Tarasco Maria Cristina, Rinaldi Elena, Frangiamore Rita, Vanoli Fiammetta, Berni Alessia, Iacomino Nicola, Canciello Amalia, Andreetta Francesca, Ciusani Emilio, Bonanno Silvia, Maggi Lorenzo, Baggi Fulvio, Mantegazza Renato, Antozzi Carlo, Cavalcante Paola
Neurology 4-Neuroimmunology and Neuromuscular Diseases, Fondazione IRCCS Istituto Neurologico Carlo Besta, Milan, Italy.
Ph.D. Program in Neuroscience, University of Milano-Bicocca, Monza, Italy.
Neurol Neuroimmunol Neuroinflamm. 2025 Sep;12(5):e200455. doi: 10.1212/NXI.0000000000200455. Epub 2025 Jul 31.
Efgartigimod (EFG), a biological drug targeting the IgG recycling neonatal Fc receptor (FcRn), leads to clinical improvements in patients affected by myasthenia gravis (MG), a prototypic autoantibody (Ab)-mediated autoimmune disease affecting neuromuscular junction. Because FcRn is a multifunctional protein expressed in different immune system cells, including B cells, we investigated whether FcRn blockade by EFG may have further immunologic effects, other than IgG reduction, in patients with MG.
Anti-acetylcholine receptor Ab-positive (AChR-MG) patients were treated with EFG according to the GENERATIVE protocol. Clinical evaluation, IgG and autoAb quantification, and circulating T-cell and B-cell subpopulation analyses by flow cytometry were performed at different time points. The expression of regulatory plasma cell-related candidate genes (CD38, lymphocyte-activation gene 3 [LAG3], IL-12a, Ebi3) was assessed by real-time PCR in peripheral blood mononuclear cells (PBMCs) from patients on treatment and in PBMCs either untreated or in vitro treated with an EFG-mimicking anti-FcRn monoclonal Ab (mAb) or with EFG (Vyvgart).
A significantly increased percentage of CD19+/CD27+ memory B cells and CD27+/CD138+ plasma cells was observed at the end of EFG treatment cycle 1 and cycle 2 in patients with AChR-MG. Plasma cell increase, maintained up to cycle 3, significantly correlated with Quantitative Myasthenia Gravis score improvement. Moreover, PBMCs from EFG-treated patients showed overexpression of CD38, LAG3, and IL-12a genes, suggesting EFG's ability to induce non-pathogenic regulatory plasma cells. This ability was confirmed in vitro, because anti-FcRn mAb-treated and EFG-treated PBMCs displayed an up-regulation of CD38 and LAG3 compared with untreated cells.
Our findings indicate an unknown immunoregulatory action of EFG in patients with AChR-MG, by unraveling a drug effect on B-cell differentiation, and suggest the induction of regulatory plasma cells as a further mechanism, beyond IgG reduction, associated with clinical improvement. A deep understanding of the immunologic effects of EFG can help to optimize its usage over time in individual patients and disclose biomarkers suitable for monitoring the long-term patient-specific response.
艾加莫德(EFG)是一种靶向IgG再循环新生儿Fc受体(FcRn)的生物药物,可使重症肌无力(MG)患者的临床症状得到改善。MG是一种典型的自身抗体(Ab)介导的自身免疫性疾病,会影响神经肌肉接头。由于FcRn是一种在包括B细胞在内的不同免疫系统细胞中表达的多功能蛋白,我们研究了EFG阻断FcRn是否可能在MG患者中产生除降低IgG之外的其他免疫效应。
抗乙酰胆碱受体抗体阳性(AChR-MG)患者按照GENERATIVE方案接受EFG治疗。在不同时间点进行临床评估、IgG和自身抗体定量分析,以及通过流式细胞术分析循环T细胞和B细胞亚群。通过实时PCR评估治疗患者外周血单个核细胞(PBMC)以及未治疗或体外经模拟EFG的抗FcRn单克隆抗体(mAb)或EFG(Vyvgart)处理的PBMC中调节性浆细胞相关候选基因(CD38、淋巴细胞激活基因3 [LAG3]、IL-12a、Ebi3)的表达。
在AChR-MG患者的EFG治疗第1周期和第2周期结束时,观察到CD19 + / CD27 +记忆B细胞和CD27 + / CD138 +浆细胞的百分比显著增加。浆细胞增加一直持续到第3周期,与重症肌无力定量评分的改善显著相关。此外,EFG治疗患者的PBMC显示CD38、LAG3和IL-12a基因的过表达,表明EFG能够诱导非致病性调节性浆细胞。这种能力在体外得到证实,因为与未处理细胞相比,抗FcRn mAb处理和EFG处理的PBMC显示CD38和LAG3上调。
我们的研究结果揭示了EFG在AChR-MG患者中未知的免疫调节作用,阐明了其对B细胞分化的药物效应,并表明诱导调节性浆细胞是除降低IgG之外与临床改善相关的另一种机制。深入了解EFG的免疫效应有助于随着时间的推移在个体患者中优化其使用,并发现适合监测长期患者特异性反应的生物标志物。
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