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急性氧张力降低增强了人成纤维细胞向神经元的诱导。

Acute reduction in oxygen tension enhances the induction of neurons from human fibroblasts.

机构信息

Institute for Stem Cell Biology and Regenerative Medicine, Stanford, CA 94305, USA.

出版信息

J Neurosci Methods. 2013 Jun 15;216(2):104-9. doi: 10.1016/j.jneumeth.2013.03.020. Epub 2013 Apr 3.

Abstract

We and others have reported the successful conversion of human fibroblasts into functional induced neuronal (iN) cells; however the reprogramming efficiencies were very low. Robust reprogramming methods must be developed before iN cells can be used for translational applications such as disease modeling or transplantation-based therapies. Here, we describe a novel approach in which we significantly enhance iN cell conversion efficiency of human fibroblast cells by reprogramming under hypoxic conditions (5% O₂). Fibroblasts were derived under high (21%) or low (5%) oxygen conditions and reprogrammed into iN cells using a combination of the four transcription factors BRN2, ASCL1, MYT1L and NEUROD1. An increase in Map2 immunostaining was only observed when fibroblasts experienced an acute drop in O₂ tension upon infection. Interestingly, cells derived and reprogrammed under hypoxic conditions did not produce more iN cells. Approximately 100% of patched cells fired action potentials in low O₂ conditions compared to 50% under high O₂ growth conditions, confirming the beneficial aspect of reprogramming under low O₂. Further characterization showed no significant difference in the intrinsic properties of iN cells reprogrammed in either condition. Surprisingly, the acute drop in oxygen tension did not affect cell proliferation or cell survival and was not synergistic with the blockade of GSK3β and Smad-mediated pathways. Our results showed that lowering the O₂ tension at the initiation of reprogramming is a simple and efficient strategy to enhance the production of iN cells which will facilitate their use for basic discovery and regenerative medicine.

摘要

我们和其他人已经报道了将人类成纤维细胞成功转化为功能性诱导神经元(iN)细胞的方法;然而,其重编程效率非常低。在 iN 细胞可用于转化应用(如疾病建模或基于移植的治疗)之前,必须开发强大的重编程方法。在这里,我们描述了一种新方法,即在低氧(5% O₂)条件下进行重编程,可显著提高人类成纤维细胞 iN 细胞的转化率。成纤维细胞在高(21%)或低(5%)氧条件下产生,并使用 BRN2、ASCL1、MYT1L 和 NEUROD1 这四种转录因子的组合重编程为 iN 细胞。只有在感染时成纤维细胞经历 O₂张力的急性下降时,才会观察到 Map2 免疫染色增加。有趣的是,在低氧条件下产生和重编程的细胞并没有产生更多的 iN 细胞。与高 O₂生长条件下的 50%相比,约 100%的 patched 细胞在低 O₂条件下会产生动作电位,证实了低 O₂条件下重编程的有益方面。进一步的特征表明,在两种条件下重编程的 iN 细胞的内在特性没有显著差异。令人惊讶的是,氧气张力的急性下降不会影响细胞增殖或细胞存活,并且与 GSK3β 和 Smad 介导的途径阻断没有协同作用。我们的结果表明,在重编程开始时降低 O₂张力是一种简单有效的策略,可以提高 iN 细胞的产量,这将有助于它们在基础发现和再生医学中的应用。

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