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Published in: Translational Stroke Research 1/2020

Open Access 01-02-2020 | Stroke | Original Research

Transplantation of Directly Reprogrammed Human Neural Precursor Cells Following Stroke Promotes Synaptogenesis and Functional Recovery

Authors: Ilan Vonderwalde, Ashkan Azimi, Gabrielle Rolvink, Jan-Eric Ahlfors, Molly S. Shoichet, Cindi M. Morshead

Published in: Translational Stroke Research | Issue 1/2020

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Abstract

Stroke is one of the leading causes of long-term disability. Cell transplantation is a promising strategy to treat stroke. We explored the efficacy of directly reprogrammed human neural precursor cell (drNPC) transplants to promote functional recovery in a model of focal ischemic stroke in the mouse sensorimotor cortex. We show that drNPCs express neural precursor cell markers and are neurally committed at the time of transplantation. Mice that received drNPC transplants recovered motor function, irrespective of transplant vehicle or recipient sex, and with no correlation to lesion volume or glial scarring. The majority of drNPCs found in vivo, at the time of functional recovery, remained undifferentiated. Notably, no correlation between functional recovery and long-term xenograft survival was observed, indicating that drNPCs provide therapeutic benefits beyond their survival. Furthermore, increased synaptophysin expression in transplanted brains suggests that drNPCs promote neuroplasticity through enhanced synaptogenesis. Our findings provide insight into the mechanistic underpinnings of drNPC-mediated recovery for stroke and support the notion that drNPCs may have clinical applications for stroke therapy.
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Metadata
Title
Transplantation of Directly Reprogrammed Human Neural Precursor Cells Following Stroke Promotes Synaptogenesis and Functional Recovery
Authors
Ilan Vonderwalde
Ashkan Azimi
Gabrielle Rolvink
Jan-Eric Ahlfors
Molly S. Shoichet
Cindi M. Morshead
Publication date
01-02-2020
Publisher
Springer US
Keyword
Stroke
Published in
Translational Stroke Research / Issue 1/2020
Print ISSN: 1868-4483
Electronic ISSN: 1868-601X
DOI
https://doi.org/10.1007/s12975-019-0691-x

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