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Direct reprogramming of mouse fibroblasts to neural stem cells by small molecules

机译:通过小分子直接将小鼠成纤维细胞重编程为神经干细胞

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摘要

Although it is possible to generate neural stem cells (NSC) from somatic cells by reprogramming technologies with transcription factors, clinical utilization of patient-specific NSC for the treatment of human diseases remains elusive. The risk hurdles are associated with viral transduction vectors induced mutagenesis, tumor formation from undifferentiated stem cells, and transcription factors-induced genomic instability. Here we describe a viral vector-free and more efficient method to induce mouse fibroblasts into NSC using small molecules. The small molecule-induced neural stem (SMINS) cells closely resemble NSC in morphology, gene expression patterns, self-renewal, excitability, and multipotency. Furthermore, the SMINS cells are able to differentiate into astrocytes, functional neurons, and oligodendrocytes in vitro and in vivo.Thus, we have established a novelway to efficiently induce neural stemcells (iNSC) fromfibroblasts using only smallmolecules without altering the genome. Such chemical induction removes the risks associated with current techniques such as the use of viral vectors or the induction of oncogenic factors. This technique may, therefore, enable NSC to be utilized in various applications within clinical medicine.
机译:尽管可以通过利用转录因子进行重编程技术从体细胞生成神经干细胞(NSC),但是患者特异性NSC在人类疾病治疗中的临床应用仍然难以捉摸。风险障碍与病毒转导载体引起的诱变,未分化干细胞形成的肿瘤以及转录因子引起的基因组不稳定有关。在这里,我们描述了一种无病毒载体且更有效的方法,可以使用小分子将小鼠成纤维细胞诱导为NSC。小分子诱导的神经干(SMINS)细胞在形态,基因表达模式,自我更新,兴奋性和专能方面与NSC非常相似。此外,SMINS细胞能够在体外和体内分化为星形胶质细胞,功能性神经元和少突胶质细胞。因此,我们建立了一种新颖的方法,可以仅使用小分子即可有效地从成纤维细胞诱导神经干细胞(iNSC),而无需改变基因组。这种化学诱导消除了与当前技术相关的风险,例如使用病毒载体或诱导致癌因子。因此,该技术可以使NSC在临床医学中的各种应用中得到利用。

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