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首页> 外文期刊>Journal for ImmunoTherapy of Cancer >Conditional immune toxicity rate in patients with metastatic renal and urothelial cancer treated with immune checkpoint inhibitors
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Conditional immune toxicity rate in patients with metastatic renal and urothelial cancer treated with immune checkpoint inhibitors

机译:用免疫检查点抑制剂治疗转移性肾病患者的条件免疫毒性率

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Background Immune checkpoint inhibitors (ICIs) are associated with immune-related adverse events (irAEs). Although the incidence and prevalence of irAEs have been well characterized in the literature, less is known about the cumulative incidence rate of irAEs. We studied the cumulative incidence of irAEs, defined as the probability of irAE occurrence over time and the risk factors for irAE development in metastatic urothelial carcinoma (mUC) and renal cell carcinoma (mRCC) patients treated with ICIs. Methods We identified a cohort of patients who received ICIs for mUC and mRCC. irAEs were classified using Common Terminology Criteria for Adverse Event (CTCAE) V.5.0 guidelines. The monthly incidence of irAEs over time was reported after landmark duration of therapy. Cumulative incidence of irAEs was calculated to evaluate the time to the first occurrence of an irAE accounting for the competing risk of death. Prognostic factors for irAE were assessed using the Fine and Gray method. Results A total of 470 patients were treated with ICIs between July 2013 and October 2018 (mUC: 199 (42.3%); mRCC: 271 (57.7%)). 341 (72.6%) patients received monotherapy, 86 (18.3%) received ICIs in combination with targeted therapies, and 43 (9.2%) received dual ICI therapy. Overall, 186 patients (39.5%) experienced an irAE at any time point. Common irAEs included hypothyroidism (n=42, 22.6%), rush and pruritus (n=36, 19.4%), diarrhea/colitis (n=35, 18.8%), transaminitis (n=32, 17.2%), and pneumonitis (n=14, 7.5%). Monthly incidence rates decreased over time; however, 17 of 109 (15.6%, 95% CI: 9.4% to 23.8%) experienced their first irAE at least 1?year after treatment initiation. No differences in cumulative incidence were observed based on cancer type, agent, or irAE grade. On multivariable analysis, combined ICI therapy with another ICI or with targeted therapy (p0.001), first-line ICI therapy (p=0.011), and PD-1 inhibitor therapy (p=0.007) were all significantly associated with irAE development. Conclusions This study quantitates the incidence of developing irAEs due to ICI conditioned on time elapsed without irAE development. Although the monthly incidence of irAEs decreased over time on therapy, patients can still develop delayed irAEs beyond ICI discontinuation, and thus, continuous vigilant monitoring is warranted.
机译:背景技术免疫检查点抑制剂(ICIS)与免疫相关不良事件(IRAE)有关。虽然伊拉斯的发病率和患病率在文献中具有很好的特征,但较少是令人讨厌的伊拉克累计发病率的认识。我们研究了伊拉克的累积发病率,被定义为IRAE发生的可能性随着时间的推移,转移性尿路上皮癌(MUC)和肾细胞癌(MRCC)患者的IRAE发育的危险因素。方法我们确定了接受ICIS的患者队伍和MRCC。使用普通术语(CTCAE)V.5.0指南的常见术语标准进行分类伊拉斯。在地标持续时间后,伊拉什每月发病率随时间报告。计算额外危害的累积发病率,以评估竞争死亡风险的阿拉利核算的第一次发生的时间。使用细细和灰色法评估iRAE的预后因素。结果2013年7月至2018年7月至10月(MUC:199(42.3%); MRCC:271(57.7%)之间共有470名患者。 341(72.6%)患者接受单药治疗,86名(18.3%)接受icis与靶向疗法组合,43(9.2%)接受双重ICI治疗。总体而言,186名患者(39.5%)在任何时候都经历过iRAE。常见的伊拉斯包括甲状腺功能减退症(n = 42,22.6%),匆忙和瘙痒(n = 36,19.4%),腹泻/结肠炎(n = 35,18.8%),曲敏炎(n = 32,17.2%)和肺炎( n = 14,7.5%)。每月发病率随着时间的推移而减少;然而,109分中的17个(15.6%,95%CI:9.4%至23.8%)在治疗开始后至少1岁,他们的第一个IRAE至少有1?基于癌症类型,药剂或IRAE等级观察累积发病率没有差异。在多变量分析中,用另一种ICI或靶向治疗(P <0.001),一线ICI治疗(P = 0.011)和PD-1抑制剂治疗(P = 0.007)与ICI治疗合并(P <0.001),与IRAE发育显着相关。结论本研究规定了由于ICI调节而在没有IRAE发育的情况下显影伊拉克斯的发病率。虽然伊拉斯的月发病率随着时间的推移而减少,但患者仍然可以延迟ICI停产超越ICI停药,因此承担持续的警惕监测。

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