Change of voltage-gated sodium channel repertoire in skeletal muscle of a MuSK myasthenia gravis mouse model

Olena Butenko; Stine Marie Jensen; Yvonne E Fillié-Grijpma; Robyn Verpalen; Jan J Verschuuren; Silvère M van der Maarel; Maartje G Huijbers; Jaap J Plomp

doi:10.1111/ejn.16347

Change of voltage-gated sodium channel repertoire in skeletal muscle of a MuSK myasthenia gravis mouse model

Eur J Neurosci. 2024 Apr 22. doi: 10.1111/ejn.16347. Online ahead of print.

Authors

Olena Butenko¹, Stine Marie Jensen¹, Yvonne E Fillié-Grijpma¹, Robyn Verpalen¹, Jan J Verschuuren², Silvère M van der Maarel¹, Maartje G Huijbers^{1

2}, Jaap J Plomp²

Affiliations

¹ Department of Human Genetics, Leiden University Medical Center, Leiden, The Netherlands.
² Department of Neurology, Leiden University Medical Center, Leiden, The Netherlands.

PMID: 38650308
DOI: 10.1111/ejn.16347

Abstract

Muscle-specific kinase myasthenia gravis (MuSK MG) is caused by autoantibodies against MuSK in the neuromuscular junction (NMJ). MuSK MG patients have fluctuating, fatigable skeletal muscle weakness, in particular of bulbar muscles. Severity differs greatly between patients, in spite of comparable autoantibody levels. One explanation for inter-patient and inter-muscle variability in sensitivity might be variations in compensatory muscle responses. Previously, we developed a passive transfer mouse model for MuSK MG. In preliminary ex vivo experiments, we observed that muscle contraction of some mice, in particular those with milder myasthenia, had become partially insensitive to inhibition by μ-Conotoxin-GIIIB, a blocker of skeletal muscle Na_V1.4 voltage-gated sodium channels. We hypothesised that changes in Na_V channel expression profile, possibly co-expression of (μ-Conotoxin-GIIIB insensitive) Na_V1.5 type channels, might lower the muscle fibre's firing threshold and facilitate neuromuscular synaptic transmission. To test this hypothesis, we here performed passive transfer in immuno-compromised mice, using 'high', 'intermediate' and 'low' dosing regimens of purified MuSK MG patient IgG4. We compared myasthenia levels, μ-Conotoxin-GIIIB resistance and muscle fibre action potential characteristics and firing thresholds. High- and intermediate-dosed mice showed clear, progressive myasthenia, not seen in low-dosed animals. However, diaphragm NMJ electrophysiology demonstrated almost equal myasthenic severities amongst all regimens. Nonetheless, low-dosed mouse diaphragms showed a much higher degree of μ-Conotoxin-GIIIB resistance. This was not explained by upregulation of Scn5a (the Na_V1.5 gene), lowered muscle fibre firing thresholds or histologically detectable upregulated Na_V1.5 channels. It remains to be established which factors are responsible for the observed μ-Conotoxin-GIIIB insensitivity and whether the Na_V repertoire change is compensatory beneficial or a bystander effect.

Keywords: MuSK; NaV channels; homeostasis; myasthenia gravis; neuromuscular junction; passive transfer.

Grants and funding

W.OR17-13/Prinses Beatrix Spierfonds