抗程序性死亡-1 抗体引起的风湿免疫相关不良事件及皮质类固醇对肿瘤反应影响的初步分析:病例系列研究。
Rheumatic immune-related adverse events secondary to anti-programmed death-1 antibodies and preliminary analysis on the impact of corticosteroids on anti-tumour response: A case series.
机构信息
Department of Rheumatology, Royal Melbourne Hospital, Australia; Department of Rheumatology, Austin Health, Melbourne, Australia.
Department of Medical Oncology, Peter MacCallum Cancer Centre, Melbourne, Australia.
出版信息
Eur J Cancer. 2018 Dec;105:88-102. doi: 10.1016/j.ejca.2018.09.027. Epub 2018 Nov 13.
IMPORTANCE
Rheumatic immune-related adverse events (irAEs) occur in approximately 10-20% of anti-programmed death 1 (anti-PD1)-treated cancer patients. There are limited data on the natural history, optimal treatment and long-term oncological outcomes of patients with rheumatic irAEs.
OBJECTIVE
The objective of the study was to describe the spectrum and natural history of rheumatic irAEs and the potential impact of rheumatic irAEs and immunomodulators on anti-PD1 tumour efficacy.
METHODS
Cancer patients with pre-existing rheumatic disease before anti-PD1 therapy or de novo rheumatic irAEs on anti-PD1 therapy were retrospectively reviewed across three sites. Patient demographics, treatment history, anti-PD1 irAEs, and anti-PD1 responses were evaluated. Relationships between the development or pre-existence of rheumatic irAE, use of immunomodulatory agents and outcomes were evaluated.
RESULTS
This multicenter case series describes 36 cancer patients who had rheumatic disease before anti-PD1 therapy (n = 12) or developed de novo rheumatic irAEs (n = 24). Thirty-four of the 36 patients sustained rheumatic irAEs (median time to rheumatic irAE: 14.5 weeks), including 24 de novo (18 inflammatory arthritis, three myositis, two polymyalgia rheumatica, one fasciitis) and 10 flares in 12 patients with pre-existing rheumatic disease. Corticosteroids were used in 30 of 36 patients (median duration: 10 months), and disease-modifying antirheumatic drugs were used in 14 of 36 patients (median duration: 5.5 months). The objective response rate to anti-PD1 therapy was 69% (n = 25/36) overall and 81% (n = 21/26) in the melanoma subgroup.
CONCLUSIONS
Rheumatic irAEs are often chronic and require prolonged immunomodulatory therapy. Prospective studies are required to define optimal management of rheumatic irAEs that maintain long-term anticancer outcomes.
重要性
风湿免疫相关不良事件(irAEs)在约 10-20%接受抗程序性死亡 1(anti-PD1)治疗的癌症患者中发生。关于风湿 irAEs 的自然病史、最佳治疗方法和长期肿瘤学结局的数据有限。
目的
本研究旨在描述风湿 irAEs 的谱和自然病史,以及风湿 irAEs 和免疫调节剂对 anti-PD1 肿瘤疗效的潜在影响。
方法
在三个地点回顾性地检查了在抗 PD1 治疗前患有预先存在的风湿性疾病或在抗 PD1 治疗期间出现新的风湿性 irAEs 的癌症患者。评估了患者的人口统计学、治疗史、anti-PD1 irAEs 和 anti-PD1 反应。评估了风湿 irAE 的发生或预先存在、免疫调节剂的使用与结局之间的关系。
结果
该多中心病例系列描述了 36 名在抗 PD1 治疗前患有风湿性疾病(n=12)或出现新的风湿性 irAEs(n=24)的癌症患者。36 名患者中有 34 名(风湿 irAE 的中位时间:14.5 周)患有风湿 irAEs,包括 24 名新出现的(18 名炎症性关节炎、3 名肌炎、2 名巨细胞动脉炎、1 名筋膜炎)和 12 名患有预先存在的风湿性疾病的患者中 10 名的疾病复发。36 名患者中有 30 名(中位持续时间:10 个月)使用了皮质类固醇,36 名患者中有 14 名(中位持续时间:5.5 个月)使用了疾病修饰抗风湿药物。anti-PD1 治疗的客观缓解率总体为 69%(n=25/36),黑色素瘤亚组为 81%(n=21/26)。
结论
风湿 irAEs 通常是慢性的,需要长期的免疫调节治疗。需要前瞻性研究来确定维持长期抗癌结局的风湿 irAEs 的最佳治疗方法。
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