4.4 Review

Epigenetic rejuvenation by partial reprogramming

Journal

BIOESSAYS
Volume 45, Issue 4, Pages -

Publisher

WILEY
DOI: 10.1002/bies.202200208

Keywords

ageing clock; DNA methylation; epigenetic; interrupted reprogramming; iPSC; partial reprogramming; pluripotent; rejuvenation; reprogramming; transient reprogramming

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Reprogramming towards pluripotency can rejuvenate cells, reversing age-associated molecular features and evading replicative senescence. However, complete reprogramming can lead to loss of cellular identity and risk of teratoma formation. Limited exposure to reprogramming factors can partially reset epigenetic ageing clocks while maintaining cellular identity. The relationship between rejuvenation and pluripotency, as well as alternative rejuvenation approaches, are discussed in this review.
Rejuvenation of cells by reprogramming toward the pluripotent state raises increasing attention. In fact, generation of induced pluripotent stem cells (iPSCs) completely reverses age-associated molecular features, including elongation of telomeres, resetting of epigenetic clocks and age-associated transcriptomic changes, and even evasion of replicative senescence. However, reprogramming into iPSCs also entails complete de-differentiation with loss of cellular identity, as well as the risk of teratoma formation in anti-ageing treatment paradigms. Recent studies indicate that partial reprogramming by limited exposure to reprogramming factors can reset epigenetic ageing clocks while maintaining cellular identity. So far, there is no commonly accepted definition of partial reprogramming, which is alternatively called interrupted reprogramming, and it remains to be elucidated how the process can be controlled and if it resembles a stable intermediate state. In this review, we discuss if the rejuvenation program can be uncoupled from the pluripotency program or if ageing and cell fate determination are inextricably linked. Alternative rejuvenation approaches with reprogramming into a pluripotent state, partial reprogramming, transdifferentiation, and the possibility of selective resetting of cellular clocks are also discussed.

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