P704 Safety of Immunosuppression in A Prospective Cohort of Inflammatory Bowel Disease Patients with a HIstoRy of CancEr: The SAPPHIRE Registry

J. Axelrad, Y. Jiang, J. Colombel, E. Scherl, D. Lukin, S. Chang, L. Chen, S. Katz, J. Kwah, A. Swaminath, K. Sultan, C. Villagra, L. Jandorf, S. Itzkowitz
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Abstract

For patients with inflammatory bowel disease (IBD) and a history of cancer, retrospective studies have failed to find evidence suggesting that exposure to biologic and/or immunomodulator (IMM) agents was associated with new or recurrent cancer. The SAPPHIRE Registry was developed to prospectively examine this issue. Patients with IBD who had a confirmed first (index) cancer 5 years prior to enrollment were recruited from centers affiliated with the New York Crohn’s and Colitis Organization (NYCCO) since 2016. Patients receiving chemotherapy or radiation therapy at enrollment or recurrent cancer within the last five years were excluded. The primary outcome was the development of an incident cancer stratified by IBD therapy exposure and adjusted for index cancer stage, index cancer type, sex, smoking history, and age at index cancer in a Cox proportional hazards model. 302 patients were analyzed. Median age at IBD diagnosis was 31.5. Patients were 47% male, 88% white, and 61% never smokers. Index cancers were solid organ (138; 46%), dermatologic (100; 33%) GI (34; 11%), hematologic (27; 9%), or of other types (3; 1%); most index cancers (excluding non-melanoma skin cancer) were diagnosed as Stage 1. Following the index cancer, 90 (30%) patients were not exposed to any immunosuppression, and the other 212 were exposed to immunosuppressive therapy: 142 biologic monotherapy (anti-TNF, anti-integrin, anti-IL12/23, anti-IL23; 47%), 13 anti-metabolite monotherapy (mercaptopurine, azathioprine, methotrexate; 4%), 41 biologic + anti-metabolite combination therapy (14%), and 16 exposed to small molecules (JAK inhibitors, ozanimod; 5%). During follow-up, 46 (15%) patients developed subsequent cancers (25 new, 21 recurrent): 22 (48%) dermatologic, 15 (33%) solid, 7 (15%) GI, and 2 (4%) hematologic malignancies at a median age of 63.5. Patients not exposed to immunosuppression experienced incident cancer at a rate of 2.58/100 person-years (PY, Table). Those exposed to immunosuppression had a rate of 5.12/100 PY, representing an additional 2.54 cancers/100 PY (95% CI: 0.22, 4.85). In a time-varying Cox proportional hazards model adjusting for clinical and demographic characteristics, the adjusted hazard ratio for incident cancer for patients exposed to immunosuppressive therapy compared to unexposed patients was 1.36 (95% CI: 0.73, 2.52). Excluding non-melanoma skin cancer, the adjusted hazard ratio was 1.38 (95% CI: 0.66, 2.91). In this ongoing prospective study, we have thus far found no association between immunosuppressive IBD therapy and risk of developing new or recurrent cancer. Ongoing enrollment and follow-up, specifically for individual drug classes and cancer types, are required to confirm these findings.
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P704 癌症风险炎症性肠病患者前瞻性队列中免疫抑制的安全性:SAPPHIRE 注册中心
对于有癌症病史的炎症性肠病(IBD)患者,回顾性研究未能发现证据表明接触生物制剂和/或免疫调节剂(IMM)与新发或复发癌症有关。SAPPHIRE 登记处的建立就是为了对这一问题进行前瞻性研究。 自 2016 年起,从纽约克罗恩病和结肠炎组织(NYCCO)下属的中心招募了入组前 5 年已确诊首次(指数)癌症的 IBD 患者。入组时正在接受化疗或放疗的患者或过去五年内癌症复发的患者除外。主要研究结果是根据IBD治疗暴露分层的癌症发病率,并在Cox比例危险模型中根据指数癌症分期、指数癌症类型、性别、吸烟史和指数癌症发生时的年龄进行调整。 共对 302 名患者进行了分析。确诊 IBD 时的中位年龄为 31.5 岁。47%的患者为男性,88%为白人,61%从不吸烟。指数癌症包括实体器官癌(138 例,占 46%)、皮肤癌(100 例,占 33%)、消化道癌症(34 例,占 11%)、血液癌(27 例,占 9%)或其他类型癌症(3 例,占 1%);大多数指数癌症(不包括非黑色素瘤皮肤癌)被诊断为 1 期。罹患指数癌症后,90 名(30%)患者未接受任何免疫抑制治疗,其他 212 名患者接受了免疫抑制治疗:142人接受了生物单药治疗(抗肿瘤坏死因子、抗整合素、抗IL12/23、抗IL23;47%),13人接受了抗代谢单药治疗(巯嘌呤、硫唑嘌呤、甲氨蝶呤;4%),41人接受了生物+抗代谢联合治疗(14%),16人接受了小分子药物治疗(JAK抑制剂、奥扎尼莫德;5%)。在随访期间,46 名患者(15%)继发癌症(25 名新发,21 名复发):22例(48%)为皮肤恶性肿瘤,15例(33%)为实体瘤,7例(15%)为消化道恶性肿瘤,2例(4%)为血液恶性肿瘤,中位年龄为63.5岁。未接受免疫抑制治疗的患者的癌症发病率为 2.58/100人年(PY,表)。暴露于免疫抑制的患者的癌症发病率为 5.12/100人年,即每 100 人年多发 2.54 例癌症(95% CI:0.22, 4.85)。在调整临床和人口统计学特征的时变考克斯比例危险模型中,与未接受免疫抑制治疗的患者相比,接受免疫抑制治疗的患者发生癌症的调整危险比为 1.36(95% CI:0.73, 2.52)。如果不包括非黑色素瘤皮肤癌,调整后的危险比为 1.38(95% CI:0.66, 2.91)。 在这项正在进行的前瞻性研究中,我们迄今尚未发现免疫抑制性 IBD 治疗与罹患新发或复发性癌症的风险之间存在关联。要证实这些发现,还需要持续的注册和随访,特别是针对个别药物类别和癌症类型的注册和随访。
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