Proteolytic ectodomain shedding of muscle-specific tyrosine kinase in myasthenia gravis

Shuuichi Mori; Shigeaki Suzuki; Tetsuro Konishi; Naoki Kawaguchi; Masahiko Kishi; Satoshi Kuwabara; Kei Ishizuchi; Heying Zhou; Futoshi Shibasaki; Hiroki Tsumoto; Takuya Omura; Yuri Miura; Seijiro Mori; Mana Higashihara; Shigeo Murayama; Kazuhiro Shigemoto

doi:10.1016/j.expneurol.2022.114300

Proteolytic ectodomain shedding of muscle-specific tyrosine kinase in myasthenia gravis

Shuuichi Mori, Shigeaki Suzuki, Tetsuro Konishi, Naoki Kawaguchi, Masahiko Kishi, Satoshi Kuwabara, Kei Ishizuchi, Heying Zhou, Futoshi Shibasaki, Hiroki Tsumoto, Takuya Omura, Yuri Miura, Seijiro Mori, Mana Higashihara, Shigeo Murayama, Kazuhiro Shigemoto

Department of Internal Medicine (Neurology)

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

Abstract

Autoantibodies to muscle-specific tyrosine kinase (MuSK) proteins at the neuromuscular junction (NMJ) cause refractory generalized myasthenia gravis (MG) with dyspnea more frequently than other MG subtypes. However, the mechanisms via which MuSK, a membrane protein locally expressed on the NMJ of skeletal muscle, is supplied to the immune system as an autoantigen remains unknown. Here, we identified MuSK in both mouse and human serum, with the amount of MuSK dramatically increasing in mice with motor nerve denervation and in MG model mice. Peptide analysis by liquid chromatography-tandem-mass spectrometry (LC-MS/MS) confirmed the presence of MuSK in both human and mouse serum. Furthermore, some patients with MG have significantly higher amounts of MuSK in serum than healthy controls. Our results indicated that the secretion of MuSK proteins from muscles into the bloodstream was induced by ectodomain shedding triggered by neuromuscular junction failure. The results may explain why MuSK-MG is refractory to treatments and causes rapid muscle atrophy in some patients due to the denervation associated with Ab-induced disruption of neuromuscular transmission at the NMJ. Such discoveries pave the way for new MG treatments, and MuSK may be used as a biomarker for other neuromuscular diseases in preclinical studies, clinical diagnostics, therapeutics, and drug discovery.

Original language	English
Article number	114300
Journal	Experimental Neurology
Volume	361
DOIs	https://doi.org/10.1016/j.expneurol.2022.114300
Publication status	Published - 2023 Mar

Keywords

Animal model
Biomarker
Denervation
Extracellular domain
Mass spectrometry
Matrix protease
Muscle-specific kinase
Myasthenia gravis
Reinnervation
Shedding

ASJC Scopus subject areas

Neurology
Developmental Neuroscience

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.expneurol.2022.114300

Cite this

Mori, S., Suzuki, S., Konishi, T., Kawaguchi, N., Kishi, M., Kuwabara, S., Ishizuchi, K., Zhou, H., Shibasaki, F., Tsumoto, H., Omura, T., Miura, Y., Mori, S., Higashihara, M., Murayama, S., & Shigemoto, K. (2023). Proteolytic ectodomain shedding of muscle-specific tyrosine kinase in myasthenia gravis. Experimental Neurology, 361, [114300]. https://doi.org/10.1016/j.expneurol.2022.114300

Mori, S, Suzuki, S, Konishi, T, Kawaguchi, N, Kishi, M, Kuwabara, S, Ishizuchi, K, Zhou, H, Shibasaki, F, Tsumoto, H, Omura, T, Miura, Y, Mori, S, Higashihara, M, Murayama, S & Shigemoto, K 2023, 'Proteolytic ectodomain shedding of muscle-specific tyrosine kinase in myasthenia gravis', Experimental Neurology, vol. 361, 114300. https://doi.org/10.1016/j.expneurol.2022.114300

@article{bd50db434d854737b2f7e14d69f9cc97,

title = "Proteolytic ectodomain shedding of muscle-specific tyrosine kinase in myasthenia gravis",

abstract = "Autoantibodies to muscle-specific tyrosine kinase (MuSK) proteins at the neuromuscular junction (NMJ) cause refractory generalized myasthenia gravis (MG) with dyspnea more frequently than other MG subtypes. However, the mechanisms via which MuSK, a membrane protein locally expressed on the NMJ of skeletal muscle, is supplied to the immune system as an autoantigen remains unknown. Here, we identified MuSK in both mouse and human serum, with the amount of MuSK dramatically increasing in mice with motor nerve denervation and in MG model mice. Peptide analysis by liquid chromatography-tandem-mass spectrometry (LC-MS/MS) confirmed the presence of MuSK in both human and mouse serum. Furthermore, some patients with MG have significantly higher amounts of MuSK in serum than healthy controls. Our results indicated that the secretion of MuSK proteins from muscles into the bloodstream was induced by ectodomain shedding triggered by neuromuscular junction failure. The results may explain why MuSK-MG is refractory to treatments and causes rapid muscle atrophy in some patients due to the denervation associated with Ab-induced disruption of neuromuscular transmission at the NMJ. Such discoveries pave the way for new MG treatments, and MuSK may be used as a biomarker for other neuromuscular diseases in preclinical studies, clinical diagnostics, therapeutics, and drug discovery.",

keywords = "Animal model, Biomarker, Denervation, Extracellular domain, Mass spectrometry, Matrix protease, Muscle-specific kinase, Myasthenia gravis, Reinnervation, Shedding",

author = "Shuuichi Mori and Shigeaki Suzuki and Tetsuro Konishi and Naoki Kawaguchi and Masahiko Kishi and Satoshi Kuwabara and Kei Ishizuchi and Heying Zhou and Futoshi Shibasaki and Hiroki Tsumoto and Takuya Omura and Yuri Miura and Seijiro Mori and Mana Higashihara and Shigeo Murayama and Kazuhiro Shigemoto",

note = "Funding Information: We thank our patients for their trust. We thank S. Kubo for assistance with hybridoma screenings and preparation of antibodies, and are grateful to H. Kishida, K. Kawano, S. Iwata, and K. Tanaka for their assistance with experiments. We thank Y. Noda, R. Takashima, and the TMIG animal facility staff for their assistance with animal experiments. We thank Editage ( www.editage.com ) for English language editing. This work was supported by the Grant-in-Aid for Scientific Research ( 16K01851 , 19K11660 , 15K01743 , 21200023 , 21591102 , 24390228 , 25670437 , 16H03266 and 19H04064 ), Grant-in-Aid for Early-Career Scientist ( 20K19737 ), AMED Leap ( JP21mg00100007 ), Takeda Science Foundation , and Mitsui Sumitomo Insurance Welfare Foundation . Publisher Copyright: {\textcopyright} 2022",

year = "2023",

month = mar,

doi = "10.1016/j.expneurol.2022.114300",

language = "English",

volume = "361",

journal = "Neurodegeneration",

issn = "0014-4886",

publisher = "Academic Press Inc.",

}

TY - JOUR

T1 - Proteolytic ectodomain shedding of muscle-specific tyrosine kinase in myasthenia gravis

AU - Mori, Shuuichi

AU - Suzuki, Shigeaki

AU - Konishi, Tetsuro

AU - Kawaguchi, Naoki

AU - Kishi, Masahiko

AU - Kuwabara, Satoshi

AU - Ishizuchi, Kei

AU - Zhou, Heying

AU - Shibasaki, Futoshi

AU - Tsumoto, Hiroki

AU - Omura, Takuya

AU - Miura, Yuri

AU - Mori, Seijiro

AU - Higashihara, Mana

AU - Murayama, Shigeo

AU - Shigemoto, Kazuhiro

N1 - Funding Information: We thank our patients for their trust. We thank S. Kubo for assistance with hybridoma screenings and preparation of antibodies, and are grateful to H. Kishida, K. Kawano, S. Iwata, and K. Tanaka for their assistance with experiments. We thank Y. Noda, R. Takashima, and the TMIG animal facility staff for their assistance with animal experiments. We thank Editage ( www.editage.com ) for English language editing. This work was supported by the Grant-in-Aid for Scientific Research ( 16K01851 , 19K11660 , 15K01743 , 21200023 , 21591102 , 24390228 , 25670437 , 16H03266 and 19H04064 ), Grant-in-Aid for Early-Career Scientist ( 20K19737 ), AMED Leap ( JP21mg00100007 ), Takeda Science Foundation , and Mitsui Sumitomo Insurance Welfare Foundation . Publisher Copyright: © 2022

PY - 2023/3

Y1 - 2023/3

N2 - Autoantibodies to muscle-specific tyrosine kinase (MuSK) proteins at the neuromuscular junction (NMJ) cause refractory generalized myasthenia gravis (MG) with dyspnea more frequently than other MG subtypes. However, the mechanisms via which MuSK, a membrane protein locally expressed on the NMJ of skeletal muscle, is supplied to the immune system as an autoantigen remains unknown. Here, we identified MuSK in both mouse and human serum, with the amount of MuSK dramatically increasing in mice with motor nerve denervation and in MG model mice. Peptide analysis by liquid chromatography-tandem-mass spectrometry (LC-MS/MS) confirmed the presence of MuSK in both human and mouse serum. Furthermore, some patients with MG have significantly higher amounts of MuSK in serum than healthy controls. Our results indicated that the secretion of MuSK proteins from muscles into the bloodstream was induced by ectodomain shedding triggered by neuromuscular junction failure. The results may explain why MuSK-MG is refractory to treatments and causes rapid muscle atrophy in some patients due to the denervation associated with Ab-induced disruption of neuromuscular transmission at the NMJ. Such discoveries pave the way for new MG treatments, and MuSK may be used as a biomarker for other neuromuscular diseases in preclinical studies, clinical diagnostics, therapeutics, and drug discovery.

AB - Autoantibodies to muscle-specific tyrosine kinase (MuSK) proteins at the neuromuscular junction (NMJ) cause refractory generalized myasthenia gravis (MG) with dyspnea more frequently than other MG subtypes. However, the mechanisms via which MuSK, a membrane protein locally expressed on the NMJ of skeletal muscle, is supplied to the immune system as an autoantigen remains unknown. Here, we identified MuSK in both mouse and human serum, with the amount of MuSK dramatically increasing in mice with motor nerve denervation and in MG model mice. Peptide analysis by liquid chromatography-tandem-mass spectrometry (LC-MS/MS) confirmed the presence of MuSK in both human and mouse serum. Furthermore, some patients with MG have significantly higher amounts of MuSK in serum than healthy controls. Our results indicated that the secretion of MuSK proteins from muscles into the bloodstream was induced by ectodomain shedding triggered by neuromuscular junction failure. The results may explain why MuSK-MG is refractory to treatments and causes rapid muscle atrophy in some patients due to the denervation associated with Ab-induced disruption of neuromuscular transmission at the NMJ. Such discoveries pave the way for new MG treatments, and MuSK may be used as a biomarker for other neuromuscular diseases in preclinical studies, clinical diagnostics, therapeutics, and drug discovery.

KW - Animal model

KW - Biomarker

KW - Denervation

KW - Extracellular domain

KW - Mass spectrometry

KW - Matrix protease

KW - Muscle-specific kinase

KW - Myasthenia gravis

KW - Reinnervation

KW - Shedding

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U2 - 10.1016/j.expneurol.2022.114300

DO - 10.1016/j.expneurol.2022.114300

M3 - Article

C2 - 36525997

AN - SCOPUS:85144773688

SN - 0014-4886

VL - 361

JO - Neurodegeneration

JF - Neurodegeneration

M1 - 114300

ER -

Proteolytic ectodomain shedding of muscle-specific tyrosine kinase in myasthenia gravis

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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