GIT1 protects traumatically injured spinal cord by prompting microvascular endothelial cells to clear myelin debris

The clearance of myelin debris is a critical step in the functional recovery following spinal cord injury (SCI). As phagocytes do, microvascular endothelial cells (MECs) participate in myelin debris clearance at the injury site within one week. Our group has verified that G protein-coupled receptor...

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Autores principales: Wan, Bowen, Li, Cong, Wang, Ming, Kong, Fanqi, Ding, Qirui, Zhang, Chenliang, Liu, Hao, Qian, Dingfei, Deng, Wenlin, Chen, Jian, Tang, Pengyu, Wang, Qian, Zhao, Shujie, Zhou, Zheng, Xu, Tao, Huang, Yifan, Gu, Jun, Fan, Jin, Yin, Guoyong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals 2021
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7993661/
https://www.ncbi.nlm.nih.gov/pubmed/33621952
http://dx.doi.org/10.18632/aging.202560
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author Wan, Bowen
Li, Cong
Wang, Ming
Kong, Fanqi
Ding, Qirui
Zhang, Chenliang
Liu, Hao
Qian, Dingfei
Deng, Wenlin
Chen, Jian
Tang, Pengyu
Wang, Qian
Zhao, Shujie
Zhou, Zheng
Xu, Tao
Huang, Yifan
Gu, Jun
Fan, Jin
Yin, Guoyong
author_facet Wan, Bowen
Li, Cong
Wang, Ming
Kong, Fanqi
Ding, Qirui
Zhang, Chenliang
Liu, Hao
Qian, Dingfei
Deng, Wenlin
Chen, Jian
Tang, Pengyu
Wang, Qian
Zhao, Shujie
Zhou, Zheng
Xu, Tao
Huang, Yifan
Gu, Jun
Fan, Jin
Yin, Guoyong
author_sort Wan, Bowen
collection PubMed
description The clearance of myelin debris is a critical step in the functional recovery following spinal cord injury (SCI). As phagocytes do, microvascular endothelial cells (MECs) participate in myelin debris clearance at the injury site within one week. Our group has verified that G protein-coupled receptor kinase 2 interacting protein-1 (GIT1) is essential in autophagy and angiogenesis, both of which are tightly related to the uptake and degradation of myelin debris by MECs. Here, we analyzed the performance and mechanism of GIT1 in myelin debris clearance after SCI. The SCI contusion model was established and in vitro MECs were treated with myelin debris. Better recovery from traumatic SCI was observed in the GIT1 WT mice than in the GIT1 KO mice. More importantly, we found that GIT1 prompted MECs to clear myelin debris and further enhanced MECs angiogenesis in vivo and in vitro. Mechanistically, GIT1-mediated autophagy contributed to the clearance of myelin debris by MECs. In this study, we demonstrated that GIT1 may prompt MECs to clear myelin debris via autophagy and further stimulate MECs angiogenesis via upregulating VEGF. Our results indicate that GITI may serve as a promising target for accelerating myelin debris clearance and improving SCI recovery.
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spelling pubmed-79936612021-04-06 GIT1 protects traumatically injured spinal cord by prompting microvascular endothelial cells to clear myelin debris Wan, Bowen Li, Cong Wang, Ming Kong, Fanqi Ding, Qirui Zhang, Chenliang Liu, Hao Qian, Dingfei Deng, Wenlin Chen, Jian Tang, Pengyu Wang, Qian Zhao, Shujie Zhou, Zheng Xu, Tao Huang, Yifan Gu, Jun Fan, Jin Yin, Guoyong Aging (Albany NY) Research Paper The clearance of myelin debris is a critical step in the functional recovery following spinal cord injury (SCI). As phagocytes do, microvascular endothelial cells (MECs) participate in myelin debris clearance at the injury site within one week. Our group has verified that G protein-coupled receptor kinase 2 interacting protein-1 (GIT1) is essential in autophagy and angiogenesis, both of which are tightly related to the uptake and degradation of myelin debris by MECs. Here, we analyzed the performance and mechanism of GIT1 in myelin debris clearance after SCI. The SCI contusion model was established and in vitro MECs were treated with myelin debris. Better recovery from traumatic SCI was observed in the GIT1 WT mice than in the GIT1 KO mice. More importantly, we found that GIT1 prompted MECs to clear myelin debris and further enhanced MECs angiogenesis in vivo and in vitro. Mechanistically, GIT1-mediated autophagy contributed to the clearance of myelin debris by MECs. In this study, we demonstrated that GIT1 may prompt MECs to clear myelin debris via autophagy and further stimulate MECs angiogenesis via upregulating VEGF. Our results indicate that GITI may serve as a promising target for accelerating myelin debris clearance and improving SCI recovery. Impact Journals 2021-02-17 /pmc/articles/PMC7993661/ /pubmed/33621952 http://dx.doi.org/10.18632/aging.202560 Text en Copyright: © 2021 Wan et al. https://creativecommons.org/licenses/by/3.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/3.0/) (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Wan, Bowen
Li, Cong
Wang, Ming
Kong, Fanqi
Ding, Qirui
Zhang, Chenliang
Liu, Hao
Qian, Dingfei
Deng, Wenlin
Chen, Jian
Tang, Pengyu
Wang, Qian
Zhao, Shujie
Zhou, Zheng
Xu, Tao
Huang, Yifan
Gu, Jun
Fan, Jin
Yin, Guoyong
GIT1 protects traumatically injured spinal cord by prompting microvascular endothelial cells to clear myelin debris
title GIT1 protects traumatically injured spinal cord by prompting microvascular endothelial cells to clear myelin debris
title_full GIT1 protects traumatically injured spinal cord by prompting microvascular endothelial cells to clear myelin debris
title_fullStr GIT1 protects traumatically injured spinal cord by prompting microvascular endothelial cells to clear myelin debris
title_full_unstemmed GIT1 protects traumatically injured spinal cord by prompting microvascular endothelial cells to clear myelin debris
title_short GIT1 protects traumatically injured spinal cord by prompting microvascular endothelial cells to clear myelin debris
title_sort git1 protects traumatically injured spinal cord by prompting microvascular endothelial cells to clear myelin debris
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7993661/
https://www.ncbi.nlm.nih.gov/pubmed/33621952
http://dx.doi.org/10.18632/aging.202560
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