Knocking Out Non-muscle Myosin II in Retinal Ganglion Cells Promotes Long-Distance Optic Nerve Regeneration

Xue Wei Wang; Shu Guang Yang; Chi Zhang; Ming Wen Hu; Jiang Qian; Jin Jin Ma; Yingchi Zhang; Bin Bin Yang; Yi Lan Weng; Guo Li Ming; Anish R. Kosanam; Saijilafu; Feng Quan Zhou

doi:10.1016/j.celrep.2020.107537

Knocking Out Non-muscle Myosin II in Retinal Ganglion Cells Promotes Long-Distance Optic Nerve Regeneration

Xue Wei Wang, Shu Guang Yang, Chi Zhang, Ming Wen Hu, Jiang Qian, Jin Jin Ma, Yingchi Zhang, Bin Bin Yang, Yi Lan Weng, Guo Li Ming, Anish R. Kosanam, Saijilafu, Feng Quan Zhou

Research output: Contribution to journal › Article › peer-review

27 Scopus citations

Abstract

In addition to altered gene expression, pathological cytoskeletal dynamics in the axon are another key intrinsic barrier for axon regeneration in the central nervous system (CNS). Here, we show that knocking out myosin IIA and IIB (myosin IIA/B) in retinal ganglion cells alone, either before or after optic nerve crush, induces significant optic nerve regeneration. Combined Lin28a overexpression and myosin IIA/B knockout lead to an additive promoting effect and long-distance axon regeneration. Immunostaining, RNA sequencing, and western blot analyses reveal that myosin II deletion does not affect known axon regeneration signaling pathways or the expression of regeneration-associated genes. Instead, it abolishes the retraction bulb formation and significantly enhances the axon extension efficiency. The study provides clear evidence that directly targeting neuronal cytoskeleton is sufficient to induce significant CNS axon regeneration and that combining altered gene expression in the soma and modified cytoskeletal dynamics in the axon is a promising approach for long-distance CNS axon regeneration.

Original language	English (US)
Article number	107537
Pages (from-to)	107537
Journal	Cell Reports
Volume	31
Issue number	3
DOIs	https://doi.org/10.1016/j.celrep.2020.107537
State	Published - Apr 21 2020

Keywords

Lin28
axon regeneration
cytoskeleton
growth cone
non-muscle myosin II
optic nerve regeneration
post-injury treatment
retinal ganglion cells
retraction bulb

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

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10.1016/j.celrep.2020.107537

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@article{9afa9f8467694919b477fb2d7c73dcf3,

title = "Knocking Out Non-muscle Myosin II in Retinal Ganglion Cells Promotes Long-Distance Optic Nerve Regeneration",

abstract = "In addition to altered gene expression, pathological cytoskeletal dynamics in the axon are another key intrinsic barrier for axon regeneration in the central nervous system (CNS). Here, we show that knocking out myosin IIA and IIB (myosin IIA/B) in retinal ganglion cells alone, either before or after optic nerve crush, induces significant optic nerve regeneration. Combined Lin28a overexpression and myosin IIA/B knockout lead to an additive promoting effect and long-distance axon regeneration. Immunostaining, RNA sequencing, and western blot analyses reveal that myosin II deletion does not affect known axon regeneration signaling pathways or the expression of regeneration-associated genes. Instead, it abolishes the retraction bulb formation and significantly enhances the axon extension efficiency. The study provides clear evidence that directly targeting neuronal cytoskeleton is sufficient to induce significant CNS axon regeneration and that combining altered gene expression in the soma and modified cytoskeletal dynamics in the axon is a promising approach for long-distance CNS axon regeneration.",

keywords = "Lin28, axon regeneration, cytoskeleton, growth cone, non-muscle myosin II, optic nerve regeneration, post-injury treatment, retinal ganglion cells, retraction bulb",

author = "Wang, {Xue Wei} and Yang, {Shu Guang} and Chi Zhang and Hu, {Ming Wen} and Jiang Qian and Ma, {Jin Jin} and Yingchi Zhang and Yang, {Bin Bin} and Weng, {Yi Lan} and Ming, {Guo Li} and Kosanam, {Anish R.} and Saijilafu and Zhou, {Feng Quan}",

note = "Funding Information: We acknowledge Dr. Michele Pucak from the Multiphoton Imaging Core (supported by NS050274) of the Department of Neuroscience, Johns Hopkins School of Medicine for her help in confocal microscopy. We thank Hao Zhang from the Flow Cytometry Cell Sorting Core Facility at Bloomberg School of Public Health, Johns Hopkins University for doing FACS sorting. The facility was supported by 1S10OD016315-01 and 1S10RR13777001 and, in part, by CFAR: 5P30AI094189-04 (Chaisson). We appreciate the Johns Hopkins Transcriptomics and Deep Sequencing Core for doing the RGC RNA-seq experiment. We also thank Ying Zhang for drawing the graphical abstract. The study was supported by grants (to F.-Q.Z. and J.Q.) from NIH (R01NS064288, R01NS085176, R01GM111514, R01EY027347, and R01EY029548), the Craig H. Neilsen Foundation (259450), and the BrightFocus Foundation (G2017037). S. was supported by the grants from the National Natural Science Foundation of China (81571189 and 81772353), the National Key Research and Development Program (2016YFC1100203), and Innovation and Entrepreneurship Program of Jiangsu Province. X.-W.W. S.-G.Y. S. and F.-Q.Z. conceived the study and designed the project; X.-W.W. and S.-G.Y. performed most of the experiments; X.-W.W. and C.Z. performed and analyzed the immunostaining and western blot experiments; M.-W.H. and J.Q. analyzed the RGC RNA-seq data; Y.Z. analyzed optic nerve regeneration; C.Z. and Y.Z. analyzed the axon morphologies and trajectories; J.-J.M. performed the DRG RNA-seq experiment; Y.-L.W. and G.-L.M. helped with the optic nerve regeneration experiments; B.-B.Y. and A.R.K. helped with the data analyses; X.-W.W. and F.-Q.Z. wrote the manuscript with contributions from all authors. The authors declare no competing financial interests. Funding Information: We acknowledge Dr. Michele Pucak from the Multiphoton Imaging Core (supported by NS050274) of the Department of Neuroscience, Johns Hopkins School of Medicine for her help in confocal microscopy. We thank Hao Zhang from the Flow Cytometry Cell Sorting Core Facility at Bloomberg School of Public Health, Johns Hopkins University for doing FACS sorting. The facility was supported by 1S10OD016315-01 and 1S10RR13777001 and, in part, by CFAR : 5P30AI094189-04 (Chaisson). We appreciate the Johns Hopkins Transcriptomics and Deep Sequencing Core for doing the RGC RNA-seq experiment. We also thank Ying Zhang for drawing the graphical abstract. The study was supported by grants (to F.-Q.Z. and J.Q.) from NIH ( R01NS064288 , R01NS085176 , R01GM111514 , R01EY027347 , and R01EY029548 ), the Craig H. Neilsen Foundation ( 259450 ), and the BrightFocus Foundation ( G2017037 ). S. was supported by the grants from the National Natural Science Foundation of China ( 81571189 and 81772353 ), the National Key Research and Development Program ( 2016YFC1100203 ), and Innovation and Entrepreneurship Program of Jiangsu Province . Publisher Copyright: {\textcopyright} 2020 The Author(s)",

year = "2020",

month = apr,

day = "21",

doi = "10.1016/j.celrep.2020.107537",

language = "English (US)",

volume = "31",

pages = "107537",

journal = "Cell Reports",

issn = "2211-1247",

publisher = "Cell Press",

number = "3",

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TY - JOUR

T1 - Knocking Out Non-muscle Myosin II in Retinal Ganglion Cells Promotes Long-Distance Optic Nerve Regeneration

AU - Wang, Xue Wei

AU - Yang, Shu Guang

AU - Zhang, Chi

AU - Hu, Ming Wen

AU - Qian, Jiang

AU - Ma, Jin Jin

AU - Zhang, Yingchi

AU - Yang, Bin Bin

AU - Weng, Yi Lan

AU - Ming, Guo Li

AU - Kosanam, Anish R.

AU - Saijilafu,

AU - Zhou, Feng Quan

N1 - Funding Information: We acknowledge Dr. Michele Pucak from the Multiphoton Imaging Core (supported by NS050274) of the Department of Neuroscience, Johns Hopkins School of Medicine for her help in confocal microscopy. We thank Hao Zhang from the Flow Cytometry Cell Sorting Core Facility at Bloomberg School of Public Health, Johns Hopkins University for doing FACS sorting. The facility was supported by 1S10OD016315-01 and 1S10RR13777001 and, in part, by CFAR: 5P30AI094189-04 (Chaisson). We appreciate the Johns Hopkins Transcriptomics and Deep Sequencing Core for doing the RGC RNA-seq experiment. We also thank Ying Zhang for drawing the graphical abstract. The study was supported by grants (to F.-Q.Z. and J.Q.) from NIH (R01NS064288, R01NS085176, R01GM111514, R01EY027347, and R01EY029548), the Craig H. Neilsen Foundation (259450), and the BrightFocus Foundation (G2017037). S. was supported by the grants from the National Natural Science Foundation of China (81571189 and 81772353), the National Key Research and Development Program (2016YFC1100203), and Innovation and Entrepreneurship Program of Jiangsu Province. X.-W.W. S.-G.Y. S. and F.-Q.Z. conceived the study and designed the project; X.-W.W. and S.-G.Y. performed most of the experiments; X.-W.W. and C.Z. performed and analyzed the immunostaining and western blot experiments; M.-W.H. and J.Q. analyzed the RGC RNA-seq data; Y.Z. analyzed optic nerve regeneration; C.Z. and Y.Z. analyzed the axon morphologies and trajectories; J.-J.M. performed the DRG RNA-seq experiment; Y.-L.W. and G.-L.M. helped with the optic nerve regeneration experiments; B.-B.Y. and A.R.K. helped with the data analyses; X.-W.W. and F.-Q.Z. wrote the manuscript with contributions from all authors. The authors declare no competing financial interests. Funding Information: We acknowledge Dr. Michele Pucak from the Multiphoton Imaging Core (supported by NS050274) of the Department of Neuroscience, Johns Hopkins School of Medicine for her help in confocal microscopy. We thank Hao Zhang from the Flow Cytometry Cell Sorting Core Facility at Bloomberg School of Public Health, Johns Hopkins University for doing FACS sorting. The facility was supported by 1S10OD016315-01 and 1S10RR13777001 and, in part, by CFAR : 5P30AI094189-04 (Chaisson). We appreciate the Johns Hopkins Transcriptomics and Deep Sequencing Core for doing the RGC RNA-seq experiment. We also thank Ying Zhang for drawing the graphical abstract. The study was supported by grants (to F.-Q.Z. and J.Q.) from NIH ( R01NS064288 , R01NS085176 , R01GM111514 , R01EY027347 , and R01EY029548 ), the Craig H. Neilsen Foundation ( 259450 ), and the BrightFocus Foundation ( G2017037 ). S. was supported by the grants from the National Natural Science Foundation of China ( 81571189 and 81772353 ), the National Key Research and Development Program ( 2016YFC1100203 ), and Innovation and Entrepreneurship Program of Jiangsu Province . Publisher Copyright: © 2020 The Author(s)

PY - 2020/4/21

Y1 - 2020/4/21

N2 - In addition to altered gene expression, pathological cytoskeletal dynamics in the axon are another key intrinsic barrier for axon regeneration in the central nervous system (CNS). Here, we show that knocking out myosin IIA and IIB (myosin IIA/B) in retinal ganglion cells alone, either before or after optic nerve crush, induces significant optic nerve regeneration. Combined Lin28a overexpression and myosin IIA/B knockout lead to an additive promoting effect and long-distance axon regeneration. Immunostaining, RNA sequencing, and western blot analyses reveal that myosin II deletion does not affect known axon regeneration signaling pathways or the expression of regeneration-associated genes. Instead, it abolishes the retraction bulb formation and significantly enhances the axon extension efficiency. The study provides clear evidence that directly targeting neuronal cytoskeleton is sufficient to induce significant CNS axon regeneration and that combining altered gene expression in the soma and modified cytoskeletal dynamics in the axon is a promising approach for long-distance CNS axon regeneration.

AB - In addition to altered gene expression, pathological cytoskeletal dynamics in the axon are another key intrinsic barrier for axon regeneration in the central nervous system (CNS). Here, we show that knocking out myosin IIA and IIB (myosin IIA/B) in retinal ganglion cells alone, either before or after optic nerve crush, induces significant optic nerve regeneration. Combined Lin28a overexpression and myosin IIA/B knockout lead to an additive promoting effect and long-distance axon regeneration. Immunostaining, RNA sequencing, and western blot analyses reveal that myosin II deletion does not affect known axon regeneration signaling pathways or the expression of regeneration-associated genes. Instead, it abolishes the retraction bulb formation and significantly enhances the axon extension efficiency. The study provides clear evidence that directly targeting neuronal cytoskeleton is sufficient to induce significant CNS axon regeneration and that combining altered gene expression in the soma and modified cytoskeletal dynamics in the axon is a promising approach for long-distance CNS axon regeneration.

KW - Lin28

KW - axon regeneration

KW - cytoskeleton

KW - growth cone

KW - non-muscle myosin II

KW - optic nerve regeneration

KW - post-injury treatment

KW - retinal ganglion cells

KW - retraction bulb

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DO - 10.1016/j.celrep.2020.107537

M3 - Article

C2 - 32320663

AN - SCOPUS:85083326747

SN - 2211-1247

VL - 31

SP - 107537

JO - Cell Reports

JF - Cell Reports

IS - 3

M1 - 107537

ER -

Knocking Out Non-muscle Myosin II in Retinal Ganglion Cells Promotes Long-Distance Optic Nerve Regeneration

Abstract

Keywords

ASJC Scopus subject areas

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