Pembrolizumab在一例转移性肺腺癌患者中诱导的侵蚀性地衣反应:一例报告

F. Venturi, B. Melotti, M. Lambertini, A. Alessandrini, A. Ardizzoni, E. Dika
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引用次数: 0

摘要

免疫检查点抑制剂诱导的免疫相关不良事件非常常见。皮肤类地衣免疫相关的不良事件是最常见的。然而,口腔类地衣不良反应极为罕见。我们在此描述了一名接受pembrolizumab治疗转移性肺癌癌症的患者,该患者在免疫疗法诱导下出现侵蚀性口腔地衣样反应。一名87岁的男性接受pembrolizumab治疗转移性肺腺癌(基于AJCC 2018的IVa期),出现口腔粘膜多灶性侵蚀,主要位于颊粘膜、腭和嘴唇内部,有多个小的、不规则的、角化过度的区域。组织病理学检查显示上皮坏死,真皮上部有一层致密的带状炎症浸润淋巴细胞和组织细胞。IgG和C3的直接免疫荧光均为阴性。建立了免疫疗法诱导的糜烂性口腔粘膜类地衣反应的诊断方法。考虑到病情的严重性,pembrolizumab治疗被暂停,并开始伴随使用局部和全身类固醇。1个月后,药物毒性得到改善,并重新引入免疫疗法。到目前为止,只有一例pembrolizumab诱导的口腔粘膜糜烂性扁平苔藓被描述。先前报道的药物引起的地衣样皮疹主要局限于皮肤。临床上,苔藓样侵蚀性病变的主要鉴别诊断是大疱性免疫相关疾病,应予以排除。在我们的患者中,组织学检查结合直接免疫荧光和酶联免疫吸附试验的阴性结果证实了侵蚀性地衣类药物反应的诊断。临床医生应该意识到口腔粘膜的地衣样病变,因为相关的疼痛和食物摄入困难可能会严重影响治疗依从性。及时治疗口服药物相关反应可以防止免疫治疗中断,提高患者的生活质量。
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Pembrolizumab-induced erosive lichenoid reaction in a patient with metastatic lung adenocarcinoma: A case report
Immune-related adverse events induced by immune checkpoint inhibitors are quite common. Cutaneous lichenoid immune-related adverse events are among the most frequent. However, oral lichenoid adverse reactions are extremely rare. We herein describe a patient who was treated with pembrolizumab for metastatic lung cancer and developed an erosive oral lichenoid reaction induced by immunotherapy. An 87-year-old man treated with pembrolizumab for metastatic lung adenocarcinoma (stage IVa based on AJCC 2018) developed multifocal erosions of the oral mucosa mainly located on the buccal mucosa, palate, and inner portion of the lips with multiple small, irregular, hyperkeratotic areas. Histopathological examination showed epithelial necrosis and a dense band-like layer of an inflammatory infiltrate of lymphocytes and histiocytes within the upper dermis. Direct immunofluorescence was negative for both IgG and C3. A diagnosis of erosive oral lichenoid reaction of the mucosa induced by immunotherapy was established. Given the severity of the condition, pembrolizumab treatment was withheld and concomitant topical and systemic steroids were started. After 1 month, the drug-related toxicity was ameliorated and immunotherapy was re-introduced. Only one other case of pembrolizumab-induced erosive lichen planus of the oral mucosa has been described to date. Previously reported drug-induced lichenoid rashes were mainly localized on the skin. Clinically, the main differential diagnoses of lichenoid erosive lesions are bullous immune-related disorders and should be excluded. In our patient, histological examination combined with negative results of both direct immunofluorescence and enzyme-linked immunosorbent assays confirmed the diagnosis of erosive lichenoid drug reaction. Clinicians should be aware of lichenoid involvement of the oral mucosa because related pain and food intake difficulties may seriously compromise treatment compliance. Prompt treatment of oral drug-related reactions may prevent interruption of immunotherapy and improve patients’ quality of life.
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2950
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