Stem Cell Reports (Nov 2017)

Naked Mole Rat Cells Have a Stable Epigenome that Resists iPSC Reprogramming

  • Li Tan,
  • Zhonghe Ke,
  • Gregory Tombline,
  • Nicholas Macoretta,
  • Kevin Hayes,
  • Xiao Tian,
  • Ruitu Lv,
  • Julia Ablaeva,
  • Michael Gilbert,
  • Natarajan V. Bhanu,
  • Zuo-Fei Yuan,
  • Benjamin A. Garcia,
  • Yujiang G. Shi,
  • Yang Shi,
  • Andrei Seluanov,
  • Vera Gorbunova

Journal volume & issue
Vol. 9, no. 5
pp. 1721 – 1734

Abstract

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Summary: Naked mole rat (NMR) is a valuable model for aging and cancer research due to its exceptional longevity and cancer resistance. We observed that the reprogramming efficiency of NMR fibroblasts in response to OSKM was drastically lower than that of mouse fibroblasts. Expression of SV40 LargeT antigen (LT) dramatically improved reprogramming of NMR fibroblasts. Inactivation of Rb alone, but not p53, was sufficient to improve reprogramming efficiency, suggesting that NMR chromatin may be refractory to reprogramming. Analysis of the global histone landscape revealed that NMR had higher levels of repressive H3K27 methylation marks and lower levels of activating H3K27 acetylation marks than mouse. ATAC-seq revealed that in NMR, promoters of reprogramming genes were more closed than mouse promoters, while expression of LT led to massive opening of the NMR promoters. These results suggest that NMR displays a more stable epigenome that resists de-differentiation, contributing to the cancer resistance and longevity of this species. : Tan et al. show that a more stable epigenome contributes to the resistance of NMR iPSCs to OSKM reprogramming. Reprogramming is facilitated by inactivation of Rb, which leads to opening of promoters of reprogramming genes. Keywords: naked mole rat, iPS cells, epigenome