Novel Hyperactive Transposons for Genetic Modification of Induced Pluripotent and Adult Stem Cells: A Nonviral Paradigm for Coaxed Differentiation

Author:

Belay Eyayu1,Mátrai Janka1,Acosta-Sanchez Abel1,Ma Ling1,Quattrocelli Mattia2,Mátés Lajos3,Sancho-Bru Pau2,Geraerts Martine2,Yan Bing1,Vermeesch Joris4,Rincón Melvin Yesid1,Samara-Kuko Ermira1,Ivics Zoltán35,Verfaillie Catherine2,Sampaolesi Maurilio2,Izsvák Zsuzsanna35,VandenDriessche Thierry16,Chuah Marinee K. L.16

Affiliation:

1. Flanders Institute for Biotechnology (VIB), Vesalius Research Center, University of Leuven, Leuven, Belgium

2. Stem Cell Institute, University of Leuven, Leuven, Belgium

3. Max Delbrück Center for Molecular Medicine, Mobile DNA Group, Berlin, Germany

4. Center for Human Genetics, University Hospital Gasthuisberg, Leuven, Belgium

5. University of Debrecen, Department of Human Genetics, Debrecen, Hungary

6. Free University of Brussels (VUB), Brussels, Belgium

Abstract

Abstract Adult stem cells and induced pluripotent stem cells (iPS) hold great promise for regenerative medicine. The development of robust nonviral approaches for stem cell gene transfer would facilitate functional studies and potential clinical applications. We have previously generated hyperactive transposases derived from Sleeping Beauty, using an in vitro molecular evolution and selection paradigm. We now demonstrate that these hyperactive transposases resulted in superior gene transfer efficiencies and expression in mesenchymal and muscle stem/progenitor cells, consistent with higher expression levels of therapeutically relevant proteins including coagulation factor IX. Their differentiation potential and karyotype was not affected. Moreover, stable transposition could also be achieved in iPS, which retained their ability to differentiate along neuronal, cardiac, and hepatic lineages without causing cytogenetic abnormalities. Most importantly, transposon-mediated delivery of the myogenic PAX3 transcription factor into iPS coaxed their differentiation into MYOD+ myogenic progenitors and multinucleated myofibers, suggesting that PAX3 may serve as a myogenic “molecular switch” in iPS. Hence, this hyperactive transposon system represents an attractive nonviral gene transfer platform with broad implications for regenerative medicine, cell and gene therapy.

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Developmental Biology,Molecular Medicine

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