論文

査読有り 国際誌
2018年12月

Epigenetic-scale comparison of human iPSCs generated by retrovirus, Sendai virus or episomal vectors.

Regenerative therapy
  • Koichiro Nishino
  • Yoshikazu Arai
  • Ken Takasawa
  • Masashi Toyoda
  • Mayu Yamazaki-Inoue
  • Tohru Sugawara
  • Hidenori Akutsu
  • Ken Nishimura
  • Manami Ohtaka
  • Mahito Nakanishi
  • Akihiro Umezawa
  • 全て表示

9
開始ページ
71
終了ページ
78
記述言語
英語
掲載種別
研究論文(学術雑誌)
DOI
10.1016/j.reth.2018.08.002
出版者・発行元
ELSEVIER SCIENCE BV

Human induced pluripotent stem cells (iPSCs) are established by introducing several reprogramming factors, such as OCT3/4, SOX2, KLF4, c-MYC. Because of their pluripotency and immortality, iPSCs are considered to be a powerful tool for regenerative medicine. To date, iPSCs have been established all over the world by various gene delivery methods. All methods induced high-quality iPSCs, but epigenetic analysis of abnormalities derived from differences in the gene delivery methods has not yet been performed. Here, we generated genetically matched human iPSCs from menstrual blood cells by using three kinds of vectors, i.e., retrovirus, Sendai virus, and episomal vectors, and compared genome-wide DNA methylation profiles among them. Although comparison of aberrant methylation revealed that iPSCs generated by Sendai virus vector have lowest number of aberrant methylation sites among the three vectors, the iPSCs generated by non-integrating methods did not show vector-specific aberrant methylation. However, the differences between the iPSC lines were determined to be the number of random aberrant hypermethylated regions compared with embryonic stem cells. These random aberrant hypermethylations might be a cause of the differences in the properties of each of the iPSC lines.

リンク情報
DOI
https://doi.org/10.1016/j.reth.2018.08.002
PubMed
https://www.ncbi.nlm.nih.gov/pubmed/30525077
PubMed Central
https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6222281
ID情報
  • DOI : 10.1016/j.reth.2018.08.002
  • ISSN : 2352-3204
  • PubMed ID : 30525077
  • PubMed Central 記事ID : PMC6222281

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