Risk of severe immune-related adverse events in cancer patients with pre-existing autoimmunity receiving immune checkpoint inhibitor therapy

D. Isaacs, N. Kathuria-Prakash, Robin Hilder, Melissa G. Lechner, Alexandra Drakaki
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Abstract

Introduction: Immune checkpoint inhibitors (ICI) are widely used cancer therapies that harness the immune system to target malignant cells but subsequently can cause serious off-target immune-related Adverse Effects (irAEs). Patients with pre-existing autoimmune disease have historically been excluded from ICI clinical trials due to scientific concerns over increased risk of irAEs and flares of underlying autoimmune disease.Methods: We designed a retrospective, single-center, case-control study at a large, academic medical center to evaluate the incidence and severity of irAEs in patients with pre-existing autoimmunity compared to controls. Controls were matched 2:1 for age, sex, cancer histology, and ICI class. Patients were identified with ICD 9 and 10 codes followed by manual chart extraction. Cases were defined as patients with pre-existing, systemic autoimmunity. The primary outcome was severe irAE (Grade 3 or higher by Common Terminology Criteria for Adverse Events) within 6 months of ICI therapy. Secondary outcomes included response to ICIs, resolution of the irAE, ICI rechallenge success, and survival. Statistical analyses were performed by Chi-square, Fishers exact, Mann-Whitney, and Log-rank tests.Results: Of 3,130 patients treated with ICIs from 2015-2021, 28 cases with pre-existing autoimmune disease were identified and were matched with 56 controls. Pre-existing autoimmune conditions included antiphospholipid syndrome, inflammatory polyarthritis, juvenile rheumatoid arthritis, multiple sclerosis, psoriatic arthritis, rheumatoid arthritis, and type I diabetes. Multiple cancer histologies, including genitourinary, gynecologic, head & neck, hepatobiliary, lung, melanoma, and pancreatic, were represented. Six of 28 cases (21.4%) experienced severe irAEs compared to 9/56 (16.1%) controls; the odds of developing a severe irAE were not significantly different (OR 0.43, 95% CI 0.083-2.33, p = 0.627, ns). Moreover, there were no significant differences in overall survival or tumor response between the two groups. The majority of irAEs resolved without long-term sequelae (66.7% of cases, 55.6% of controls). The majority of patients who were rechallenged with ICIs were successful in continuing therapy (66.7% of cases, 100% of controls).Conclusion: Our study suggests that patients with pre-existing autoimmune disease can be treated with ICI cancer therapies and experience rates of severe irAEs and overall survival that are similar to those of the general population. These data can aid oncologists in discussing risks and benefits of ICIs when treating patients with pre-existing autoimmunity and solid tumors.
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接受免疫检查点抑制剂治疗的已有自身免疫疾病的癌症患者发生严重免疫相关不良事件的风险
导言:免疫检查点抑制剂(ICI)是一种广泛使用的癌症疗法,它利用免疫系统来靶向恶性细胞,但随后可能会引起严重的非靶向免疫相关不良反应(irAEs)。由于科学界担心irAEs风险增加和潜在自身免疫性疾病复发,患有自身免疫性疾病的患者历来被排除在ICI临床试验之外:我们在一家大型学术医疗中心设计了一项回顾性、单中心、病例对照研究,以评估与对照组相比,既往存在自身免疫疾病的患者的 irAEs 发生率和严重程度。对照组的年龄、性别、癌症组织学和 ICI 分级均为 2:1。通过 ICD 9 和 10 编码识别患者,然后手动提取病历。病例定义为已有系统性自身免疫的患者。主要研究结果是接受 ICI 治疗 6 个月内出现的严重 irAE(根据不良事件通用术语标准为 3 级或以上)。次要结果包括对 ICIs 的反应、irAE 的缓解、ICI 再挑战成功率和存活率。统计分析采用Chi-square、Fishers exact、Mann-Whitney和Log-rank检验:在2015-2021年接受ICIs治疗的3130名患者中,发现了28例患有既往自身免疫性疾病的病例,并与56例对照组进行了配对。既往自身免疫性疾病包括抗磷脂综合征、炎性多关节炎、幼年类风湿性关节炎、多发性硬化症、银屑病关节炎、类风湿性关节炎和I型糖尿病。病例中有多种癌症组织类型,包括泌尿生殖系统癌症、妇科癌症、头颈部癌症、肝胆癌、肺癌、黑色素瘤和胰腺癌。28例病例中有6例(21.4%)出现了严重的虹膜AE,而对照组为9/56(16.1%);出现严重虹膜AE的几率没有显著差异(OR 0.43,95% CI 0.083-2.33,p = 0.627,ns)。此外,两组患者的总生存率和肿瘤反应也无明显差异。大多数虹膜急性睫状体功能障碍都得到了缓解,没有留下长期后遗症(66.7%的病例,55.6%的对照组)。大多数重新接受 ICIs 治疗的患者都能成功地继续治疗(66.7% 的病例,100% 的对照组):我们的研究表明,原有自身免疫性疾病的患者可以接受 ICI 癌症治疗,其严重虹膜不良反应发生率和总生存率与普通人群相似。这些数据有助于肿瘤学家在治疗原有自身免疫性疾病和实体瘤患者时讨论 ICIs 的风险和益处。
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