Rare bullous pemphigoid during PD-1 inhibitor therapy: a case report

2区 医学 Q1 Medicine Advances in Cancer Research Pub Date : 2022-01-01 DOI:10.53388/2022522006
Zuopeng Xiao, Mengjun Nie, X. Zou
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Abstract

1. Abstract Immunotherapy is an important treatment modality in cancer, but it can also cause adverse reactions, with skin toxicity being the most common. The increasing number of immune checkpoint inhibitors being used in the clinic will inevitably cause an increase in the rate of adverse skin reactions that markedly affect the patient’s quality of life. A 58-year-old patient with intrahepatic cholangiocarcinoma developed bullous pemphigoid (BP) nearly a year after using immune checkpoint inhibitors, which is different from what has been reported in the literature within two weeks of treatment. Pathologically, the skin biopsy diagnosis was epidermal hyperplasia and focal sub-epidermal pustule formation, consistent with drug-induced dermatitis. The patient was treated with methylprednisolone, minocycline, colchicine, nicotinamide, triamcinolone, and traditional Chinese medicine decoction. No new blisters developed after 1 week of treatment. The medication was gradually discontinued, and BP did not recur. Clinicians should carefully consider the risk-benefit ratio when using PD-1 inhibitors, particularly with respect to rash severity. Further studies are needed to investigate relationship between adverse skin reactions and drug efficacy. 2. Introduction Immune checkpoint inhibitors, such as anti-programmed cell death 1 (PD-1), can enhance the anti-tumor function of T cells and increase the activity of the immune system. However, normal tissues and organs can be affected by an overactive immune system, causing an immune-related adverse reaction [1,2]. Adverse skin reactions are the most common side effects of immune checkpoint inhibitor treatment. However, adverse skin reactions are completely atypical [3]. We report herein a case of uncommon features of adverse skin from immunotherapy treatment. The case is the first that we have experienced to present such features since using PD-1 inhibitor treatment. 3. Case presentation In May 2017, the patient underwent right hepatectomy + cholecystectomy due to liver lesions found on physical examination. Postoperative pathology revealed intrahepatic cholangiocarcinoma, moderately differentiated tumor measuring 8×5×5 cm, blood vessel invasion, and no obvious nerve invasion. Tegafur (1.5 mg days 1-14) oral chemotherapy was administered for six cycles after surgery. Magnetic resonance imaging (MRI) on September 2019 showed liver lesions, and recurrence was considered. However, the patient was ineligible for surgery; as such, seven cycles of oxaliplatin (150 mg day 1) + gemcitabine (1 g day 1) chemotherapy combined with lenvatinib targeted therapy and with toripalimab (240 mg day 1) immunotherapy was initiated. After tumor
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罕见大疱性类天疱疮在PD-1抑制剂治疗:1例报告
1. 免疫治疗是癌症的一种重要治疗方式,但它也会引起不良反应,以皮肤毒性最为常见。越来越多的免疫检查点抑制剂被用于临床,不可避免地会导致皮肤不良反应的发生率增加,从而显著影响患者的生活质量。一名58岁的肝内胆管癌患者在使用免疫检查点抑制剂近一年后出现大疱性类天疱疮(BP),这与文献报道的在治疗两周内发生的情况不同。病理上,皮肤活检诊断为表皮增生和局灶性表皮下脓疱形成,符合药物性皮炎。给予甲强的松龙、米诺环素、秋水仙碱、烟酰胺、曲安奈德、中药汤剂治疗。治疗1周后未出现新的水疱。逐渐停药,BP未复发。临床医生在使用PD-1抑制剂时应仔细考虑风险-收益比,特别是在皮疹严重程度方面。皮肤不良反应与药物疗效的关系有待进一步研究。2. 免疫检查点抑制剂,如抗程序性细胞死亡1 (anti-programmed cell death 1, PD-1),可以增强T细胞的抗肿瘤功能,提高免疫系统的活性。然而,过度活跃的免疫系统会影响正常的组织和器官,引起免疫相关的不良反应[1,2]。皮肤不良反应是免疫检查点抑制剂治疗最常见的副作用。然而,皮肤不良反应是完全不典型的[3]。我们在此报告一例罕见的特征,不良皮肤从免疫治疗。该病例是我们使用PD-1抑制剂治疗以来第一例出现此类特征的病例。3.2017年5月,患者体检发现肝脏病变,行右肝+胆囊切除术。术后病理示肝内胆管癌,中分化肿瘤,尺寸8×5×5 cm,血管侵犯,未见明显神经侵犯。替加富(1.5 mg,第1-14天)口服化疗,术后6个周期。2019年9月MRI示肝脏病变,考虑复发。然而,患者不符合手术条件;因此,开始了7个周期的奥沙利铂(150 mg第1天)+吉西他滨(1 g第1天)化疗联合lenvatinib靶向治疗和托利莫单抗(240 mg第1天)免疫治疗。后肿瘤
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来源期刊
Advances in Cancer Research
Advances in Cancer Research 医学-肿瘤学
CiteScore
10.00
自引率
0.00%
发文量
52
期刊介绍: Advances in Cancer Research (ACR) has covered a remarkable period of discovery that encompasses the beginning of the revolution in biology. Advances in Cancer Research (ACR) has covered a remarkable period of discovery that encompasses the beginning of the revolution in biology. The first ACR volume came out in the year that Watson and Crick reported on the central dogma of biology, the DNA double helix. In the first 100 volumes are found many contributions by some of those who helped shape the revolution and who made many of the remarkable discoveries in cancer research that have developed from it.
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