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终末分化的肝细胞向功能性神经元的直接谱系转化。

Direct lineage conversion of terminally differentiated hepatocytes to functional neurons.

机构信息

Institute for Stem Cell Biology and Regenerative Medicine and Department of Pathology, Stanford University School of Medicine, CA 94305, USA.

出版信息

Cell Stem Cell. 2011 Oct 4;9(4):374-82. doi: 10.1016/j.stem.2011.09.002. Epub 2011 Sep 29.

Abstract

Several recent studies have showed that mouse and human fibroblasts can be directly reprogrammed into induced neuronal (iN) cells, bypassing a pluripotent intermediate state. However, fibroblasts represent heterogeneous mesenchymal progenitor cells that potentially contain neural crest lineages, and the cell of origin remained undefined. This raises the fundamental question of whether lineage reprogramming is possible between cell types derived from different germ layers. Here, we demonstrate that terminally differentiated hepatocytes can be directly converted into functional iN cells. Importantly, single-cell and genome-wide expression analyses showed that fibroblast- and hepatocyte-derived iN cells not only induced a neuronal transcriptional program, but also silenced their donor transcriptome. The remaining donor signature decreased over time and could not support functional hepatocyte properties. Thus, the reprogramming factors lead to a binary lineage switch decision rather than an induction of hybrid phenotypes, but iN cells retain a small but detectable epigenetic memory of their donor cells.

摘要

最近的几项研究表明,小鼠和人类成纤维细胞可以直接重编程为诱导性神经元(iN)细胞,绕过多能性中间状态。然而,成纤维细胞代表异质性的间充质祖细胞,其中可能包含神经嵴谱系,而细胞起源尚未确定。这就提出了一个基本问题,即不同胚层来源的细胞类型之间是否可能进行谱系重编程。在这里,我们证明了终末分化的肝细胞可以直接转化为功能性 iN 细胞。重要的是,单细胞和全基因组表达分析表明,成纤维细胞和肝细胞来源的 iN 细胞不仅诱导了神经元转录程序,而且还沉默了它们的供体细胞转录组。随着时间的推移,剩余的供体特征减少,并且不能支持功能性肝细胞特性。因此,重编程因子导致二元谱系转换决定,而不是诱导杂种表型,但 iN 细胞保留其供体细胞的小但可检测的表观遗传记忆。

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