Neuronal deletion of MnSOD in mice leads to demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis

Shylesh Bhaskaran; Gaurav Kumar; Nidheesh Thadathil; Katarzyna M. Piekarz; Sabira Mohammed; Sergio Dominguez Lopez; Rizwan Qaisar; Dorothy Walton; Jacob L. Brown; Ashley Murphy; Nataliya Smith; Debra Saunders; Michael J. Beckstead; Scott Plafker; Tommy L. Lewis; Rheal Towner; Sathyaseelan S. Deepa; Arlan Richardson; Robert C. Axtell; Holly Van Remmen

doi:10.1016/j.redox.2022.102550

Neuronal deletion of MnSOD in mice leads to demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis

Shylesh Bhaskaran
, Gaurav Kumar
, Nidheesh Thadathil
, Katarzyna M. Piekarz
, Sabira Mohammed
, Sergio Dominguez Lopez
, Rizwan Qaisar
, Dorothy Walton
, Jacob L. Brown
, Ashley Murphy
, Nataliya Smith
, Debra Saunders
, Michael J. Beckstead
, Scott Plafker
, Tommy L. Lewis
, Rheal Towner
, Sathyaseelan S. Deepa
, Arlan Richardson
, Robert C. Axtell
, Holly Van Remmen

Pharmacology and Toxicology

University at Buffalo

Oklahoma Medical Research Foundation
University of Oklahoma
Department of Veterans Affairs

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

31 Scopus citations

Abstract

Neuronal oxidative stress has been implicated in aging and neurodegenerative disease. Here we investigated the impact of elevated oxidative stress induced in mouse spinal cord by deletion of Mn-Superoxide dismutase (MnSOD) using a neuron specific Cre recombinase in Sod2 floxed mice (i-mn-Sod2 KO). Sod2 deletion in spinal cord neurons was associated with mitochondrial alterations and peroxide generation. Phenotypically, i-mn-Sod2 KO mice experienced hindlimb paralysis and clasping behavior associated with extensive demyelination and reduced nerve conduction velocity, axonal degeneration, enhanced blood brain barrier permeability, elevated inflammatory cytokines, microglia activation, infiltration of neutrophils and necroptosis in spinal cord. In contrast, spinal cord motor neuron number, innervation of neuromuscular junctions, muscle mass, and contractile function were not altered. Overall, our findings show that loss of MnSOD in spinal cord promotes a phenotype of demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis.

Original language	English
Article number	102550
Journal	Redox Biology
Volume	59
DOIs	https://doi.org/10.1016/j.redox.2022.102550
State	Published - Feb 2023

Keywords

Demyelination
Inflammation
Mitochondria
Mn superoxide dismutase
Multiple sclerosis
Necroptosis
Neurons

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10.1016/j.redox.2022.102550

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Bhaskaran, S., Kumar, G., Thadathil, N., Piekarz, K. M., Mohammed, S., Lopez, S. D., Qaisar, R., Walton, D., Brown, J. L., Murphy, A., Smith, N., Saunders, D., Beckstead, M. J., Plafker, S., Lewis, T. L., Towner, R., Deepa, S. S., Richardson, A., Axtell, R. C., & Van Remmen, H. (2023). Neuronal deletion of MnSOD in mice leads to demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis. Redox Biology, 59, Article 102550. https://doi.org/10.1016/j.redox.2022.102550

@article{d35e50d41731442885f38a8914e08c76,

title = "Neuronal deletion of MnSOD in mice leads to demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis",

abstract = "Neuronal oxidative stress has been implicated in aging and neurodegenerative disease. Here we investigated the impact of elevated oxidative stress induced in mouse spinal cord by deletion of Mn-Superoxide dismutase (MnSOD) using a neuron specific Cre recombinase in Sod2 floxed mice (i-mn-Sod2 KO). Sod2 deletion in spinal cord neurons was associated with mitochondrial alterations and peroxide generation. Phenotypically, i-mn-Sod2 KO mice experienced hindlimb paralysis and clasping behavior associated with extensive demyelination and reduced nerve conduction velocity, axonal degeneration, enhanced blood brain barrier permeability, elevated inflammatory cytokines, microglia activation, infiltration of neutrophils and necroptosis in spinal cord. In contrast, spinal cord motor neuron number, innervation of neuromuscular junctions, muscle mass, and contractile function were not altered. Overall, our findings show that loss of MnSOD in spinal cord promotes a phenotype of demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis.",

keywords = "Demyelination, Inflammation, Mitochondria, Mn superoxide dismutase, Multiple sclerosis, Necroptosis, Neurons",

author = "Shylesh Bhaskaran and Gaurav Kumar and Nidheesh Thadathil and Piekarz, \{Katarzyna M.\} and Sabira Mohammed and Lopez, \{Sergio Dominguez\} and Rizwan Qaisar and Dorothy Walton and Brown, \{Jacob L.\} and Ashley Murphy and Nataliya Smith and Debra Saunders and Beckstead, \{Michael J.\} and Scott Plafker and Lewis, \{Tommy L.\} and Rheal Towner and Deepa, \{Sathyaseelan S.\} and Arlan Richardson and Axtell, \{Robert C.\} and \{Van Remmen\}, Holly",

note = "Publisher Copyright: {\textcopyright} 2022 The Authors",

year = "2023",

month = feb,

doi = "10.1016/j.redox.2022.102550",

language = "English",

volume = "59",

journal = "Redox Biology",

issn = "2213-2317",

publisher = "Elsevier B.V.",

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Bhaskaran, S, Kumar, G, Thadathil, N, Piekarz, KM, Mohammed, S, Lopez, SD, Qaisar, R, Walton, D, Brown, JL, Murphy, A, Smith, N, Saunders, D, Beckstead, MJ, Plafker, S, Lewis, TL, Towner, R, Deepa, SS, Richardson, A, Axtell, RC & Van Remmen, H 2023, 'Neuronal deletion of MnSOD in mice leads to demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis', Redox Biology, vol. 59, 102550. https://doi.org/10.1016/j.redox.2022.102550

TY - JOUR

T1 - Neuronal deletion of MnSOD in mice leads to demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis

AU - Bhaskaran, Shylesh

AU - Kumar, Gaurav

AU - Thadathil, Nidheesh

AU - Piekarz, Katarzyna M.

AU - Mohammed, Sabira

AU - Lopez, Sergio Dominguez

AU - Qaisar, Rizwan

AU - Walton, Dorothy

AU - Brown, Jacob L.

AU - Murphy, Ashley

AU - Smith, Nataliya

AU - Saunders, Debra

AU - Beckstead, Michael J.

AU - Plafker, Scott

AU - Lewis, Tommy L.

AU - Towner, Rheal

AU - Deepa, Sathyaseelan S.

AU - Richardson, Arlan

AU - Axtell, Robert C.

AU - Van Remmen, Holly

PY - 2023/2

Y1 - 2023/2

N2 - Neuronal oxidative stress has been implicated in aging and neurodegenerative disease. Here we investigated the impact of elevated oxidative stress induced in mouse spinal cord by deletion of Mn-Superoxide dismutase (MnSOD) using a neuron specific Cre recombinase in Sod2 floxed mice (i-mn-Sod2 KO). Sod2 deletion in spinal cord neurons was associated with mitochondrial alterations and peroxide generation. Phenotypically, i-mn-Sod2 KO mice experienced hindlimb paralysis and clasping behavior associated with extensive demyelination and reduced nerve conduction velocity, axonal degeneration, enhanced blood brain barrier permeability, elevated inflammatory cytokines, microglia activation, infiltration of neutrophils and necroptosis in spinal cord. In contrast, spinal cord motor neuron number, innervation of neuromuscular junctions, muscle mass, and contractile function were not altered. Overall, our findings show that loss of MnSOD in spinal cord promotes a phenotype of demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis.

AB - Neuronal oxidative stress has been implicated in aging and neurodegenerative disease. Here we investigated the impact of elevated oxidative stress induced in mouse spinal cord by deletion of Mn-Superoxide dismutase (MnSOD) using a neuron specific Cre recombinase in Sod2 floxed mice (i-mn-Sod2 KO). Sod2 deletion in spinal cord neurons was associated with mitochondrial alterations and peroxide generation. Phenotypically, i-mn-Sod2 KO mice experienced hindlimb paralysis and clasping behavior associated with extensive demyelination and reduced nerve conduction velocity, axonal degeneration, enhanced blood brain barrier permeability, elevated inflammatory cytokines, microglia activation, infiltration of neutrophils and necroptosis in spinal cord. In contrast, spinal cord motor neuron number, innervation of neuromuscular junctions, muscle mass, and contractile function were not altered. Overall, our findings show that loss of MnSOD in spinal cord promotes a phenotype of demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis.

KW - Demyelination

KW - Inflammation

KW - Mitochondria

KW - Mn superoxide dismutase

KW - Multiple sclerosis

KW - Necroptosis

KW - Neurons

UR - https://www.scopus.com/pages/publications/85143319524

U2 - 10.1016/j.redox.2022.102550

DO - 10.1016/j.redox.2022.102550

M3 - Article

C2 - 36470129

SN - 2213-2317

VL - 59

JO - Redox Biology

JF - Redox Biology

M1 - 102550

ER -

Neuronal deletion of MnSOD in mice leads to demyelination, inflammation and progressive paralysis that mimics phenotypes associated with progressive multiple sclerosis

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