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Robust activation of the human but not mouse telomerase gene during the induction of pluripotency
R. Allen Matthew, Wenwen Jia, Arati Sharma, Yuanjun Zhao, Loren E. Clarke, Xiang Cheng, Huayan Wang, Ugur Salli, Kent E. Vrana, Gavin P. Robertson, Jiyue Zhu, Shuwen Wang
The FASEB Journal · 2010 · ▲ 55 citations
Telomere attrition
Stem-cell exhaustion
Partial reprogramming (OSK)
Telomerase activation
Cell culture / in vitro
Human
Mouse
In vitro
Abstract
Pluripotent stem cells (PSCs) express telomerase and have unlimited proliferative potential. To study telomerase activation during reprogramming, 3 classes of embryonic stem cell (ESC)-like clones were isolated from mouse fibroblasts containing a transgenic hTERT reporter. Class I expressed few pluripotency markers, whereas class II contained many, but not Oct4, Nanog, and Sox2. Neither class of cells differentiated efficiently. Class III cells, the fully reprogrammed induced PSCs (iPSCs), expressed all pluripotency markers, formed teratomas indistinguishable from those of mESCs, and underwent efficient osteogenic differentiation in vitro. Interestingly, whereas the endogenous mTERT gene expression was only moderately increased during reprogramming, the hTERT promoter was strongly activated in class II cells and was further elevated in class III cells. Treatment of class II cells with chemical inhibitors of MEKs and glycogen synthase kinase 3 resulted in their further reprogramming into class III cells, accompanied by a strong activation of hTERT promoter. In reprogrammed human cells, the endogenous telomerase level, although variable among different clones, was dramatically elevated. Only in cells with the highest telomerase were telomeres restored to the lengths in hESCs. Our data, for the first time, demonstrated that the hTERT promoter was strongly activated in discrete steps, revealing a critical difference in human and mouse cell reprogramming. Because telomere(definition) elongation is crucial for self-renewal of hPSCs and replicative aging of their differentiated progeny, these findings have important implications in the generation and applications of iPSCs.
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- 10.1096/fj.09-148973
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- 2026-06-22 MST
Cite this
APA
Matthew, R.A., Jia, W., Sharma, A., Zhao, Y., Clarke, L.E., Cheng, X., Wang, H., Salli, U., Vrana, K.E., Robertson, G.P., Zhu, J., & Wang, S. (2010). Robust activation of the human but not mouse telomerase gene during the induction of pluripotency. <em>The FASEB Journal</em>. https://doi.org/10.1096/fj.09-148973
Vancouver
Matthew RA, Jia W, Sharma A, Zhao Y, Clarke LE, Cheng X, et al. Robust activation of the human but not mouse telomerase gene during the induction of pluripotency. The FASEB Journal. 2010. doi:10.1096/fj.09-148973.
BibTeX
@unpublished{r2010Robust,
title = {Robust activation of the human but not mouse telomerase gene during the induction of pluripotency},
author = {R. Allen Matthew and Wenwen Jia and Arati Sharma and Yuanjun Zhao and Loren E. Clarke and Xiang Cheng and Huayan Wang and Ugur Salli and Kent E. Vrana and Gavin P. Robertson and Jiyue Zhu and Shuwen Wang},
journal = {The FASEB Journal},
year = {2010},
doi = {10.1096/fj.09-148973},
}
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