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. 2019 Feb;139:63-68.
doi: 10.1016/j.neures.2018.08.016. Epub 2018 Sep 5.

Inhibition of Collapsin Response Mediator protein-2 Phosphorylation Ameliorates Motor Phenotype of ALS Model Mice Expressing SOD1G93A

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Inhibition of Collapsin Response Mediator protein-2 Phosphorylation Ameliorates Motor Phenotype of ALS Model Mice Expressing SOD1G93A

Yurika Numata-Uematsu et al. Neurosci Res. .

Abstract

Amyotrophic lateral sclerosis (ALS) is an adult-onset neurological disease characterized by the selective degeneration of motor neurons leading to paralysis and immobility. Missense mutations in the gene coding for the Cu2+/Zn2+ superoxide dismutase 1 (SOD1) accounts for 15-20% of familial ALS, and mice overexpressing ALS-linked SOD1 mutants have been frequently used as an animal model for ALS. Degeneration of motor neurons in ALS progresses in a manner called "dying back", in which the degeneration of synapses and axons precedes the loss of cell bodies. Phosphorylation of collapsin response mediator protein 2 (CRMP2) is implicated in the progression of neuronal/axonal degeneration of different etiologies. To evaluate the role of CRMP2 phosphorylation in ALS pathogenesis, we utilized CRMP2 S522A knock-in (CRMP2ki/ki) mice, in which the serine residue 522 was homozygously replaced with alanine and thereby making CRMP2 no longer phosphorylatable by CDK5 or GSK3B. We found that the CRMP2ki/ki/SOD1G93A mice showed delay in the progression of the motor phenotype compared to their SOD1G93-Tg littermates. Histological analysis revealed that the CRMP2ki/ki/SOD1G93A mice retained more intact axons and NMJs than their SOD1G93A-Tg littermates. These results suggest that the phosphorylation of CRMP2 may contribute to the axonal degeneration of motor neurons in ALS.

Keywords: ALS; Axonal degeneration; CRMP2; Neuromuscular junction.

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