基于利妥昔单抗的两种不同策略对继发于斯约格伦病的低温球蛋白血症性血管炎的影响：一项单中心队列研究。

IF 3.4 4区医学 Q2 RHEUMATOLOGY Clinical and experimental rheumatology Pub Date : 2024-12-01 Epub Date: 2024-09-13 DOI:10.55563/clinexprheumatol/gakvbr

Simone Longhino, Elena Treppo, Valeria Manfrè, Maria De Martino, Maria Teresa Rizzo, Miriam Isola, Salvatore De Vita, Luca Quartuccio

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引用次数: 0

摘要

研究目的比较两种不同的利妥昔单抗（RTX）治疗方法对继发于斯约格伦病的冷球蛋白血症性血管炎（Sjögren-CryoVasc）患者的血管炎和淋巴细胞增生相关疾病活动以及非霍奇金淋巴瘤（NHL）发展的影响：方法：确定了三个Sjögren-CryoVasc治疗组：方法：确定了三种 Sjögren-CryoVasc 治疗组：1）早期 RTX 诱导，随后进行维持治疗；2）晚期 RTX 诱导，可能按需进行再治疗；3）不进行 RTX 治疗。对以下结果进行了评估：a）累积ESSDAI的变化，考虑到血管炎相关领域和淋巴增生相关领域，以及每一个血管炎相关领域和淋巴增生相关领域特有的ESSDAI变化；b）NHL的发展；c）与严重感染相关的持续性低丙种球蛋白血症的发生：结果：共发现13例Sjögren-CryoVasc患者：结果：13 例 Sjögren-CryoVasc 患者中：1）5/13 例早期接受 RTX 治疗，随后维持治疗；2）5/13 例晚期接受 RTX 治疗，可能按需再治疗；3）3/13 例未接受 RTX 治疗。两组 RTX 患者的 ESSDAI 评分均有所下降，其中第 1 组下降幅度最大（p=0.028）。接受RTX治疗的患者在皮肤、PNS和关节血管炎相关的ESSDAI领域均有明显改善（分别为p=0.007；p=0.006；p=0.03）。相比之下，RTX 对淋巴细胞增生相关的 ESSDAI 领域影响不大，即使第 1 组的腺体和结节领域有所改善（p=0.03；p=0.03）。各组之间在NHL发生率或安全问题上未发现差异：RTX是控制Sjögren-CryoVasc疾病活动的一种有效而安全的治疗方法，在早期使用并采用维持治疗方案时效果更好。结论：RTX 是控制 Sjögren-CryoVasc 疾病活动的有效、安全的治疗方法，在较早使用维持治疗方案时效果更佳。

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The impact of two different rituximab-based strategies in cryoglobulinaemic vasculitis secondary to Sjögren's disease: a monocentric cohort study.

Objectives: To compare two different rituximab (RTX)-based therapeutic approaches on vasculitic and lymphoproliferative-related disease activity and on non-Hodgkin lymphoma (NHL) development in a cohort of patients affected by cryoglobulinaemic vasculitis secondary to Sjögren's disease (Sjögren-CryoVasc).

Methods: Three Sjögren-CryoVasc treatment groups were identified: 1) early RTX induction followed by maintenance; 2) late RTX induction with possible on-demand retreatment; 3) no RTX treatment. The following outcomes were evaluated: a) changes in cumulative ESSDAI, considering vasculitic-related and lymphoproliferative-related domains and changes in ESSDAI specific to each single vasculitic-related and lymphoproliferative-related domain; b) development of NHL; c) occurrence of persistent hypogammaglobulinemia associated with serious infections.

Results: 13 Sjögren-CryoVasc patients were identified: 1) 5/13 treated earlier with RTX with subsequent maintenance; 2) 5/13 treated late with RTX with possible on-demand retreatment; 3) 3/13 not treated with RTX. The two RTX groups showed a decrease in the ESSDAI score with group 1 showing the most substantial reduction (p=0.028). Patients receiving RTX exhibited significant improvement in cutaneous, PNS, and articular vasculitic-related ESSDAI domains (p=0.007; p=0.006; p=0.03, respectively). By contrast RTX did not greatly affect the lymphoproliferative-related ESSDAI domains, even if an improvement was noted in the glandular and nodal domains for group 1 (p=0.03; p=0.03, respectively). No differences in NHL occurrence or safety concerns were observed between the groups.

Conclusions: RTX is an effective and safe treatment to control Sjögren-CryoVasc disease activity with a greater impact when administered earlier with a maintenance regimen. RTX alone cannot, however, affect the possible evolution of Sjögren-CryoVasc into an overt NHL.

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来源期刊

Clinical and experimental rheumatology 医学-风湿病学

CiteScore

6.10

自引率

18.90%

发文量

377

审稿时长

3-6 weeks

期刊介绍： Clinical and Experimental Rheumatology is a bi-monthly international peer-reviewed journal which has been covering all clinical, experimental and translational aspects of musculoskeletal, arthritic and connective tissue diseases since 1983.