Generation of Footprint-Free Canine Induced Pluripotent Stem Cells Using Auto-Erasable Sendai Virus Vector

Masaya Tsukamoto(Osaka Prefecture University), T. Nishimura(Stanford University), Kyohei Yodoe(Osaka Prefecture University), Ryoji Kanegi(Osaka Prefecture University), Yasunori TSUJIMOTO(Osaka Prefecture University), Md Emtiaj Alam(Osaka Prefecture University), Mizuki Kuramochi(Osaka Prefecture University), Mitsuru Kuwamura(Osaka Prefecture University), Manami Ohtaka(National Institute of Advanced Industrial Science and Technology), Ken Nishimura(University of Tsukuba), Mahito Nakanishi(National Institute of Advanced Industrial Science and Technology), Toshio Inaba(Osaka Prefecture University), Kikuya Sugiura(Osaka Prefecture University), Shingo Hatoya(Osaka Prefecture University)
Stem Cells and Development
September 14, 2018
Cited by 31

Abstract

Canine induced pluripotent stem cells (ciPSCs) can be used in regenerative medicine. However, there are no reports on the generation of genome integration-free and completely exogenous gene-silenced (footprint free) ciPSCs that are tolerant to enzymatic single-cell passage. In this study, we reprogrammed canine embryonic fibroblasts using the auto-erasable replication-defective and persistent Sendai virus vector, SeVdp(KOSM)302L, and generated two ciPSC lines. The ciPSCs were positive for pluripotent markers, including alkaline phosphatase activity as well as OCT3/4, SOX2, and NANOG transcripts, and NANOG, stage-specific embryonic antigen-1, and partial TRA-1-60 protein expression, even after SeVdp(KOSM)302L removal. The ciPSCs were induced to differentiate into all the three germ layers as embryoid bodies in vitro and as teratomas in vivo. Furthermore, SeVdp(KOSM)302L-free ciPSCs maintained a normal karyotype even after repeated enzymatic single-cell passaging. Therefore, to our knowledge, for the first time, we demonstrated the generation of footprint-free and high-quality ciPSCs that can be passaged at the single-cell stage using enzymatic methods. Our method for generation of ciPSCs is a good step toward the development of clinical application of ciPSCs.


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