A robust culture system to generate neural progenitors with gliogenic competence from clinically relevant induced pluripotent stem cells for treatment of spinal cord injury

Author:

Kamata Yasuhiro12,Isoda Miho13,Sanosaka Tsukasa1,Shibata Reo2,Ito Shuhei2,Okubo Toshiki2,Shinozaki Munehisa1,Inoue Mitsuhiro13,Koya Ikuko1,Shibata Shinsuke1,Shindo Tomoko1,Matsumoto Morio2,Nakamura Masaya2,Okano Hideyuki1,Nagoshi Narihito2,Kohyama Jun1

Affiliation:

1. Department of Physiology Keio University School of Medicine, Tokyo, Japan

2. Department of Orthopedic Surgery Keio University School of Medicine, Tokyo, Japan

3. Regenerative & Cellular Medicine Kobe Center Sumitomo Dainippon Pharma Co., Ltd, Kobe, Japan

Abstract

Abstract Cell-based therapy targeting spinal cord injury (SCI) is an attractive approach to promote functional recovery by replacing damaged tissue. We and other groups have reported the effectiveness of transplanting neural stem/progenitor cells (NS/PCs) derived from human induced pluripotent stem cells (hiPSCs) in SCI animal models for neuronal replacement. Glial replacement is an additional approach for tissue repair; however, the lack of robust procedures to drive iPSCs into NS/PCs which can produce glial cells has hindered the development of glial cell transplantation for the restoration of neuronal functions after SCI. Here, we established a method to generate NS/PCs with gliogenic competence (gNS/PCs) optimized for clinical relevance and utilized them as a source of therapeutic NS/PCs for SCI. We could successfully generate gNS/PCs from clinically relevant hiPSCs, which efficiently produced astrocytes and oligodendrocytes in vitro. We also performed comparison between gNS/PCs and neurogenic NS/PCs based on single cell RNA-seq analysis and found that gNS/PCs were distinguished by expression of several transcription factors including HEY2 and NFIB. After gNS/PC transplantation, the graft did not exhibit tumor-like tissue formation, indicating the safety of them as a source of cell therapy. Importantly, the gNS/PCs triggered functional recovery in an SCI animal model, with remyelination of demyelinated axons and improved motor function. Given the inherent safety of gNS/PCs and favorable outcomes observed after their transplantation, cell-based medicine using the gNS/PCs-induction procedure described here together with clinically relevant iPSCs is realistic and would be beneficial for SCI patients.

Funder

General Insurance Association of Japan

Japan Agency for Medical Research and Development

Research Center Network for Realization of Regenerative Medicine of the Japan Science and Technology Agency

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Developmental Biology,General Medicine

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