Selective deletion of zinc transporter 3 in amacrine cells promotes retinal ganglion cell survival and optic nerve regeneration after injury

Vision depends on accurate signal conduction from the retina to the brain through the optic nerve, an important part of the central nervous system that consists of bundles of axons originating from retinal ganglion cells. The mammalian optic nerve, an important part of the central nervous system, ca...

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Autores principales: Liu, Zhe, Xue, Jingfei, Liu, Canying, Tang, Jiahui, Wu, Siting, Lin, Jicheng, Han, Jiaxu, Zhang, Qi, Wu, Caiqing, Huang, Haishun, Zhao, Ling, Zhuo, Yehong, Li, Yiqing
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Wolters Kluwer - Medknow 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10358645/
https://www.ncbi.nlm.nih.gov/pubmed/37449644
http://dx.doi.org/10.4103/1673-5374.373660
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author Liu, Zhe
Xue, Jingfei
Liu, Canying
Tang, Jiahui
Wu, Siting
Lin, Jicheng
Han, Jiaxu
Zhang, Qi
Wu, Caiqing
Huang, Haishun
Zhao, Ling
Zhuo, Yehong
Li, Yiqing
author_facet Liu, Zhe
Xue, Jingfei
Liu, Canying
Tang, Jiahui
Wu, Siting
Lin, Jicheng
Han, Jiaxu
Zhang, Qi
Wu, Caiqing
Huang, Haishun
Zhao, Ling
Zhuo, Yehong
Li, Yiqing
author_sort Liu, Zhe
collection PubMed
description Vision depends on accurate signal conduction from the retina to the brain through the optic nerve, an important part of the central nervous system that consists of bundles of axons originating from retinal ganglion cells. The mammalian optic nerve, an important part of the central nervous system, cannot regenerate once it is injured, leading to permanent vision loss. To date, there is no clinical treatment that can regenerate the optic nerve and restore vision. Our previous study found that the mobile zinc (Zn((2)+)) level increased rapidly after optic nerve injury in the retina, specifically in the vesicles of the inner plexiform layer. Furthermore, chelating Zn((2)+) significantly promoted axonal regeneration with a long-term effect. In this study, we conditionally knocked out zinc transporter 3 (ZnT3) in amacrine cells or retinal ganglion cells to construct two transgenic mouse lines (VGAT(Cre)ZnT3(fl/fl) and VGLUT2(Cre)ZnT3(fl/fl), respectively). We obtained direct evidence that the rapidly increased mobile Zn((2)+) in response to injury was from amacrine cells. We also found that selective deletion of ZnT3 in amacrine cells promoted retinal ganglion cell survival and axonal regeneration after optic nerve crush injury, improved retinal ganglion cell function, and promoted vision recovery. Sequencing analysis of reginal ganglion cells revealed that inhibiting the release of presynaptic Zn((2)+) affected the transcription of key genes related to the survival of retinal ganglion cells in postsynaptic neurons, regulated the synaptic connection between amacrine cells and retinal ganglion cells, and affected the fate of retinal ganglion cells. These results suggest that amacrine cells release Zn((2)+) to trigger transcriptomic changes related to neuronal growth and survival in reginal ganglion cells, thereby influencing the synaptic plasticity of retinal networks. These results make the theory of zinc-dependent retinal ganglion cell death more accurate and complete and provide new insights into the complex interactions between retinal cell networks.
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spelling pubmed-103586452023-07-21 Selective deletion of zinc transporter 3 in amacrine cells promotes retinal ganglion cell survival and optic nerve regeneration after injury Liu, Zhe Xue, Jingfei Liu, Canying Tang, Jiahui Wu, Siting Lin, Jicheng Han, Jiaxu Zhang, Qi Wu, Caiqing Huang, Haishun Zhao, Ling Zhuo, Yehong Li, Yiqing Neural Regen Res Research Article Vision depends on accurate signal conduction from the retina to the brain through the optic nerve, an important part of the central nervous system that consists of bundles of axons originating from retinal ganglion cells. The mammalian optic nerve, an important part of the central nervous system, cannot regenerate once it is injured, leading to permanent vision loss. To date, there is no clinical treatment that can regenerate the optic nerve and restore vision. Our previous study found that the mobile zinc (Zn((2)+)) level increased rapidly after optic nerve injury in the retina, specifically in the vesicles of the inner plexiform layer. Furthermore, chelating Zn((2)+) significantly promoted axonal regeneration with a long-term effect. In this study, we conditionally knocked out zinc transporter 3 (ZnT3) in amacrine cells or retinal ganglion cells to construct two transgenic mouse lines (VGAT(Cre)ZnT3(fl/fl) and VGLUT2(Cre)ZnT3(fl/fl), respectively). We obtained direct evidence that the rapidly increased mobile Zn((2)+) in response to injury was from amacrine cells. We also found that selective deletion of ZnT3 in amacrine cells promoted retinal ganglion cell survival and axonal regeneration after optic nerve crush injury, improved retinal ganglion cell function, and promoted vision recovery. Sequencing analysis of reginal ganglion cells revealed that inhibiting the release of presynaptic Zn((2)+) affected the transcription of key genes related to the survival of retinal ganglion cells in postsynaptic neurons, regulated the synaptic connection between amacrine cells and retinal ganglion cells, and affected the fate of retinal ganglion cells. These results suggest that amacrine cells release Zn((2)+) to trigger transcriptomic changes related to neuronal growth and survival in reginal ganglion cells, thereby influencing the synaptic plasticity of retinal networks. These results make the theory of zinc-dependent retinal ganglion cell death more accurate and complete and provide new insights into the complex interactions between retinal cell networks. Wolters Kluwer - Medknow 2023-04-10 /pmc/articles/PMC10358645/ /pubmed/37449644 http://dx.doi.org/10.4103/1673-5374.373660 Text en Copyright: © Neural Regeneration Research https://creativecommons.org/licenses/by-nc-sa/4.0/This is an open access journal, and articles are distributed under the terms of the Creative Commons Attribution-NonCommercial-ShareAlike 4.0 License, which allows others to remix, tweak, and build upon the work non-commercially, as long as appropriate credit is given and the new creations are licensed under the identical terms.
spellingShingle Research Article
Liu, Zhe
Xue, Jingfei
Liu, Canying
Tang, Jiahui
Wu, Siting
Lin, Jicheng
Han, Jiaxu
Zhang, Qi
Wu, Caiqing
Huang, Haishun
Zhao, Ling
Zhuo, Yehong
Li, Yiqing
Selective deletion of zinc transporter 3 in amacrine cells promotes retinal ganglion cell survival and optic nerve regeneration after injury
title Selective deletion of zinc transporter 3 in amacrine cells promotes retinal ganglion cell survival and optic nerve regeneration after injury
title_full Selective deletion of zinc transporter 3 in amacrine cells promotes retinal ganglion cell survival and optic nerve regeneration after injury
title_fullStr Selective deletion of zinc transporter 3 in amacrine cells promotes retinal ganglion cell survival and optic nerve regeneration after injury
title_full_unstemmed Selective deletion of zinc transporter 3 in amacrine cells promotes retinal ganglion cell survival and optic nerve regeneration after injury
title_short Selective deletion of zinc transporter 3 in amacrine cells promotes retinal ganglion cell survival and optic nerve regeneration after injury
title_sort selective deletion of zinc transporter 3 in amacrine cells promotes retinal ganglion cell survival and optic nerve regeneration after injury
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10358645/
https://www.ncbi.nlm.nih.gov/pubmed/37449644
http://dx.doi.org/10.4103/1673-5374.373660
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