Optogenetic spinal stimulation promotes new axonal growth and skilled forelimb recovery in rats with sub-chronic cervical spinal cord injury

Sarah E Mondello; Lisa Young; Viet Dang; Amanda E Fischedick; Nicholas M Tolley; Tian Wang; Madison A Bravo; Dalton Lee; Belinda Tucker; Megan Knoernschild; Benjamin D Pedigo; Philip J Horner; Chet Moritz

doi:10.1088/1741-2552/acec13

Optogenetic spinal stimulation promotes new axonal growth and skilled forelimb recovery in rats with sub-chronic cervical spinal cord injury

Sarah E Mondello, Lisa Young, Viet Dang, Amanda E Fischedick, Nicholas M Tolley, Tian Wang, Madison A Bravo, Dalton Lee, Belinda Tucker, Megan Knoernschild, Benjamin D Pedigo, Philip J Horner, Chet Moritz

Research output: Contribution to journal › Article

2 Scopus citations

Abstract

Objective. Spinal cord injury (SCI) leads to debilitating sensorimotor deficits that greatly limit quality of life. This work aims to develop a mechanistic understanding of how to best promote functional recovery following SCI. Electrical spinal stimulation is one promising approach that is effective in both animal models and humans with SCI. Optogenetic stimulation is an alternative method of stimulating the spinal cord that allows for cell-type-specific stimulation. The present work investigates the effects of preferentially stimulating neurons within the spinal cord and not glial cells, termed ‘neuron-specific’ optogenetic spinal stimulation. We examined forelimb recovery, axonal growth, and vasculature after optogenetic or sham stimulation in rats with cervical SCI. Approach. Adult female rats received a moderate cervical hemicontusion followed by the injection of a neuron-specific optogenetic viral vector ipsilateral and caudal to the lesion site. Animals then began rehabilitation on the skilled forelimb reaching task. At four weeks post-injury, rats received a micro-light emitting diode (µLED) implant to optogenetically stimulate the caudal spinal cord. Stimulation began at six weeks post-injury and occurred in conjunction with activities to promote use of the forelimbs. Following six weeks of stimulation, rats were perfused, and tissue stained for GAP-43, laminin, Nissl bodies and myelin. Location of viral transduction and transduced cell types were also assessed. Main Results. Our results demonstrate that neuron-specific optogenetic spinal stimulation significantly enhances recovery of skilled forelimb reaching. We also found significantly more GAP-43 and laminin labeling in the optogenetically stimulated groups indicating stimulation promotes axonal growth and angiogenesis. Significance. These findings indicate that optogenetic stimulation is a robust neuromodulator that could enable future therapies and investigations into the role of specific cell types, pathways, and neuronal populations in supporting recovery after SCI.

Original language	English (US)
Article number	056005
Journal	Journal of neural engineering
Volume	20
Issue number	5
Early online date	Jul 31 2023
DOIs	https://doi.org/10.1088/1741-2552/acec13
State	Published - Sep 12 2023

Keywords

angiogenesis
axonal growth
forelimb rehabilitation
optogenetics
spinal cord injury
Humans
GAP-43 Protein
Recovery of Function/physiology
Rats
Optogenetics
Cervical Cord
Animals
Laminin
Spinal Cord Injuries
Spinal Cord
Quality of Life
Female
Forelimb/pathology

ASJC Scopus subject areas

Cellular and Molecular Neuroscience
Biomedical Engineering

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10.1088/1741-2552/acec13

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Mondello, S. E., Young, L., Dang, V., Fischedick, A. E., Tolley, N. M., Wang, T., Bravo, M. A., Lee, D., Tucker, B., Knoernschild, M., Pedigo, B. D., Horner, P. J., & Moritz, C. (2023). Optogenetic spinal stimulation promotes new axonal growth and skilled forelimb recovery in rats with sub-chronic cervical spinal cord injury. Journal of neural engineering, 20(5), Article 056005. https://doi.org/10.1088/1741-2552/acec13

Mondello, SE, Young, L, Dang, V, Fischedick, AE, Tolley, NM, Wang, T, Bravo, MA, Lee, D, Tucker, B, Knoernschild, M, Pedigo, BD, Horner, PJ & Moritz, C 2023, 'Optogenetic spinal stimulation promotes new axonal growth and skilled forelimb recovery in rats with sub-chronic cervical spinal cord injury', Journal of neural engineering, vol. 20, no. 5, 056005. https://doi.org/10.1088/1741-2552/acec13

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title = "Optogenetic spinal stimulation promotes new axonal growth and skilled forelimb recovery in rats with sub-chronic cervical spinal cord injury",

abstract = "Objective. Spinal cord injury (SCI) leads to debilitating sensorimotor deficits that greatly limit quality of life. This work aims to develop a mechanistic understanding of how to best promote functional recovery following SCI. Electrical spinal stimulation is one promising approach that is effective in both animal models and humans with SCI. Optogenetic stimulation is an alternative method of stimulating the spinal cord that allows for cell-type-specific stimulation. The present work investigates the effects of preferentially stimulating neurons within the spinal cord and not glial cells, termed {\textquoteleft}neuron-specific{\textquoteright} optogenetic spinal stimulation. We examined forelimb recovery, axonal growth, and vasculature after optogenetic or sham stimulation in rats with cervical SCI. Approach. Adult female rats received a moderate cervical hemicontusion followed by the injection of a neuron-specific optogenetic viral vector ipsilateral and caudal to the lesion site. Animals then began rehabilitation on the skilled forelimb reaching task. At four weeks post-injury, rats received a micro-light emitting diode (µLED) implant to optogenetically stimulate the caudal spinal cord. Stimulation began at six weeks post-injury and occurred in conjunction with activities to promote use of the forelimbs. Following six weeks of stimulation, rats were perfused, and tissue stained for GAP-43, laminin, Nissl bodies and myelin. Location of viral transduction and transduced cell types were also assessed. Main Results. Our results demonstrate that neuron-specific optogenetic spinal stimulation significantly enhances recovery of skilled forelimb reaching. We also found significantly more GAP-43 and laminin labeling in the optogenetically stimulated groups indicating stimulation promotes axonal growth and angiogenesis. Significance. These findings indicate that optogenetic stimulation is a robust neuromodulator that could enable future therapies and investigations into the role of specific cell types, pathways, and neuronal populations in supporting recovery after SCI.",

keywords = "angiogenesis, axonal growth, forelimb rehabilitation, optogenetics, spinal cord injury, Humans, GAP-43 Protein, Recovery of Function/physiology, Rats, Optogenetics, Cervical Cord, Animals, Laminin, Spinal Cord Injuries, Spinal Cord, Quality of Life, Female, Forelimb/pathology",

author = "Mondello, {Sarah E} and Lisa Young and Viet Dang and Fischedick, {Amanda E} and Tolley, {Nicholas M} and Tian Wang and Bravo, {Madison A} and Dalton Lee and Belinda Tucker and Megan Knoernschild and Pedigo, {Benjamin D} and Horner, {Philip J} and Chet Moritz",

note = "Funding Information: This study was funded by the Craig H Neilsen Foundation Pilot Grant (476694), Morton Cure Paralysis Fund, NIH/NINDS R01NS115025, The Center for Neurotechnology, and the Christopher and Dana Reeve Foundation International Consortium on Spinal Cord Repair. We would like to acknowledge Diana Dang for assisting with video analysis, Cleah Winston and Ria Bahadur for assisting with tissue quantification, and Jared Pradarelli for helping design figure artwork. Publisher Copyright: {\textcopyright} 2023 The Author(s). Published by IOP Publishing Ltd.",

year = "2023",

month = sep,

day = "12",

doi = "10.1088/1741-2552/acec13",

language = "English (US)",

volume = "20",

journal = "Journal of neural engineering",

issn = "1741-2560",

publisher = "IOP Publishing Ltd.",

number = "5",

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TY - JOUR

T1 - Optogenetic spinal stimulation promotes new axonal growth and skilled forelimb recovery in rats with sub-chronic cervical spinal cord injury

AU - Mondello, Sarah E

AU - Young, Lisa

AU - Dang, Viet

AU - Fischedick, Amanda E

AU - Tolley, Nicholas M

AU - Wang, Tian

AU - Bravo, Madison A

AU - Lee, Dalton

AU - Tucker, Belinda

AU - Knoernschild, Megan

AU - Pedigo, Benjamin D

AU - Horner, Philip J

AU - Moritz, Chet

N1 - Funding Information: This study was funded by the Craig H Neilsen Foundation Pilot Grant (476694), Morton Cure Paralysis Fund, NIH/NINDS R01NS115025, The Center for Neurotechnology, and the Christopher and Dana Reeve Foundation International Consortium on Spinal Cord Repair. We would like to acknowledge Diana Dang for assisting with video analysis, Cleah Winston and Ria Bahadur for assisting with tissue quantification, and Jared Pradarelli for helping design figure artwork. Publisher Copyright: © 2023 The Author(s). Published by IOP Publishing Ltd.

PY - 2023/9/12

Y1 - 2023/9/12

N2 - Objective. Spinal cord injury (SCI) leads to debilitating sensorimotor deficits that greatly limit quality of life. This work aims to develop a mechanistic understanding of how to best promote functional recovery following SCI. Electrical spinal stimulation is one promising approach that is effective in both animal models and humans with SCI. Optogenetic stimulation is an alternative method of stimulating the spinal cord that allows for cell-type-specific stimulation. The present work investigates the effects of preferentially stimulating neurons within the spinal cord and not glial cells, termed ‘neuron-specific’ optogenetic spinal stimulation. We examined forelimb recovery, axonal growth, and vasculature after optogenetic or sham stimulation in rats with cervical SCI. Approach. Adult female rats received a moderate cervical hemicontusion followed by the injection of a neuron-specific optogenetic viral vector ipsilateral and caudal to the lesion site. Animals then began rehabilitation on the skilled forelimb reaching task. At four weeks post-injury, rats received a micro-light emitting diode (µLED) implant to optogenetically stimulate the caudal spinal cord. Stimulation began at six weeks post-injury and occurred in conjunction with activities to promote use of the forelimbs. Following six weeks of stimulation, rats were perfused, and tissue stained for GAP-43, laminin, Nissl bodies and myelin. Location of viral transduction and transduced cell types were also assessed. Main Results. Our results demonstrate that neuron-specific optogenetic spinal stimulation significantly enhances recovery of skilled forelimb reaching. We also found significantly more GAP-43 and laminin labeling in the optogenetically stimulated groups indicating stimulation promotes axonal growth and angiogenesis. Significance. These findings indicate that optogenetic stimulation is a robust neuromodulator that could enable future therapies and investigations into the role of specific cell types, pathways, and neuronal populations in supporting recovery after SCI.

AB - Objective. Spinal cord injury (SCI) leads to debilitating sensorimotor deficits that greatly limit quality of life. This work aims to develop a mechanistic understanding of how to best promote functional recovery following SCI. Electrical spinal stimulation is one promising approach that is effective in both animal models and humans with SCI. Optogenetic stimulation is an alternative method of stimulating the spinal cord that allows for cell-type-specific stimulation. The present work investigates the effects of preferentially stimulating neurons within the spinal cord and not glial cells, termed ‘neuron-specific’ optogenetic spinal stimulation. We examined forelimb recovery, axonal growth, and vasculature after optogenetic or sham stimulation in rats with cervical SCI. Approach. Adult female rats received a moderate cervical hemicontusion followed by the injection of a neuron-specific optogenetic viral vector ipsilateral and caudal to the lesion site. Animals then began rehabilitation on the skilled forelimb reaching task. At four weeks post-injury, rats received a micro-light emitting diode (µLED) implant to optogenetically stimulate the caudal spinal cord. Stimulation began at six weeks post-injury and occurred in conjunction with activities to promote use of the forelimbs. Following six weeks of stimulation, rats were perfused, and tissue stained for GAP-43, laminin, Nissl bodies and myelin. Location of viral transduction and transduced cell types were also assessed. Main Results. Our results demonstrate that neuron-specific optogenetic spinal stimulation significantly enhances recovery of skilled forelimb reaching. We also found significantly more GAP-43 and laminin labeling in the optogenetically stimulated groups indicating stimulation promotes axonal growth and angiogenesis. Significance. These findings indicate that optogenetic stimulation is a robust neuromodulator that could enable future therapies and investigations into the role of specific cell types, pathways, and neuronal populations in supporting recovery after SCI.

KW - angiogenesis

KW - axonal growth

KW - forelimb rehabilitation

KW - optogenetics

KW - spinal cord injury

KW - Humans

KW - GAP-43 Protein

KW - Recovery of Function/physiology

KW - Rats

KW - Optogenetics

KW - Cervical Cord

KW - Animals

KW - Laminin

KW - Spinal Cord Injuries

KW - Spinal Cord

KW - Quality of Life

KW - Female

KW - Forelimb/pathology

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DO - 10.1088/1741-2552/acec13

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VL - 20

JO - Journal of neural engineering

JF - Journal of neural engineering

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ER -

Optogenetic spinal stimulation promotes new axonal growth and skilled forelimb recovery in rats with sub-chronic cervical spinal cord injury

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