FCGR3A-V158F 基因多态性:中国视神经脊髓炎谱系疾病患者利妥昔单抗剂量优化的潜在预测指标。
FCGR3A-V158F gene polymorphism: A potential predictor for rituximab dosing optimization in Chinese patients with neuromyelitis optica spectrum disorder.
机构信息
Department of Neurology, China-Japan Friendship Hospital, Beijing, 100029 China.
Department of Neurology, the First Affiliated Hospital of Tsinghua University, 100016 China.
出版信息
Mult Scler Relat Disord. 2024 Jun;86:105600. doi: 10.1016/j.msard.2024.105600. Epub 2024 Apr 1.
BACKGROUND
Rituximab (RTX), an anti-CD20 monoclonal antibody, has shown promise in managing neuromyelitis optica spectrum disorders (NMOSD) by depleting B cells and reducing relapses. However, there is no consensus on the optimal RTX dosing regimen, and genetic factors, such as FCGR3A-V158F polymorphism, may influence treatment outcomes. This study investigates how FCGR3A-V158F genotypes influence RTX efficacy in Chinese NMOSD patients under varying dosing regimens and aims to optimize treatment protocols.
METHODS
We conducted a retrospective analysis of 25 Chinese NMOSD patients treated with RTX, grouped into standardized and low-dosage regimens. FCGR3A-V158F genotypes were determined, and treatment responses were evaluated, including relapse rates, time to first relapse (TFR), B-cell depletion, dose adjustments, and treatment retention.
RESULTS
Among all patients, 15 received standardized dosages, while 10 received varied induction doses (500 mg to 1200 mg) in low-dose regimens. For FCGR3A-V158F genotypes, 15 had the FF genotype, and 10 were V carriers (3 VV genotype, 7 VF genotype). Regardless of dosing, FF genotype patients had a higher relapse rate post-RTX treatment compared to V carriers (P < 0.05). None of the 3 VV genotype patients in either dose group experienced relapses post-RTX. In both dose groups, FF genotype patients had significantly shorter TFR and required more RTX dose adjustments post-RTX treatment compared to V carriers in the standardized dosage group (P < 0.05). FF genotype patients in the low dosage group were more likely to experience insufficient B-cell depletion, had lower treatment retention rates, and more discontinuations than V carriers in the standardized dosage group (P < 0.05). Insufficient B-cell depletion significantly predicted clinical relapses after RTX treatment (P < 0.05). In survival analysis, FF genotype patients, regardless of dosing, experienced earlier relapses post-RTX treatment (P < 0.05).
CONCLUSIONS
This study highlights the importance of RTX dosage selection in NMOSD treatment, particularly for FCGR3A-FF genotype patients. Standard-dose RTX therapy with vigilant monitoring of peripheral blood B-cell levels is recommended for these individuals to optimize treatment efficacy.
背景
利妥昔单抗(RTX)是一种抗 CD20 单克隆抗体,通过耗尽 B 细胞和减少复发,在管理视神经脊髓炎谱系疾病(NMOSD)方面显示出前景。然而,对于最佳 RTX 剂量方案尚无共识,遗传因素(如 FCGR3A-V158F 多态性)可能会影响治疗结果。本研究调查了在中国 NMOSD 患者中,不同剂量方案下 FCGR3A-V158F 基因型如何影响 RTX 的疗效,并旨在优化治疗方案。
方法
我们对 25 名接受 RTX 治疗的中国 NMOSD 患者进行了回顾性分析,将其分为标准化和低剂量方案组。确定了 FCGR3A-V158F 基因型,并评估了治疗反应,包括复发率、首次复发时间(TFR)、B 细胞耗竭、剂量调整和治疗保留率。
结果
所有患者中,15 例接受标准化剂量,10 例接受低剂量方案中不同诱导剂量(500mg 至 1200mg)。对于 FCGR3A-V158F 基因型,15 例为 FF 基因型,10 例为 V 携带者(3 例 VV 基因型,7 例 VF 基因型)。无论剂量如何,FF 基因型患者在 RTX 治疗后复发率均高于 V 携带者(P < 0.05)。在任何剂量组中,均无 3 例 VV 基因型患者出现复发。在两个剂量组中,与标准化剂量组的 V 携带者相比,FF 基因型患者在 RTX 治疗后 TFR 显著缩短,需要更多的 RTX 剂量调整(P < 0.05)。在低剂量组中,FF 基因型患者 B 细胞耗竭不足的可能性更大,治疗保留率更低,停药率也更高,而标准化剂量组的 V 携带者则更高(P < 0.05)。B 细胞耗竭不足显著预测了 RTX 治疗后的临床复发(P < 0.05)。在生存分析中,无论剂量如何,FF 基因型患者在 RTX 治疗后更早出现复发(P < 0.05)。
结论
本研究强调了 NMOSD 治疗中 RTX 剂量选择的重要性,特别是对于 FCGR3A-FF 基因型患者。建议对这些患者采用标准剂量 RTX 治疗,并密切监测外周血 B 细胞水平,以优化治疗效果。
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