The 2 main subgroups of autoimmune myasthenia gravis, a neuromuscular junction disorder associated with muscle weakness, are early-and late-onset forms, defined by onset before or after 50 years of age. Both carry acetylcholine-receptor autoantibodies but differ in sex ratios, genetics, and occurrence of disease-specific thymus inflammation. To distinguish the 2 forms by cellular immune phenotyping, we applied multimodal techniques, including deep spectral cytometric phenotyping and single-cell sequencing. Analysis of 2 independent cohorts identified immunological differences driven by 3 main lymphocyte populations. Lower frequencies of mucosa-associated invariant T cells and naive CD8+ T cells were observed in late-onset myasthenia, suggesting enhanced immune senescence. A highly differentiated, canonical NK cell population was reduced in early-onset myasthenia and negatively correlated with the degree of thymic hyperplasia. Using only the frequency of these 3 populations, correct myasthenia subgroup assignment could be predicted with 90% accuracy. These distinct immunocellular endophenotypes for early-and late-onset disease suggest differences in immunopathogenic processes. Along with demographic factors and other disease subgroup-specific features, the frequency of the identified cell subpopulations may improve clinical classification.
Cellular immune endophenotypes separating early and late-onset myasthenia gravis / Theorell, Jakob; Ruffin, Nicolas; Fower, Andrew; Sorini, Chiara; Ambrose, Philip; Damato, Valentina; Handunnetthi, Lahiru; Leite, Isabel; Irani, Sarosh R.; Brauner, Susanna; Handel, Adam E.; Piehl, Fredrik. - In: JCI INSIGHT. - ISSN 2379-3708. - ELETTRONICO. - 11:(2025), pp. 0-0. [10.1172/jci.insight.199679]
Cellular immune endophenotypes separating early and late-onset myasthenia gravis
Damato, ValentinaInvestigation
;
2025
Abstract
The 2 main subgroups of autoimmune myasthenia gravis, a neuromuscular junction disorder associated with muscle weakness, are early-and late-onset forms, defined by onset before or after 50 years of age. Both carry acetylcholine-receptor autoantibodies but differ in sex ratios, genetics, and occurrence of disease-specific thymus inflammation. To distinguish the 2 forms by cellular immune phenotyping, we applied multimodal techniques, including deep spectral cytometric phenotyping and single-cell sequencing. Analysis of 2 independent cohorts identified immunological differences driven by 3 main lymphocyte populations. Lower frequencies of mucosa-associated invariant T cells and naive CD8+ T cells were observed in late-onset myasthenia, suggesting enhanced immune senescence. A highly differentiated, canonical NK cell population was reduced in early-onset myasthenia and negatively correlated with the degree of thymic hyperplasia. Using only the frequency of these 3 populations, correct myasthenia subgroup assignment could be predicted with 90% accuracy. These distinct immunocellular endophenotypes for early-and late-onset disease suggest differences in immunopathogenic processes. Along with demographic factors and other disease subgroup-specific features, the frequency of the identified cell subpopulations may improve clinical classification.
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