免疫检查点抑制剂对银屑病逆亚型患病率的影响

IF 4.1 Q2 IMMUNOLOGY
Immunotherapy advances Pub Date : 2022-09-23 eCollection Date: 2022-01-01 DOI:10.1093/immadv/ltac016
Abdulhadi Jfri, Bonnie Leung, Jordan T Said, Yevgeniy Semenov, Nicole R LeBoeuf
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引用次数: 3

摘要

背景:皮肤免疫相关不良事件(irAEs)是由免疫检查点抑制剂(ICI)引起的最常见的irAEs。牛皮癣状的爆发,包括新发和爆发。银屑病逆型缺乏相关证据。方法:到2020年2月,在丹娜-法伯癌症研究所/麻省总医院布里格姆进行了一项回顾性研究。包括ici开始前/后确诊的逆型牛皮癣病例,无论是独立的还是与其他牛皮癣亚型一起。排除ici后无耀斑的已知牛皮癣病例。结果:在8683例DFCI ci治疗的患者中,共鉴定出262例(3%)患有ci介导的牛皮癣样皮肤irAE。其中,13例(占银屑病患者的5%)为逆型银屑病(平均年龄68.7岁;7/13男性)。从ICI开始到银屑病逆转发展或发作的中位时间(范围)分别为7(4-12)周和3.5(2-6)周。12/13例(92.30%)出现瘙痒。11例(85%)受累于腹股沟;其他部位包括臀裂(6;46%),乳突(3;23%),肛周(2;15%),腋窝(2;15%),脐部(2;15%),腹下褶皱(1;8%)。大多数(9/13)人涉及不止一个站点。不良事件严重程度的通用术语标准为10人中有1人(76.92%),3人中有2人(15.38%)。6例(46.15%)患者最初接受肿瘤治疗,外用(制霉菌素、康康唑或克霉唑)或全身抗真菌药物(氟康唑)治疗,中位(范围)为3.5(1-7)个月,未见好转。结论:ICI患者可发展为逆型银屑病,最初可能与真菌性三间症混淆。延迟诊断可延长症状,而局部/全身抗真菌药物对疑似念珠菌感染的患者治疗无效。肿瘤学家和皮肤科医生的认识对于提高ici介导的逆型牛皮癣的诊断、治疗和影响患者的生活质量都很重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Prevalence of inverse psoriasis subtype with immune checkpoint inhibitors.

Prevalence of inverse psoriasis subtype with immune checkpoint inhibitors.

Prevalence of inverse psoriasis subtype with immune checkpoint inhibitors.

Prevalence of inverse psoriasis subtype with immune checkpoint inhibitors.

Background: Cutaneous immune-related adverse events (irAEs) are the most common irAEs caused by immune-checkpoint inhibitors (ICI). Psoriasiform eruptions, both de novo and flares, may occur. Evidence is lacking on inverse psoriasis subtype.

Methods: A retrospective study was conducted at Dana-Farber Cancer Institute/Mass General Brigham through February 2020 using databases. Confirmed inverse psoriasis cases pre-/post-ICI initiation either independently or in conjunction with other psoriasis subtypes were included. Known psoriasis cases without flare post-ICI were excluded.

Results: A total of 262 (3%) individuals with any ICI-mediated psoriasiform cutaneous irAE were identified out of the 8683 DFCI ICI-treated patients. Of these, 13 (5% of psoriasis patients) had inverse psoriasis (mean age 68.7 years; 7/13 male sex). Median (range) time from ICI initiation to inverse psoriasis development or flare was 7 (4-12) and 3.5 (2-6) weeks, respectively. Pruritus occurred in 12/13 (92.30%) cases. 11 (85%) had inguinal involvement; other sites included gluteal cleft (6; 46%), inframammary (3; 23%), perianal (2; 15%), axilla (2; 15%), umbilicus (2; 15%), and infra-abdominal folds (1; 8%). Most (9/13) individuals had more than one site involved. The Common Terminology Criteria for Adverse Events severity was 1 in 10 (76.92%) individuals and 2 in 3 (15.38%) individuals. Six (46.15%) patients were treated initially by oncology with topical (nystatin, econazole, or clotrimazole) or systemic antifungals (fluconazole) for median (range) of 3.5 (1-7) months without improvement, for presumed candida intertrigo.

Conclusion: Patients on ICI may develop inverse psoriasis, which may be initially confused for fungal intertrigo. Delayed diagnosis can prolong symptoms, while patients are treated ineffectively with topical/systemic antifungals for presumed candida infection. Oncologist and dermatologist awareness is important to improve diagnosis of ICI-mediated inverse psoriasis, its management and affected patients' quality of life.

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