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Partial reprogramming induces a steady decline in epigenetic age before loss of somatic identity
Nelly Olova, Daniel J. Simpson, Riccardo E. Marioni, Tamir Chandra
bioRxiv (Cold Spring Harbor Laboratory) · 2018 · ▲ 7 citations
Abstract
Summary Induced pluripotent stem cells (IPSCs), with their unlimited regenerative capacity, carry the promise for tissue replacement to counter age-related decline. However, attempts to realise in vivo iPSC have invariably resulted in the formation of teratomas. Partial reprogramming(definition) in prematurely aged mice has shown promising results in alleviating age-related symptoms without teratoma formation. Does partial reprogramming lead to rejuvenation (i.e. “younger” cells), rather than dedifferentiation, which bears the risk of cancer? Here we analyse the dynamics of cellular age during human iPSC reprogramming and find that partial reprogramming leads to a reduction in the epigenetic age of cells. We also find that the loss of somatic gene expression and epigenetic age follow different kinetics, suggesting that they can be uncoupled and there could be a safe window where rejuvenation can be achieved with a minimised risk of cancer.
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- 10.1101/292680
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- 2026-06-18 MST
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APA
Olova, N., Simpson, D.J., Marioni, R.E., & Chandra, T. (2018). Partial reprogramming induces a steady decline in epigenetic age before loss of somatic identity. <em>bioRxiv (Cold Spring Harbor Laboratory)</em>. https://doi.org/10.1101/292680
Vancouver
Olova N, Simpson DJ, Marioni RE, Chandra T. Partial reprogramming induces a steady decline in epigenetic age before loss of somatic identity. bioRxiv (Cold Spring Harbor Laboratory). 2018. doi:10.1101/292680.
BibTeX
@unpublished{nelly2018Partia,
title = {Partial reprogramming induces a steady decline in epigenetic age before loss of somatic identity},
author = {Nelly Olova and Daniel J. Simpson and Riccardo E. Marioni and Tamir Chandra},
journal = {bioRxiv (Cold Spring Harbor Laboratory)},
year = {2018},
doi = {10.1101/292680},
}
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