Looming of the Era for the Induced Pluripotent Stem Cells by Direct Nuclear Reprogram

China Biotechnology

2009, Vol. 29

Issue (08): 124-128 DOI:

Looming of the Era for the Induced Pluripotent Stem Cells by Direct Nuclear Reprogram

MAO Yi, SUN Ji

West China Second University Hospital Sichuan University, Chengdu610041,China

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Abstract

Induced pluripotent stem cells (iPS) are derived from the differentiated somatic cells that regain the differentiation capabilities by the direct nuclear reprogramming with the exogenous factors. The methods for iPS induction evolved from transcription factors to RNA binding proteins, small molecules, and extracellular signals with the efforts in improving biosafty. The cellular and epigenetic characterization for iPS generation is a progressive and timedependent process, which is tightly associated with the cellular differentiation status. However, epigenetics of iPS is not same as the embryonic stem cells. In combination with gene therapy and cellular transplantation therapy, the achievements of iPS had been applied in animal disease model treatment.

Key words： induced pluripotent stem cells;direct nuclear reprogram;transcriptional regulation;cell therapy

Received: 07 November 2008 Published: 28 July 2009

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MAO Yi, SUN Ji. Looming of the Era for the Induced Pluripotent Stem Cells by Direct Nuclear Reprogram. China Biotechnology, 2009, 29(08): 124-128.

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https://manu60.magtech.com.cn/biotech/ OR https://manu60.magtech.com.cn/biotech/Y2009/V29/I08/124

［1］ Zaehres H,Scholer H R.Induction of pluripotency: from mouse to human. Cell, 2007, 131(5):834~835
［2］ Takahashi K,Yamanaka S.Induction of pluripotent stem cells from mouse embryonic and adult fibroblast cultures by defined factors. Cell, 2006, 126(4):663~676
［3］ Okita K, Ichisaka T,Yamanaka S.Generation of germlinecompetent induced pluripotent stem cells. Nature, 2007, 448(7151):313~317
［4］ Jiang J, Chan Y S, Loh Y H, et al.A core klf circuitry regulates selfrenewal of embryonic stem cells. Nat Cell Biol, 2008, 10(3):353~360
［5］ Yu J, Vodyanik MA, SmugaOtto K, et al.Induced pluripotent stem cell lines derived from human somatic cells. Science, 2007, 318(5858):1917~1920
［6］ Rybak A, Fuchs H, Smirnova L, et al. a feedback loop comprising lin28 and let7 controls prelet7 maturation during neural stemcell commitment. Nat Cell Biol, 2008, 10(8):987~993
［7］ Viswanathan S R, Daley G Q,Gregory R I.Selective blockade of microrna processing by lin28. Science, 2008, 320(5872):97~100
［8］ Shi Y, Tae Do J, Desponts C, et al.A combined chemical and genetic approach for the generation of induced pluripotent stem cells. Cell Stem Cell, 2008, 2(6):525~528
［9］ Marson A, Foreman R, Chevalier B, et al.Wnt signaling promotes reprogramming of somatic cells to pluripotency. Cell Stem Cell, 2008, 3(2):132~135
［10］ Wernig M, Meissner A, Cassady J P, et al.Cmyc is dispensable for direct reprogramming of mouse fibroblasts. Cell Stem Cell, 2008, 2(1):10~12
［11］ Kim J B, Zaehres H, Wu G, et al.Pluripotent stem cells induced from adult neural stem cells by reprogramming with two factors. Nature, 2008, 454(7204):646~650
［12］ Duinsbergen D, Eriksson M, Hoen PAC, et al. induced pluripotency with endogenous and inducible genes. Experimental Cell Research(in press)
［13］ Bru T, Clarke C, McGrew M J, et al.Rapid induction of pluripotency genes after exposure of human somatic cells to mouse es cell extracts. Experimental Cell Research, 2008, 314(14):2634~2642
［14］ Cyranoski D,Baker M.Stemcell claim gets cold reception. Nature, 2008, 452(7184):132
［15］ Brambrink T, Foreman R, Welstead G G, et al.Sequential expression of pluripotency markers during direct reprogramming of mouse somatic cells. Cell Stem Cell, 2008, 2(2):151~159
［16］ Stadtfeld M, Maherali N, Breault D T, et al.Defining molecular cornerstones during fibroblast to ips cell reprogramming in mouse. Cell Stem Cell, 2008, 2(3):230~240
［17］ Nakagawa M, Koyanagi M, Tanabe K, et al.Generation of induced pluripotent stem cells without myc from mouse and human fibroblasts. Nat Biotech, 2008, 26(1):101~106
［18］ Aoi T, Yae K, Nakagawa M, et al.Generation of pluripotent stem cells from adult mouse liver and stomach cells. Science, 2008, 321(5889):699~702
［19］ Hanna J, Markoulaki S, Schorderet P, et al.Direct reprogramming of terminally differentiated mature b lymphocytes to pluripotency. Cell, 2008, 133(2):250~264
［20］ Mikkelsen T S, Hanna J, Zhang X, et al.Dissecting direct reprogramming through integrative genomic analysis. Nature, 2008, 454(7200):49~55
［21］ Maherali N, Sridharan R, Xie W, et al.Directly reprogrammed fibroblasts show global epigenetic remodeling and widespread tissue contribution. Cell Stem Cell, 2007, 1(1):55~70
［22］ Stadtfeld M, Brennand K,Hochedlinger K.Reprogramming of pancreatic ［beta］ cells into induced pluripotent stem cells. Current Biology, 2008, 18(12):890~894
［23］ Dimos J T, Rodolfa K T, Niakan K K, et al.Induced pluripotent stem cells generated from patients with als can be differentiated into motor neurons. Science, 2008,321(5879):9
［24］ Lowry W E, Richter L, Yachechko R, et al.Generation of human induced pluripotent stem cells from dermal fibroblasts. Proceedings of the National Academy of Sciences, 2008, 105(8):2883~2888
［25］ Narazaki G, Uosaki H, Teranishi M, et al.Directed and systematic differentiation of cardiovascular cells from mouse induced pluripotent stem cells. Circulation, 2008, 118(5):498~506
［26］ Mauritz C, Schwanke K, Reppel M, et al.Generation of functional murine cardiac myocytes from induced pluripotent stem cells. Circulation, 2008, 118(5):507~517
［27］ Hanna J, Wernig M, Markoulaki S, et al.Treatment of sickle cell anemia mouse model with ips cells generated from autologous skin. Science, 2007, 318(5858):1920~1923
［28］ Rodolfa K T,Eggan K.A transcriptional logic for nuclear reprogramming. Cell, 2006, 126(4):652~655

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