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Functional Signature of LRP4 Antibodies in Myasthenia Gravis

Omar Chuquisana, Frauke Stascheit, Christian W. Keller, Maja Pučić‐Baković, Anne‐Marie Patenaude, Gordan Lauc, Socrates J. Tzartos, Heinz Wiendl, Nick Willcox, Andreas Meisel, Jan D. Lünemann

2024Neurology Neuroimmunology & Neuroinflammation20 citationsDOIOpen Access PDF

Abstract

BACKGROUND AND OBJECTIVES: Antibodies (Abs) specific for the low-density lipoprotein receptor-related protein 4 (LRP4) occur in up to 5% of patients with myasthenia gravis (MG). The objective of this study was to profile LRP4-Ab effector actions. METHODS: MG cohort. Levels of circulating activated complement proteins and frequency of Fc glycovariants were quantified and compared with demographically matched 19 healthy controls. RESULTS: Effector actions that required binding of Fc domains to cellular FcRs such as ADCC and ADCP were detectable for both LRP4-specific and AChR-specific Abs. In contrast to AChR-Abs, LRP4-binding Abs showed poor efficacy in inducing complement deposition. Levels of circulating activated complement proteins were not substantially increased in LRP4-Ab-positive MG. Frequency of IgG glycovariants carrying 2 sialic acid residues, indicative for anti-inflammatory IgG activity, was decreased in patients with LRP4-Ab-positive MG. DISCUSSION: LRP4-Abs are more effective in inducing cellular FcR-mediated effector mechanisms than Ab-dependent complement activation. Their functional signature is different from AChR-specific Abs.

Topics & Concepts

Complement systemAntibody-dependent cell-mediated cytotoxicityImmunologyEffectorAntibodyAcetylcholine receptorMyasthenia gravisChemistryBiologyReceptorBiochemistryMonoclonal antibodyMyasthenia Gravis and ThymomaCoagulation, Bradykinin, Polyphosphates, and AngioedemaProtease and Inhibitor Mechanisms
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