Update on targeted treatments for ANCA-associated vasculitis

IF 3.8 3区 医学 Q1 RHEUMATOLOGY Joint Bone Spine Pub Date : 2024-07-30 DOI:10.1016/j.jbspin.2024.105768
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Abstract

Targeted therapy has revolutionized the management of ANCA-associated vasculitis (AAV) over the last fifteen years. Rituximab, an approved induction and maintenance agent for severe AAV, is no less effective than cyclophosphamide as induction therapy and particularly useful in relapsing or refractory disease, or in women. In patients with relapsing AAV, granulomatosis with polyangiitis or PR3-ANCA, it is more effective than cyclophosphamide. Rituximab maintenance is superior to the conventional immunosuppressive drugs that it replaces. Low-dose preemptive rituximab infusions are recommended every 6 months for 18 months, followed by re-evaluation to decide whether 4 additional biannual infusions should be administered, balancing the probability of relapse and the risk of serious infections on rituximab. A growing body of experimental and clinical data shows that C5a pathway inhibition is a promising therapeutic option for AAV, which could reduce glucocorticoids needs. Avacopan is a first approved oral C5A receptor antagonist, used when there is a high risk that glucocorticoids will cause serious adverse events. In eosinophilic granulomatosis with polyangiitis, the importance of IL-5 for eosinophil activation and survival led to evaluation and approval of mepolizumab, a humanized monoclonal antibody directed against IL-5. Mepolizumab showed a steroid-sparing effect. Its effectiveness in active vasculitis remains uncertain and is currently being evaluated. Benralizumab targeting the IL-5 receptor was recently shown to be noninferior to mepolizumab. Rituximab has had disappointing results in non-severe active vasculitis and is being evaluated as maintenance therapy. Plasma exchange is not indicated as first-line treatment but remains recommended when creatinine levels exceed 300 μmol/L.

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ANCA相关性血管炎靶向治疗的最新进展。
在过去的十五年里,靶向治疗彻底改变了ANCA相关性血管炎(AAV)的治疗方法。利妥昔单抗是一种已获批准的重症AAV诱导和维持治疗药物,其诱导治疗效果不亚于环磷酰胺,尤其适用于复发或难治性疾病或女性患者。对于复发性 AAV、肉芽肿伴多血管炎或 PR3-ANCA 患者,它比环磷酰胺更有效。利妥昔单抗的维持治疗效果优于其替代的传统免疫抑制剂。建议每六个月进行一次低剂量的利妥昔单抗抢先输注,持续 18 个月,然后进行重新评估,以决定是否再进行 4 次一年两次的输注,同时平衡利妥昔单抗的复发概率和严重感染风险。越来越多的实验和临床数据表明,C5a通路抑制是一种很有前景的AAV治疗方案,可以减少对糖皮质激素的需求。Avacopan 是首个获批的口服 C5A 受体拮抗剂,用于糖皮质激素极有可能导致严重不良反应的情况。在嗜酸性粒细胞肉芽肿伴多血管炎中,IL-5 对嗜酸性粒细胞的活化和存活非常重要,因此评估并批准了针对 IL-5 的人源化单克隆抗体 mepolizumab。美泊利珠单抗具有节省类固醇的作用。它对活动性血管炎的疗效仍不确定,目前正在评估中。以 IL-5 受体为靶点的 Benralizumab 最近被证明并不比 mepolizumab 差。利妥昔单抗在非严重活动性血管炎中的疗效令人失望,目前正将其作为维持疗法进行评估。血浆置换不作为一线治疗,但在肌酐水平超过 300 µmol/L 时仍被推荐使用。
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来源期刊
Joint Bone Spine
Joint Bone Spine 医学-风湿病学
CiteScore
4.50
自引率
11.90%
发文量
184
审稿时长
25 days
期刊介绍: Bimonthly e-only international journal, Joint Bone Spine publishes in English original research articles and all the latest advances that deal with disorders affecting the joints, bones, and spine and, more generally, the entire field of rheumatology. All submitted manuscripts to the journal are subjected to rigorous peer review by international experts: under no circumstances does the journal guarantee publication before the editorial board makes its final decision. (Surgical techniques and work focusing specifically on orthopedic surgery are not within the scope of the journal.)Joint Bone Spine is indexed in the main international databases and is accessible worldwide through the ScienceDirect and ClinicalKey platforms.
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