Harnessing the potential of induced pluripotent stem cells for regenerative medicine

被引:0
|
作者
Sean M. Wu
Konrad Hochedlinger
机构
[1] Sean M. Wu is at the Cardiovascular Research Center,Division of Cardiology
[2] Massachusetts General Hospital,USA; the Department of Stem Cell and Regenerative Biology, Department of Stem Cell and Regenerative Biology
[3] Boston 02114,undefined
[4] Massachusetts,undefined
[5] USA and the Harvard Stem Cell Institute,undefined
[6] Cambridge,undefined
[7] Massachusetts 02138,undefined
[8] USA,undefined
[9] Konrad Hochedlinger is at the Harvard Stem Cell Institute,undefined
[10] Cambridge,undefined
[11] Massachusetts 02138,undefined
[12] USA; the Center for Regenerative Medicine and Cancer Center,undefined
[13] Massachusetts General Hospital,undefined
[14] Boston,undefined
[15] Massachusetts 02114,undefined
[16] Harvard University,undefined
[17] Cambridge,undefined
[18] Massachusetts 02138,undefined
[19] USA and the Howard Hughes Medical Institute,undefined
[20] Harvard University,undefined
[21] Cambridge,undefined
[22] Massachusetts 02138,undefined
[23] USA,undefined
[24] the Center for Regenerative Medicine and Cancer Center,undefined
[25] Massachusetts General Hospital,undefined
[26] Boston,undefined
[27] Massachusetts 02114,undefined
[28] USA,undefined
来源
Nature Cell Biology | 2011年 / 13卷
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摘要
The discovery of methods to convert somatic cells into induced pluripotent stem cells (iPSCs) through expression of a small combination of transcription factors has raised the possibility of producing custom-tailored cells for the study and treatment of numerous diseases. Indeed, iPSCs have already been derived from patients suffering from a large variety of disorders. Here we review recent progress that has been made in establishing iPSC-based disease models, discuss associated technical and biological challenges, and highlight possible solutions to overcome these barriers. We believe that a better understanding of the molecular basis of pluripotency, cellular reprogramming and lineage-specific differentiation of iPSCs is necessary for progress in regenerative medicine.
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页码:497 / 505
页数:8
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