What does this research mean for the field?

Neuromuscular junction (NMJ) dysfunction is present in a specific subset of Charcot-Marie Tooth (CMT) disease mouse models, indicating that NMJ-targeted therapies may benefit certain CMT patient populations. Novelty: ClaimNovelty.INCREMENTAL. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

The aim is to explore neuromuscular junction (NMJ) dysfunction in various mouse models of Charcot-Marie Tooth (CMT) disease.

May 19, 2026Open Access

Neuromuscular junction dysfunction in a subset of Charcot-Marie Tooth and related peripheral neuropathies mouse models

Key Points

The aim is to explore neuromuscular junction (NMJ) dysfunction in various mouse models of Charcot-Marie Tooth (CMT) disease.
Investigated eight CMT subtypes for NMJ phenotypes using mouse models.
Assessed morphological and functional deficits through electromyography (EMG).
Examined multiple models including Gjb1, Yars1, Ighmbp2, and PMP22 for NMJ abnormalities.
Gars +/ΔETAQ mice displayed robust synaptic deficits with reduced EMG function.
Nadk2 S330P/S330P mice exhibited an EMG phenotype that coincided with symptom onset.
Nefl +/N98S mice showed normal EMG but had dysmorphic pre-synaptic axon terminals.

Abstract

Charcot-Marie Tooth (CMT) disease is a clinically and genetically heterogeneous inherited peripheral neuropathy for which there is no treatment. CMT patients often present with weakness, fatigue, and muscle atrophy in the distal limbs. Improving function at the neuromuscular junction (NMJ) may improve function in some CMT patients. Using mouse models, we investigated eight CMT subtypes for NMJ phenotypes by morphology and functional deficits assessed by electromyography (EMG). We did not find NMJ abnormalities in mice with mutations in Gjb1 Y/Δ2 (CMT1X), or Yars1 E196K/E196K (diCMTC). Mice with mutations in Ighmbp2 Y918S/Y918S (CMT2S) and Pla2g6 M1J/M1J (Infantile Neuroaxonal Dystrophy) have neuromuscular phenotypes that could imply NMJ dysfunction, but we did not find defects in synaptic transmission or anatomy. A transgenic model of PMP22 overexpression (CMT1A) had EMG deficits with high frequency stimulation that are consistent with NMJ involvement. Three models showed indications of altered NMJ morphology and/or function. Gars +/ΔETAQ mice, modeling CMT2D, displayed robust synaptic deficits morphologically and by EMG. Nadk2 S330P/S330P mice , modeling an ultrarare neuromuscular disease, had an EMG phenotype coinciding with symptom onset. Nefl +/N98S mice, modeling CMT2E, had normal EMG; but pre-synaptic axon terminals were dysmorphic, with large varicosities, which were more pronounced in proximal muscles. Across multiple models, we found that the extensor digitorum longus was resistant to disease phenotypes based on NMJ innervation status and/or muscle weight and atrophy. Our results indicate that some subtypes of CMT have NMJ deficits, and that assessing neuromuscular disease patients for NMJ dysfunction may reveal a population that could benefit from therapies that enhance transmission. • NMJ dysfunction is found in subset of CMT mouse models. • NMJs may be a therapeutic target for some CMT patients. • NMJ defects may arise in CMTs associated with mitochondrial involvement.

Neuromuscular junction dysfunction in a subset of Charcot-Marie Tooth and related peripheral neuropathies mouse models

Key Points

Abstract

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