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摘要:
In 2006, the "wall came down" that limited the experimental conversion of differentiated cells into the pluripotent state. In a landmark report, Shinya Yamanaka''s group described that a handful of transcription factors(Oct4, Sox2, KIN and c-Myc)can convert a differentiated cell back to pluripotency over the course of a few weeks, thus reprograming them into induced pluripotent stem(iPS)cells. The birth of iPS cells started off a rush among researchers to increase the efficiency of the reprogramming process, to reveal the underlying mechanistic events, and allowed the generation of patient- and disease-specific human iPS cells, which have the potential to be converted into relevant specialized cell types for replacement therapies and disease modeling. This review addresses the steps involved in resetting the epigenetic landscape during reprogramming. Apparently, defined events occur during the course of the reprogramming process. Immediately, upon expression of the reprogramming factors, some cells start to divide faster and quickly begin to lose their differentiated cell characteristics with robust downregulation of somatic genes.Only a subset of cells continue to upregulate the embryonic expression program, and finally, pluripotency genes are upregulated establishing an embryonic stem cell-like transcriptome and epigenome with pluripotent capabilities. Understanding reprogramming to pluripotency will inform mechanistic studies of lineage switching, in which differentiated cells from one lineage can be directly reprogrammed into another without going through a pluripotent intermediate.
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篇名 Reprogramming to pluripotency: stepwise resetting of the epigenetic landscape
来源期刊 细胞研究(英文版) 学科 生物学
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年,卷(期) 2011,(3) 所属期刊栏目
研究方向 页码范围 486-501
页数 16页 分类号 Q2
字数 语种 中文
DOI 10.10381cr.2011.28
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期刊影响力
细胞研究(英文版)
月刊
1001-0602
31-1568/Q
16开
上海岳阳路319号中科院上海生命科学研究院31B,401室
4-645
1990
eng
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2692
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0
总被引数(次)
40708
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