Long-term results of therapy with sequential use of rituximab and belimumab in patients with systemic lupus erythematosus

S. K. Solovyev, A. A. Mesnyankina, E. A. Aseeva, N. Yu. Nikishina
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Abstract

Objective: To evaluate the efficacy of combination therapy with rituximab (RTM) and belimumab (BLM) in patients with systemic lupus erythematosus (SLE) during long-term follow-up. Material and methods. Twelve patients with definite high- and moderate activity SLE were included in the study. Nine of them had skin and joint manifestations, and the others had renal, peripheral nervous system involvement, and vasculitis. Patients received RTM at a dose of 500–2000 mg with premedication with 6-methylprednisolone and then BLM according to the standard regimen of 10 mg/kg once a month. Patients were divided into two groups according to the timing of assessment of long-term outcomes. In the 1 st group, data were evaluated after 7–9 years (n = 4), and in the 2 nd group – after 2–4 years (n = 8) after the prescription of biologic disease-modifying antirheumatic drugs (bDMARDs). Efficacy and tolerability of therapy, SLE activity, and dose of oral glucocorticoids (GC) were evaluated. Results and discussion. Against the background of combination therapy, clinical and immunological response was achieved in 11 of 12 patients after one year (median SLEDAI-2K at baseline – 10 [9.5; 14.5] points, 6 and 12 months after administratrion of BLM – 4 [2; 6] points). When bDMARDs were prescribed in the first two years of the disease, patients responded better to therapy and showed more significant positive dynamics in clinical and laboratory parameters. Subsequently, BLM therapy was limited to an average of 2 years, during which a stable remission was achieved. Prescribing bDMARDs allowed GC to be used as initial therapy in an exacerbation of SLE in medium and low doses (subsequently further reduced). Clinical remission was achieved and maintained in 7 patients, exacerbation at different time points after discontinuation of bDMARDs occurred in 3 patients, efficacy waned in one patient, and no result was achieved with combination therapy in another patient. Conclusion. The most pronounced positive result can be expected when a bDMARDs are prescribed as early as possible after diagnosis of SLE (in the first 2 years of the disease). It is advisable to administer BLM infusions as recommended once a month without long breaks between injections for at least 2 years and to continue until a durable effect is achieved. The use of low-dose GC and its discontinuation is an achievable goal, but careful monitoring of patients is needed to detect early symptoms of exacerbation.
连续使用利妥昔单抗和贝利单抗治疗系统性红斑狼疮患者的长期结果
目的:评价利妥昔单抗(RTM)与贝利单抗(BLM)联合治疗系统性红斑狼疮(SLE)患者的长期随访疗效。材料和方法。12例明确的高活动性和中度活动性SLE患者被纳入研究。其中9例有皮肤和关节表现,其余有肾脏、周围神经系统受累和血管炎。患者接受RTM治疗,剂量为500 - 2000mg,前用药为6-甲基强的松龙,然后按标准方案10mg /kg每月1次进行BLM治疗。根据评估长期预后的时间将患者分为两组。第一组在7-9年后(n = 4)评估数据,第二组在2 - 4年后(n = 8)评估处方生物疾病缓解抗风湿药(bDMARDs)后的数据。评估治疗的疗效和耐受性、SLE活动性和口服糖皮质激素(GC)的剂量。结果和讨论。在联合治疗的背景下,12例患者中有11例在一年后达到了临床和免疫应答(基线时SLEDAI-2K中位数为- 10 [9.5;14.5分,给药后6、12个月[2];6分)。当bdmard在疾病的前两年开处方时,患者对治疗的反应更好,在临床和实验室参数上表现出更显著的积极动态。随后,BLM治疗被限制在平均2年,在此期间实现了稳定的缓解。处方bdmard允许GC在SLE恶化时使用中、低剂量(随后进一步减少)作为初始治疗。7例患者达到并维持临床缓解,3例患者停药后不同时间点加重,1例患者疗效减弱,1例患者联合治疗无效。结论。在SLE诊断后(发病的头2年)尽早开bdmard,可预期最明显的阳性结果。建议按建议每月注射一次BLM,两次注射之间不要有长时间的休息,至少持续2年,直到取得持久的效果。低剂量GC的使用和停药是一个可以实现的目标,但需要对患者进行仔细监测,以发现早期恶化症状。
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