Stem Cell Research & Therapy (Nov 2017)

Using low-risk factors to generate non-integrated human induced pluripotent stem cells from urine-derived cells

  • Linli Wang,
  • Yuehua Chen,
  • Chunyan Guan,
  • Zhiju Zhao,
  • Qiang Li,
  • Jianguo Yang,
  • Jian Mo,
  • Bin Wang,
  • Wei Wu,
  • Xiaohui Yang,
  • Libing Song,
  • Jun Li

DOI
https://doi.org/10.1186/s13287-017-0698-8
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 13

Abstract

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Abstract Background Because the lack of an induced pluripotent stem cell (iPSC) induction system with optimal safety and efficiency limits the application of these cells, development of such a system is important. Methods To create such an induction system, we screened a variety of reprogrammed plasmid combinations and multiple compounds and then verified the system’s feasibility using urine cells from different individuals. We also compared large-scale iPSC chromosomal variations and expression of genes associated with genomic stability between this system and the traditional episomal system using karyotype and quantitative reverse transcription polymerase chain reaction analyses. Results We developed a high-efficiency episomal system, the 6F/BM1-4C system, lacking tumorigenic factors for human urine-derived cell (hUC) reprogramming. This system includes six low-risk factors (6F), Oct4, Glis1, Klf4, Sox2, L-Myc, and the miR-302 cluster. Transfected hUCs were treated with four compounds (4C), inhibitor of lysine-demethylase1, methyl ethyl ketone, glycogen synthase kinase 3 beta, and histone deacetylase, within a short time period. Comparative analysis revealed significantly decreased chromosomal variation in iPSCs and significantly increased Sirt1 expression compared with iPSCs induced using the traditional episomal system. Conclusion The 6F/BM1-4C system effectively induces reprogramming of urine cells in samples obtained from different individuals. iPSCs induced using the 6F/BM1-4C system are more stable at the cytogenetic level and have potential value for clinical application.

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