Investigating the role of Sirtuins in cell reprogramming

Jaein Shin, Junyeop Kim, Hanseul Park, Jongpil Kim

Research output: Contribution to journalReview articlepeer-review

14 Scopus citations

Abstract

Cell reprogramming has been considered a powerful technique in the regenerative medicine field. In addition to diverse its strengths, cell reprogramming technology also has several drawbacks generated during the process of reprogramming. Telomere shortening caused by the cell reprogramming process impedes the efficiency of cell reprogramming. Transcription factors used for reprogramming alter genomic contents and result in genetic mutations. Additionally, defective mitochondria functioning such as excessive mitochondrial fission leads to the limitation of pluripotency and ultimately reduces the efficiency of reprogramming. These problems including genomic instability and impaired mitochondrial dynamics should be resolved to apply cell reprograming in clinical research and to address efficiency and safety concerns. Sirtuin (NAD+-dependent histone deacetylase) has been known to control the chromatin state of the telomere and influence mitochondria function in cells. Recently, several studies reported that Sirtuins could control for genomic instability in cell reprogramming. Here, we review recent findings regarding the role of Sirtuins in cell reprogramming. And we propose that the manipulation of Sirtuins may improve defects that result from the steps of cell reprogramming.

Original languageEnglish
Pages (from-to)500-507
Number of pages8
JournalBMB Reports
Volume51
Issue number10
DOIs
StatePublished - 1 Oct 2018

Keywords

  • Cell reprogramming
  • Genome stability
  • Induced pluripotentstem cells (iPSCs)
  • Mytochondria dynamics
  • Sirtuins (Sirts)

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