Background: The objective of this study was to characterize the clinicopathologic features of sicca syndrome associated with immune checkpoint inhibitor (ICI) therapy.
Subjects, materials, and methods: Consecutive patients with new or worsening xerostomia in the setting of ICI treatment for benign or malignant neoplastic disease were evaluated, including labial salivary gland biopsy (LSGB).
Results: Twenty patients (14 male; median age 57 years) had metastatic melanoma (n = 10), metastatic carcinoma (n = 6), or recurrent respiratory papillomatosis (n = 4) and were being treated with avelumab (n = 8), nivolumab (n = 5), pembrolizumab (n = 4), nivolumab/ipilimumab (n = 2), and M7824, a biologic targeting programmed cell death ligand 1 (PD-L1) and transforming growth factor ß (n = 1). Four had pre-existing autoimmune disease. Nineteen had very low whole unstimulated saliva flow; six had new dry eye symptoms. The median interval between ICI initiation and dry mouth onset was 70 days. Rheumatoid factor and anti-Sjögren's Syndrome-related Antigen A (Anti-SSA) were both positive in two subjects. LSGB showed mild-to-severe sialadenitis with diffuse lymphocytic infiltration and architectural distortion. There were lymphocytic aggregates in eight patients, composed mainly of CD3+ T cells with a slight predominance of CD4+ over CD8+ T cells. ICI targets (e.g., programmed cell death 1 and PD-L1) were variably positive. In direct response to the advent of the sicca immune-related adverse event, the ICI was held in 12 patients and corticosteroids were initiated in 10. Subjective improvement in symptoms was achieved in the majority; however, salivary secretion remained very low.
Conclusion: ICI therapy is associated with an autoimmune-induced sicca syndrome distinct from Sjögren's syndrome, often abrupt in onset, usually developing within the first 3 months of treatment, and associated with sialadenitis and glandular injury. Improvement can be achieved with a graded approach depending on severity, including withholding the ICI and initiating corticosteroids. However, profound salivary flow deficits may be long term.
Implications for practice: Sicca syndrome has been reported as an immune-related adverse event (irAE) of immune checkpoint inhibitor therapy (ICI) for neoplastic diseases. Severe dry mouth (interfering with eating or sleeping) developed abruptly, typically within 90 days, after initiation of ICI therapy. Salivary gland biopsies demonstrated mild-to-severe sialadenitis distinct from Sjögren's syndrome, with diffuse T-cell lymphocytic infiltration and acinar injury. Recognition of the cardinal features of ICI-induced sicca will spur appropriate clinical evaluation and management, including withholding of the ICI and corticosteroid, initiation. This characterization should help oncologists, rheumatologists, and oral medicine specialists better identify patients that develop ICI-induced sicca to initiate appropriate clinical evaluation and therapy to reduce the likelihood of permanent salivary gland dysfunction.
摘要
背景。本研究旨在探讨与免疫检查点抑制剂 (ICI) 治疗相关的干燥综合征的临床病理特点。
受试者、材料和方法。评估采用 ICI 治疗新的或恶化的良性或恶性肿瘤连续发病口腔干燥症患者,包括唇腺病理活检 (LSGB)。
结果。20 例(男性患者 14 例;中位年龄 57 岁)出现转移性黑色素瘤 (n = 10)、转移癌 (n = 6) 或复发性呼吸道乳头瘤样增生 (n = 4),之后接受 Avelumab (n = 8)、纳武单抗 (n = 5)、帕博利珠单抗 (n = 4)、纳武单抗 /易普利姆玛 (n = 2) 或 M7824 生物靶向细胞程序性死亡配体 1 (PD‐L1) 和转化生长因子 ß (n = 1) 治疗。其中 4 例患者既往存在自身免疫性疾病。19 名患者整体非刺激性唾液量非常低,6 名患者出现了新的干眼症状。开始 ICI 治疗至口干舌燥的间隔时间中位数为 70 天。类风湿因子和抗Sjögren综合征相关抗原 A(抗 SSA)在两名受试者中均为阳性。LSGB 结果显示轻‐重度涎腺炎,伴有弥漫性淋巴细胞浸润和结构变形。8 例患者淋巴细胞聚集,以 CD3+ T 细胞为主,CD4+ 略高于 CD8+ T 细胞。ICI 靶细胞(如程序性细胞死亡 1 和 PD‐L1)呈变异阳性。针对干燥免疫相关不良事件的发生,12 例患者暂停接受 ICI 治疗,10 例患者开始使用皮质类固醇。大多数患者的主观症状得到了改善,但唾液分泌量仍然很低。
结论。ICI 治疗会引发一种不同于Sjögren综合征的自身免疫性干燥综合征,通常发病突然,常发病于治疗的前 3 个月内,而且会并发涎腺炎和腺体损伤。可通过根据严重程度进行分级的方法改善症状,包括停用 ICI 和开始服用皮质类固醇。但患者长期时间内都会存在严重的唾液量不足。
实践意义:研究已证实在肿瘤疾病的治疗中,使用免疫检查点抑制剂 (ICI)药物会引发干燥综合征这种免疫相关不良事件 (irAE)。通常在开始 ICI 治疗后 90 天内,会突发严重口干(影响饮食或睡眠)。涎腺病理活检结果表明出现了不同于Sjögren综合征的轻‐重度涎腺炎,伴有弥漫性 T淋巴细胞浸润和腺泡损伤。认识 ICI 引起的干燥综合征的主要特征有助于促进相应的临床评估和管理,包括停用 ICI,开始服用皮质类固醇药物。这一特征有助于肿瘤学家、风湿病学家和口腔医学专家更好地确定因 ICI 引起干燥综合征的患者,从而进行适当的临床评估和治疗,降低永久性唾液腺功能障碍的可能性。
Keywords: Immune checkpoint inhibitor; Immune‐related adverse event; Programmed cell death 1/programmed cell death ligand 1 pathway; Sialadenitis; Sicca syndrome; Sjögren's syndrome; Xerostomia.
Published 2019. This article is a U.S. Government work and is in the public domain in the USA.