Multichannel bridges and NSC synergize to enhance axon regeneration, myelination, synaptic reconnection, and recovery after SCI

Regeneration in the injured spinal cord is limited by physical and chemical barriers. Acute implantation of a multichannel poly(lactide-co-glycolide) (PLG) bridge mechanically stabilizes the injury, modulates inflammation, and provides a permissive environment for rapid cellularization and robust ax...

Descripción completa

Detalles Bibliográficos
Autores principales: Nekanti, Usha, Sakthivel, Pooja, Zahedi, Atena, Creasman, Dana A., Nishi, Rebecca A., Dumont, Courtney M., Piltti, Katja M., Guardamondo, Glenn L., Hernandez, Norbert, Chen, Xingyuan, Song, Hui, Lin, Xiaoxiao, Martinez, Joshua, On, Lillian, Lakatos, Anita, Pawar, Kiran, David, Brian T., Guo, Zhiling, Seidlits, Stephanie K., Xu, Xiangmin, Shea, Lonnie D., Cummings, Brian J., Anderson, Aileen J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Journal Experts 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10371146/
https://www.ncbi.nlm.nih.gov/pubmed/37502943
http://dx.doi.org/10.21203/rs.3.rs-3044426/v1
_version_ 1785078092218236928
author Nekanti, Usha
Sakthivel, Pooja
Zahedi, Atena
Creasman, Dana A.
Nishi, Rebecca A.
Dumont, Courtney M.
Piltti, Katja M.
Guardamondo, Glenn L.
Hernandez, Norbert
Chen, Xingyuan
Song, Hui
Lin, Xiaoxiao
Martinez, Joshua
On, Lillian
Lakatos, Anita
Pawar, Kiran
David, Brian T.
Guo, Zhiling
Seidlits, Stephanie K.
Xu, Xiangmin
Shea, Lonnie D.
Cummings, Brian J.
Anderson, Aileen J.
author_facet Nekanti, Usha
Sakthivel, Pooja
Zahedi, Atena
Creasman, Dana A.
Nishi, Rebecca A.
Dumont, Courtney M.
Piltti, Katja M.
Guardamondo, Glenn L.
Hernandez, Norbert
Chen, Xingyuan
Song, Hui
Lin, Xiaoxiao
Martinez, Joshua
On, Lillian
Lakatos, Anita
Pawar, Kiran
David, Brian T.
Guo, Zhiling
Seidlits, Stephanie K.
Xu, Xiangmin
Shea, Lonnie D.
Cummings, Brian J.
Anderson, Aileen J.
author_sort Nekanti, Usha
collection PubMed
description Regeneration in the injured spinal cord is limited by physical and chemical barriers. Acute implantation of a multichannel poly(lactide-co-glycolide) (PLG) bridge mechanically stabilizes the injury, modulates inflammation, and provides a permissive environment for rapid cellularization and robust axonal regrowth through this otherwise inhibitory milieu. However, without additional intervention, regenerated axons remain largely unmyelinated (<10%), limiting functional repair. While transplanted human neural stem cells (hNSC) myelinate axons after spinal cord injury (SCI), hNSC fate is highly influenced by the SCI inflammatory microenvironment, also limiting functional repair. Accordingly, we investigated the combination of PLG scaffold bridges with hNSC to improve histological and functional outcome after SCI. In vitro, hNSC culture on a PLG scaffold increased oligodendroglial lineage selection after inflammatory challenge. In vivo, acute PLG bridge implantation followed by chronic hNSC transplantation demonstrated a robust capacity of donor human cells to migrate into PLG bridge channels along regenerating axons and integrate into the host spinal cord as myelinating oligodendrocytes and synaptically integrated neurons. Axons that regenerated through the PLG bridge formed synaptic circuits that connected ipsilateral forelimb muscle to contralateral motor cortex. hNSC transplantation significantly enhanced the total number of regenerating and myelinated axons identified within the PLG bridge. Finally, the combination of acute bridge implantation and hNSC transplantation exhibited robust improvement in locomotor recovery vs. control and hNSC transplant alone. These data identify a successful novel strategy to enhance neurorepair through a temporally layered approach using acute bridge implantation and chronic cell transplantation to spare tissue, promote regeneration, and maximize the function of new axonal connections.
format Online
Article
Text
id pubmed-10371146
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher American Journal Experts
record_format MEDLINE/PubMed
spelling pubmed-103711462023-07-27 Multichannel bridges and NSC synergize to enhance axon regeneration, myelination, synaptic reconnection, and recovery after SCI Nekanti, Usha Sakthivel, Pooja Zahedi, Atena Creasman, Dana A. Nishi, Rebecca A. Dumont, Courtney M. Piltti, Katja M. Guardamondo, Glenn L. Hernandez, Norbert Chen, Xingyuan Song, Hui Lin, Xiaoxiao Martinez, Joshua On, Lillian Lakatos, Anita Pawar, Kiran David, Brian T. Guo, Zhiling Seidlits, Stephanie K. Xu, Xiangmin Shea, Lonnie D. Cummings, Brian J. Anderson, Aileen J. Res Sq Article Regeneration in the injured spinal cord is limited by physical and chemical barriers. Acute implantation of a multichannel poly(lactide-co-glycolide) (PLG) bridge mechanically stabilizes the injury, modulates inflammation, and provides a permissive environment for rapid cellularization and robust axonal regrowth through this otherwise inhibitory milieu. However, without additional intervention, regenerated axons remain largely unmyelinated (<10%), limiting functional repair. While transplanted human neural stem cells (hNSC) myelinate axons after spinal cord injury (SCI), hNSC fate is highly influenced by the SCI inflammatory microenvironment, also limiting functional repair. Accordingly, we investigated the combination of PLG scaffold bridges with hNSC to improve histological and functional outcome after SCI. In vitro, hNSC culture on a PLG scaffold increased oligodendroglial lineage selection after inflammatory challenge. In vivo, acute PLG bridge implantation followed by chronic hNSC transplantation demonstrated a robust capacity of donor human cells to migrate into PLG bridge channels along regenerating axons and integrate into the host spinal cord as myelinating oligodendrocytes and synaptically integrated neurons. Axons that regenerated through the PLG bridge formed synaptic circuits that connected ipsilateral forelimb muscle to contralateral motor cortex. hNSC transplantation significantly enhanced the total number of regenerating and myelinated axons identified within the PLG bridge. Finally, the combination of acute bridge implantation and hNSC transplantation exhibited robust improvement in locomotor recovery vs. control and hNSC transplant alone. These data identify a successful novel strategy to enhance neurorepair through a temporally layered approach using acute bridge implantation and chronic cell transplantation to spare tissue, promote regeneration, and maximize the function of new axonal connections. American Journal Experts 2023-07-19 /pmc/articles/PMC10371146/ /pubmed/37502943 http://dx.doi.org/10.21203/rs.3.rs-3044426/v1 Text en https://creativecommons.org/licenses/by/4.0/License: This work is licensed under a Creative Commons Attribution 4.0 International License. Read Full License (https://creativecommons.org/licenses/by/4.0/) https://creativecommons.org/licenses/by/4.0/This work is licensed under a Creative Commons Attribution 4.0 International License (https://creativecommons.org/licenses/by/4.0/) , which allows reusers to distribute, remix, adapt, and build upon the material in any medium or format, so long as attribution is given to the creator. The license allows for commercial use.
spellingShingle Article
Nekanti, Usha
Sakthivel, Pooja
Zahedi, Atena
Creasman, Dana A.
Nishi, Rebecca A.
Dumont, Courtney M.
Piltti, Katja M.
Guardamondo, Glenn L.
Hernandez, Norbert
Chen, Xingyuan
Song, Hui
Lin, Xiaoxiao
Martinez, Joshua
On, Lillian
Lakatos, Anita
Pawar, Kiran
David, Brian T.
Guo, Zhiling
Seidlits, Stephanie K.
Xu, Xiangmin
Shea, Lonnie D.
Cummings, Brian J.
Anderson, Aileen J.
Multichannel bridges and NSC synergize to enhance axon regeneration, myelination, synaptic reconnection, and recovery after SCI
title Multichannel bridges and NSC synergize to enhance axon regeneration, myelination, synaptic reconnection, and recovery after SCI
title_full Multichannel bridges and NSC synergize to enhance axon regeneration, myelination, synaptic reconnection, and recovery after SCI
title_fullStr Multichannel bridges and NSC synergize to enhance axon regeneration, myelination, synaptic reconnection, and recovery after SCI
title_full_unstemmed Multichannel bridges and NSC synergize to enhance axon regeneration, myelination, synaptic reconnection, and recovery after SCI
title_short Multichannel bridges and NSC synergize to enhance axon regeneration, myelination, synaptic reconnection, and recovery after SCI
title_sort multichannel bridges and nsc synergize to enhance axon regeneration, myelination, synaptic reconnection, and recovery after sci
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10371146/
https://www.ncbi.nlm.nih.gov/pubmed/37502943
http://dx.doi.org/10.21203/rs.3.rs-3044426/v1
work_keys_str_mv AT nekantiusha multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT sakthivelpooja multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT zahediatena multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT creasmandanaa multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT nishirebeccaa multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT dumontcourtneym multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT pilttikatjam multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT guardamondoglennl multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT hernandeznorbert multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT chenxingyuan multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT songhui multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT linxiaoxiao multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT martinezjoshua multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT onlillian multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT lakatosanita multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT pawarkiran multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT davidbriant multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT guozhiling multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT seidlitsstephaniek multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT xuxiangmin multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT shealonnied multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT cummingsbrianj multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci
AT andersonaileenj multichannelbridgesandnscsynergizetoenhanceaxonregenerationmyelinationsynapticreconnectionandrecoveryaftersci

Ejemplares similares