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Immune Toxicity with Checkpoint Inhibition for Metastatic Melanoma: Case Series and Clinical Management

机译:转移性黑色素瘤检查点抑制的免疫毒性:病例系列和临床管理

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Immune checkpoint inhibitors (anti-PD-1 and anti-CTLA-4 antibodies) are a standard of care for advanced melanoma. Novel toxicities comprise immune-related adverse events (irAE). With increasing use, irAE require recognition, practical management strategies, and multidisciplinary care. We retrospectively evaluated the incidence, kinetics, and management of irAE in 41 patients receiving anti-PD-1 antibody therapy (pembrolizumab) for advanced melanoma. 63% received prior anti-CTLA-4 antibody therapy (ipilimumab). IrAE occurred in 54%, most commonly dermatological (24%), rheumatological (22%), and thyroid dysfunction (12%). Thyroiditis was characterised by a brief asymptomatic hyperthyroid phase followed by a symptomatic hypothyroid phase requiring thyroxine replacement. Transplant rejection doses of methylprednisolone were necessary to manage refractory hepatotoxicity. A bullous pemphigoid-like skin reaction with refractory pruritus responded to corticosteroids and neuropathic analgesia. Disabling grade 3-4 oligoarthritis required sulfasalazine therapy in combination with steroids. The median interval between the last dose of anti-CTLA-4 antibody and the first dose of anti-PD-1 therapy was 2.0 months (range 0.4 to 22.4). Toxicities may occur late; this requires vigilance and multidisciplinary management which may allow effective anticancer therapy to continue. Management algorithms for thyroiditis, hypophysitis, arthralgia/arthritis, colitis, steroid-refractory hepatitis, and skin toxicity are discussed.
机译:免疫检查点抑制剂(抗PD-1和抗CTLA-4抗体)是晚期黑色素瘤的治疗标准。新的毒性包括免疫相关的不良事件(irAE)。随着使用的增加,irAE需要认可,实用的管理策略和多学科护理。我们回顾性评估了接受抗PD-1抗体疗法(派姆单抗)治疗晚期黑色素瘤的41例患者的irAE的发生率,动力学和治疗。 63%的患者接受过先前的抗CTLA-4抗体治疗(ipilimumab)。 IrAE发生率为54%,最常见的是皮肤病学(24%),风湿病学(22%)和甲状腺功能障碍(12%)。甲状腺炎的特征是短暂的无症状甲状腺功能亢进期,随后是症状性甲状腺功能减退期,需要甲状腺素替代。甲基泼尼松龙的移植排斥剂量对于控制难治性肝毒性是必要的。大疱性类天疱疮样皮肤反应伴难治性瘙痒对皮质类固醇和神经性镇痛有反应。禁用3-4级寡关节炎需要使用柳氮磺吡啶与类固醇合用。最后一剂抗CTLA-4抗体与第一剂抗PD-1治疗之间的中位间隔为2.0个月(范围为0.4至22.4)。毒性可能发生得较晚;这需要保持警惕和多学科管理,这可能会继续有效的抗癌治疗。讨论了甲状腺炎,垂体炎,关节痛/关节炎,结肠炎,类固醇难治性肝炎和皮肤毒性的管理算法。

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