Allinovi Marco, Teisseyre Maxime, Accinno Matteo, Finocchi Cecilia, Esnault Vincent L M, Cremoni Marion, Mazzierli Tommaso, Lazzarini Daniela, Casiraghi Micaela Anna, Fernandez Céline, Zorzi Kévin, Brglez Vesna, Cosmi Lorenzo, Matucci Andrea, Caroti Leonardo, Antognoli Giulia, Cirami Calogero Lino, Vultaggio Alessandra, Seitz-Polski Barbara
Nephrology, Dialysis and Transplantation Unit, Careggi University Hospital, Florence, Italy.
French Reference Center for Rare Diseases, Idiopathic Nephrotic Syndrome and Membranous Nephropathy, Nice University Hospital, Université Côte d'Azur, Nice, France.
Kidney Int Rep. 2025 May 6;10(8):2621-2629. doi: 10.1016/j.ekir.2025.04.059. eCollection 2025 Aug.
Rituximab is a first-line treatment for primary membranous nephropathy (pMN), with proven efficacy and safety. The use of monoclonal antibodies such as rituximab can lead to the formation of antidrug antibodies that may interfere with the therapeutic response. In pMN, anti-rituximab antibodies (ARAs) have been shown to neutralize the cytotoxicity of rituximab, thereby increasing the risk of relapse of nephrotic syndrome. However, the kinetics of ARAs over time and the effect of ARA titer on prognosis are unclear.
This retrospective international multicenter study included 74 patients with pMN treated with rituximab. Here we aimed to clarify the correlation between ARAs and clinical outcome, as well as to evaluate the most appropriate timing of ARA detection.
Overall, 35 out of 74 patients (47%) developed ARAs after a median of 9 (interquartile range: 6-12) months following rituximab administration. ARA monitoring at month-9, month-12 and before rituximab readministration identified 88% of patients with ARAs. Clinical remission rate at 6 and 12 months after rituximab administration was significantly lower in patients with ARAs (31% vs. 56%, = 0.03 and 54% vs. 87%, = 0.0017, respectively). ARAs were associated with a significantly higher rate of relapse (63% vs. 29%, = 0.036) and a higher rate of B-cell reconstitution at 6 months (74.2% vs. 50%, = 0.048). Notably, relapse occurred earlier in patients with ARAs (22 months vs. 32 months, = 0.01).
The development of ARAs represents one of the most important prognostic factors in pMN, being significantly associated with a reduced remission rate and a higher relapse rate after rituximab therapy. Alternative therapies with obinutuzumab or ofatumumab should be considered for these patients.
利妥昔单抗是原发性膜性肾病(pMN)的一线治疗药物,已证实其有效性和安全性。使用利妥昔单抗等单克隆抗体会导致抗药抗体的形成,这可能会干扰治疗反应。在pMN中,抗利妥昔单抗抗体(ARA)已被证明可中和利妥昔单抗的细胞毒性,从而增加肾病综合征复发的风险。然而,ARA随时间的动力学变化以及ARA滴度对预后的影响尚不清楚。
这项回顾性国际多中心研究纳入了74例接受利妥昔单抗治疗的pMN患者。我们旨在阐明ARA与临床结局之间的相关性,并评估ARA检测的最合适时机。
总体而言,74例患者中有35例(47%)在利妥昔单抗给药后中位时间为9个月(四分位间距:6 - 12个月)出现ARA。在第9个月、第12个月以及再次给予利妥昔单抗之前进行ARA监测,可识别出88%的ARA患者。出现ARA的患者在利妥昔单抗给药后6个月和12个月时的临床缓解率显著较低(分别为31%对56%,P = 0.03;54%对87%,P = 0.0017)。ARA与显著更高的复发率(63%对29%,P = 0.036)以及6个月时更高的B细胞重建率(74.2%对50%,P = 0.048)相关。值得注意的是,出现ARA的患者复发更早(22个月对32个月,P = 0.01)。
ARA的出现是pMN最重要的预后因素之一,与利妥昔单抗治疗后缓解率降低和复发率升高显著相关。对于这些患者,应考虑使用奥妥珠单抗或奥法木单抗进行替代治疗。
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