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Time-dependent changes in the microenvironment of injured spinal cord affects the therapeutic potential of neural stem cell transplantation for spinal cord injury

BACKGROUND: The transplantation of neural stem/progenitor cells (NS/PCs) at the sub-acute phase of spinal cord injury, but not at the chronic phase, can promote functional recovery. However, the reasons for this difference and whether it involves the survival and/or fate of grafted cells under these...

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Autores principales: Nishimura, Soraya, Yasuda, Akimasa, Iwai, Hiroki, Takano, Morito, Kobayashi, Yoshiomi, Nori, Satoshi, Tsuji, Osahiko, Fujiyoshi, Kanehiro, Ebise, Hayao, Toyama, Yoshiaki, Okano, Hideyuki, Nakamura, Masaya
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3556141/
https://www.ncbi.nlm.nih.gov/pubmed/23298657
http://dx.doi.org/10.1186/1756-6606-6-3
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author Nishimura, Soraya
Yasuda, Akimasa
Iwai, Hiroki
Takano, Morito
Kobayashi, Yoshiomi
Nori, Satoshi
Tsuji, Osahiko
Fujiyoshi, Kanehiro
Ebise, Hayao
Toyama, Yoshiaki
Okano, Hideyuki
Nakamura, Masaya
author_facet Nishimura, Soraya
Yasuda, Akimasa
Iwai, Hiroki
Takano, Morito
Kobayashi, Yoshiomi
Nori, Satoshi
Tsuji, Osahiko
Fujiyoshi, Kanehiro
Ebise, Hayao
Toyama, Yoshiaki
Okano, Hideyuki
Nakamura, Masaya
author_sort Nishimura, Soraya
collection PubMed
description BACKGROUND: The transplantation of neural stem/progenitor cells (NS/PCs) at the sub-acute phase of spinal cord injury, but not at the chronic phase, can promote functional recovery. However, the reasons for this difference and whether it involves the survival and/or fate of grafted cells under these two conditions remain unclear. To address this question, NS/PC transplantation was performed after contusive spinal cord injury in adult mice at the sub-acute and chronic phases. RESULTS: Quantitative analyses using bio-imaging, which can noninvasively detect surviving grafted cells in living animals, revealed no significant difference in the survival rate of grafted cells between the sub-acute and chronic transplantation groups. Additionally, immunohistology revealed no significant difference in the differentiation phenotypes of grafted cells between the two groups. Microarray analysis revealed no significant differences in the expression of genes encoding inflammatory cytokines or growth factors, which affect the survival and/or fate of grafted cells, in the injured spinal cord between the sub-acute and chronic phases. By contrast, the distribution of chronically grafted NS/PCs was restricted compared to NS/PCs grafted at the sub-acute phase because a more prominent glial scar located around the lesion epicenter enclosed the grafted cells. Furthermore, microarray and histological analysis revealed that the infiltration of macrophages, especially M2 macrophages, which have anti-inflammatory role, was significantly higher at the sub-acute phase than the chronic phase. Ultimately, NS/PCs that were transplanted in the sub-acute phase, but not the chronic phase, promoted functional recovery compared with the vehicle control group. CONCLUSIONS: The extent of glial scar formation and the characteristics of inflammation is the most remarkable difference in the injured spinal cord microenvironment between the sub-acute and chronic phases. To achieve functional recovery by NS/PC transplantation in cases at the chronic phase, modification of the microenvironment of the injured spinal cord focusing on glial scar formation and inflammatory phenotype should be considered.
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spelling pubmed-35561412013-01-31 Time-dependent changes in the microenvironment of injured spinal cord affects the therapeutic potential of neural stem cell transplantation for spinal cord injury Nishimura, Soraya Yasuda, Akimasa Iwai, Hiroki Takano, Morito Kobayashi, Yoshiomi Nori, Satoshi Tsuji, Osahiko Fujiyoshi, Kanehiro Ebise, Hayao Toyama, Yoshiaki Okano, Hideyuki Nakamura, Masaya Mol Brain Research BACKGROUND: The transplantation of neural stem/progenitor cells (NS/PCs) at the sub-acute phase of spinal cord injury, but not at the chronic phase, can promote functional recovery. However, the reasons for this difference and whether it involves the survival and/or fate of grafted cells under these two conditions remain unclear. To address this question, NS/PC transplantation was performed after contusive spinal cord injury in adult mice at the sub-acute and chronic phases. RESULTS: Quantitative analyses using bio-imaging, which can noninvasively detect surviving grafted cells in living animals, revealed no significant difference in the survival rate of grafted cells between the sub-acute and chronic transplantation groups. Additionally, immunohistology revealed no significant difference in the differentiation phenotypes of grafted cells between the two groups. Microarray analysis revealed no significant differences in the expression of genes encoding inflammatory cytokines or growth factors, which affect the survival and/or fate of grafted cells, in the injured spinal cord between the sub-acute and chronic phases. By contrast, the distribution of chronically grafted NS/PCs was restricted compared to NS/PCs grafted at the sub-acute phase because a more prominent glial scar located around the lesion epicenter enclosed the grafted cells. Furthermore, microarray and histological analysis revealed that the infiltration of macrophages, especially M2 macrophages, which have anti-inflammatory role, was significantly higher at the sub-acute phase than the chronic phase. Ultimately, NS/PCs that were transplanted in the sub-acute phase, but not the chronic phase, promoted functional recovery compared with the vehicle control group. CONCLUSIONS: The extent of glial scar formation and the characteristics of inflammation is the most remarkable difference in the injured spinal cord microenvironment between the sub-acute and chronic phases. To achieve functional recovery by NS/PC transplantation in cases at the chronic phase, modification of the microenvironment of the injured spinal cord focusing on glial scar formation and inflammatory phenotype should be considered. BioMed Central 2013-01-08 /pmc/articles/PMC3556141/ /pubmed/23298657 http://dx.doi.org/10.1186/1756-6606-6-3 Text en Copyright ©2013 Nishimura et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Nishimura, Soraya
Yasuda, Akimasa
Iwai, Hiroki
Takano, Morito
Kobayashi, Yoshiomi
Nori, Satoshi
Tsuji, Osahiko
Fujiyoshi, Kanehiro
Ebise, Hayao
Toyama, Yoshiaki
Okano, Hideyuki
Nakamura, Masaya
Time-dependent changes in the microenvironment of injured spinal cord affects the therapeutic potential of neural stem cell transplantation for spinal cord injury
title Time-dependent changes in the microenvironment of injured spinal cord affects the therapeutic potential of neural stem cell transplantation for spinal cord injury
title_full Time-dependent changes in the microenvironment of injured spinal cord affects the therapeutic potential of neural stem cell transplantation for spinal cord injury
title_fullStr Time-dependent changes in the microenvironment of injured spinal cord affects the therapeutic potential of neural stem cell transplantation for spinal cord injury
title_full_unstemmed Time-dependent changes in the microenvironment of injured spinal cord affects the therapeutic potential of neural stem cell transplantation for spinal cord injury
title_short Time-dependent changes in the microenvironment of injured spinal cord affects the therapeutic potential of neural stem cell transplantation for spinal cord injury
title_sort time-dependent changes in the microenvironment of injured spinal cord affects the therapeutic potential of neural stem cell transplantation for spinal cord injury
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3556141/
https://www.ncbi.nlm.nih.gov/pubmed/23298657
http://dx.doi.org/10.1186/1756-6606-6-3
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