨髓移植的功能单元。我们显示六个转录因子Run1t1,Hlf,Lmo2,Prdm5,Pbx1和Zfp37的瞬时表达赋予多谱系移植潜力到否则提交的淋巴和髓样祖细胞和髓样效应细胞上。包含Mycn和Meis1以及使用多顺反子病毒可提高重编程功效。重新编程的细胞称为诱导的HSC(iHSC),具有克隆多系分化潜能,重组茎/祖细胞室,并且可以串行移植。单细胞分析显示,在最佳条件下衍生的iHSC的基因表达谱与内源性HSC高度相似。这些发现表明,一组确定因子的表达足以激活定型血细胞中控制HSC功能同一性的基因网络。我们的结果提出了这样的前景,即血细胞重编程可能是用于临床应用的可移植干细胞的衍生策略。

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