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Visualization and characterization of complement activation in acetylcholine receptor antibody seropositive myasthenia gravis
Uppsala University, Disciplinary Domain of Medicine and Pharmacy, Faculty of Medicine, Department of Medical Sciences, Clinical Neurophysiology.
Linnaeus Univ, Linnaeus Ctr Biomat Chem, Kalmar, Sweden..
Uppsala University, Disciplinary Domain of Medicine and Pharmacy, Faculty of Medicine, Department of Immunology, Genetics and Pathology.ORCID iD: 0009-0006-3983-5891
Uppsala Univ, Dept Immunol Genet & Pathol, Uppsala, Sweden..
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2024 (English)In: Muscle and Nerve, ISSN 0148-639X, E-ISSN 1097-4598, Vol. 70, no 4, p. 851-861Article in journal (Refereed) Published
Abstract [en]

Introduction/Aim

There are no blood biomarkers to monitor treatment effects in myasthenia gravis (MG) or studies visualizing the acetylcholine receptor (AChR) antibody-induced membrane attack complex (MAC) at the human muscle membrane. This study aimed to compare levels of complement activation products and native complement components in MG patients and healthy controls (HCs) and to model the AChR antibody-mediated attacks in human muscle cells.

Methods

We assessed the complement components and activation product levels with enzyme-linked immunosorbent assay and magnetic bead-based sandwich assays in plasma and sera of 23 MG patients and matched HCs. Receiver operator characteristic (ROC) curve analysis evaluated the diagnostic accuracy. Complement levels were correlated with the myasthenia gravis composite (MGC) scores. AChR+ MG modeling in human muscle cells used sera from nine MG patients and three HCs.

Results

MG patients had significantly higher plasma levels of C3a (p < .0001), C5 (p = .0003), and soluble C5b-9 (sC5b-9; p < .0001) than HCs. The ROC curve analysis showed a clear separation between MG patients and HCs for plasma C3a (AUC = 0.9720; p < .0001) and sC5b-9 (AUC = 0.8917, p < .0001). MG patients had higher levels of plasma complement Factor I (FI; p = .0002) and lower properdin levels (p < .0001). The MGC had moderate correlations with plasma Factor B (FB), FI, and Factor H. AChR+ MG patient sera triggered the deposition of MAC and reduced AChRs.

Discussion

We suggest validating plasma C3a and sC5b-9 as blood biomarkers for complement activation in MG. Further, the in vitro study allowed visualization of MAC deposition after applying AChR+ MG sera on human muscle cells.
Place, publisher, year, edition, pages
John Wiley & Sons, 2024. Vol. 70, no 4, p. 851-861
Keywords [en]
biomarker, complement, membrane attack complex, MGC, myasthenia gravis
National Category
Neurology
Identifiers
URN: urn:nbn:se:uu:diva-547735DOI: 10.1002/mus.28227ISI: 001286229200001PubMedID: 39115039OAI: oai:DiVA.org:uu-547735DiVA, id: diva2:1929875
Funder
Swedish Research Council, 2020_02040Familjen Erling-Perssons Stiftelse, 2022_0030Available from: 2025-01-21 Created: 2025-01-21 Last updated: 2026-04-13Bibliographically approved
In thesis
1. Circulating Biomarkers and Complement-Associated Skeletal Muscle Pathology in Myasthenia Gravis
Open this publication in new window or tab >>Circulating Biomarkers and Complement-Associated Skeletal Muscle Pathology in Myasthenia Gravis
2026 (English)Doctoral thesis, comprehensive summary (Other academic)
Abstract [en]

Myasthenia gravis (MG) is an autoimmune neuromuscular disorder characterized by pathogenic autoantibodies targeting components of the neuromuscular junction, most commonly the nicotinic acetylcholine receptor (nAChR). In AChR seropositive (AChR+) MG, autoantibody binding to nAChRs can activate the complement cascade, leading to membrane attack complex (MAC) formation, loss of nAChRs, and impaired neuromuscular transmission. MG is heterogeneous with multiple subgroups, and reliable circulating biomarkers and mechanistic insights into skeletal muscle pathology remain limited. This thesis investigates MG-associated circulating blood biomarkers and complement-associated pathogenic mechanisms using an in vitro human skeletal muscle model.

Papers I-II demonstrated that serum miR-150-5p and miR-30e-5p were elevated in MG, with miR-30e-5p correlating with disease course. Additionally, they exhibited good temporal stability. Paper III identified an altered inflammatory protein profile in AChR+ MG, in which CCL28, FGF-23, FGF-5, TGF-α, TNFSF14, and uPA exhibited the highest differences between MG and HC. Papers IV-V demonstrated complement activation in MG. Increased C1s/C1-INH complexes indicated proximal classical pathway activation, while elevated plasma C3a and soluble C5b-9 reflected downstream and terminal pathway activation. C3a exhibited the highest diagnostic performance. Papers V-VI established a human skeletal muscle model of AChR+ MG, in which pathogenic antibodies bound to nAChRs, causing receptor loss, MAC deposition, and impaired cholinergic calcium signaling. Similar effects induced by AChR α-subunit-specific monoclonal antibodies were restored by C3 inhibition, indicating complement activation as a key driver of antibody-mediated pathogenic effects.

Taken together, these studies identify candidate circulating miRNA, inflammatory, and complement-related biomarkers in MG and demonstrate the pathogenic effects in vitro. These findings provide a broader view of immune and inflammatory activation in MG, as well as mechanistic insights into complement-associated skeletal muscle pathology, including proximal complement C3 inhibition as a promising therapeutic strategy.
Place, publisher, year, edition, pages
Uppsala: Acta Universitatis Upsaliensis, 2026. p. 58
Series
Digital Comprehensive Summaries of Uppsala Dissertations from the Faculty of Medicine, ISSN 1651-6206 ; 2269
Keywords
Myasthenia gravis, nicotinic acetylcholine receptor, biomarker, muscle cell, complement activation, calcium signaling
National Category
Medical and Health Sciences
Research subject
Medical Science
Identifiers
urn:nbn:se:uu:diva-582857 (URN)978-91-513-2835-5 (ISBN)
Public defence
2026-06-05, H:son-Holmdahlsalen, Ingång 100, 2 tr., Akademiska sjukhuset, Uppsala, 09:00 (English)
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Supervisors
Available from: 2026-05-11 Created: 2026-04-13 Last updated: 2026-05-11

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Huang, Yu-FangPersson, BarbroRostedt Punga, Anna

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