Sikorski Patricia M, Kaminski Henry J, Vincent Angela, Bauman Taylor, Jacobson Leslie, Kusner Linda L
Department of Neurology & Rehabilitation Medicine, George Washington University, Washington, DC, United States.
Neurosciences Group, Department of Clinical Neurology, Weatherall Institute of Molecular Medicine, John Radcliffe Hospital, Oxford, United Kingdom.
Front Immunol. 2025 Jun 18;16:1608160. doi: 10.3389/fimmu.2025.1608160. eCollection 2025.
Atypical B cell (atBC) subsets display significant heterogeneity across autoimmune diseases, complicating efforts to define their role and therapeutic potential. We hypothesized that this heterogeneity reflects the responses to specific immunopathology, resulting in disease-specific profiles. The myasthenia gravis (MG) subtypes acetylcholine receptor (AChR)-positive MG and muscle-specific kinase (MuSK)-positive MG provide an ideal model to explore atBCs due to the distinct immune mechanisms driven by IgG1-3 and IgG4 autoantibodies, respectively in the disease.
CD11c and IgDCD27 double-negative (DN) B cells were analyzed by spectral flow cytometry in non-autoimmune controls, AChR-MG, and MuSK-MG. Results were correlated with clinical parameters and antibody levels. In MG subtypes, atBC subsets were further examined for the impact of disease onset and prior rituximab treatment. CD11c B cells were stimulated to assess antibody secreting cell (ASC) differentiation.
CD11c and DN2 B cells were increased in late-onset AChR-MG, while MuSK-MG featured expanded DN3 B cells linked to disease severity. CD20 expression in atBCs was differentially expressed between MG subtypes, with higher levels in late-onset AChR-MG and significantly reduced levels in MuSK-MG. CD11c B cells were reduced after anti-CD20 treatment in MuSK-MG, whereas DN B cells were unaffected. Functionally, CD11c B cells from MuSK-MG exhibited greater ASC differentiation and autoantibody production.
MG subtypes exhibit distinct atBC profiles linked to immunopathology and disease onset. These findings reveal subtype-specific pathways that regulate atBCs and highlight their potential as therapeutic targets in both IgG1-3- and IgG4-mediated autoimmunity.
非典型B细胞(atBC)亚群在自身免疫性疾病中表现出显著的异质性,这使得确定它们的作用和治疗潜力变得复杂。我们假设这种异质性反映了对特定免疫病理学的反应,从而导致疾病特异性特征。重症肌无力(MG)的亚型乙酰胆碱受体(AChR)阳性MG和肌肉特异性激酶(MuSK)阳性MG提供了一个理想的模型来探索atBC,因为在该疾病中分别由IgG1 - 3和IgG4自身抗体驱动着不同的免疫机制。
通过光谱流式细胞术分析非自身免疫对照、AChR - MG和MuSK - MG中的CD11c和IgDCD27双阴性(DN)B细胞。结果与临床参数和抗体水平相关。在MG亚型中,进一步检查atBC亚群受疾病发作和先前利妥昔单抗治疗的影响。刺激CD11c B细胞以评估抗体分泌细胞(ASC)分化。
在晚发型AChR - MG中,CD11c和DN2 B细胞增加,而MuSK - MG的特征是与疾病严重程度相关的DN3 B细胞扩增。atBC中的CD20表达在MG亚型之间存在差异表达,在晚发型AChR - MG中水平较高,而在MuSK - MG中显著降低。在MuSK - MG中,抗CD20治疗后CD11c B细胞减少,而DN B细胞不受影响。在功能上,来自MuSK - MG的CD11c B细胞表现出更大的ASC分化和自身抗体产生。
MG亚型表现出与免疫病理学和疾病发作相关的不同atBC特征。这些发现揭示了调节atBC的亚型特异性途径,并突出了它们作为IgG1 - 3和IgG4介导的自身免疫性疾病治疗靶点的潜力。
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