Severe exacerbation of facial dermatitis with swelling following introduction of abrocitinib in a patient with atopic dermatitis

Shirui Chen, Chongtu Yang, Yonghong Lu
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Abstract

Abrocitinib, an oral small-molecule Janus kinase 1 (JAK1) inhibitor, has been widely accepted for the treatment of moderate-to-severe atopic dermatitis (AD). Currently there is a paucity of data on the adverse events (AEs) after abrocitinib treatment, especially on rare events such as exacerbation of facial dermatitis, and their causal relationship and subsequent management remains poorly elucidated. A 43-year-old female patient with moderate AD received dupilumab after failure of topical treatments. Facial dermatitis persisted and became refractory after dupilumab treatment, and the patient changed treatment to oral abrocitinib. Fifteen hours after the first dose of abrocitinib, she developed exacerbation of facial dermatitis with swelling. The patient was initially diagnosed as abrocitinib-induced hypersensitivity. However, a score of 3 of the Naranjo adverse drug reaction assessment indicates week correlation between abrocitinib therapy and exacerbation of facial dermatitis, and negative results from subsequent drug provocation test further suggests no causal relationship. The present case report highlights the necessity of careful determination of abrocitinib-induced hypersensitivity, which should not be diagnosed simply based on the time sequence between drug exposure and symptom occurrence. In addition, caution should be exercised for drug withdrawal, especially when confirmative evidence is absent. Drug provocation test can be helpful and effective treatments could be continued unless severe AEs occur.
特应性皮炎患者使用阿罗吉替尼后面部皮炎严重恶化并伴有肿胀
阿罗西替尼是一种口服小分子Janus激酶1(JAK1)抑制剂,已被广泛接受用于治疗中重度特应性皮炎(AD)。目前,有关阿罗西替尼治疗后不良事件(AEs)的数据很少,尤其是面部皮炎加重等罕见事件,其因果关系和后续处理方法也不甚明了。一名 43 岁的中度 AD 女性患者在局部治疗失败后接受了杜匹单抗治疗。面部皮炎持续存在,并在杜比鲁单抗治疗后变得难治,患者改用口服阿罗西替尼治疗。在首次服用阿罗吉替尼15小时后,她的面部皮炎加重并伴有肿胀。患者最初被诊断为阿罗替尼引起的过敏症。然而,纳兰霍药物不良反应评估结果为3分,表明阿罗西替尼治疗与面部皮炎加重之间存在周相关性,而随后的药物激发试验结果为阴性,进一步表明两者之间不存在因果关系。本病例报告强调了仔细判断阿罗西替尼诱导的超敏反应的必要性,不能简单地根据药物暴露和症状发生之间的时间顺序来诊断。此外,应谨慎对待停药,尤其是在缺乏确诊证据的情况下。药物激发试验可能会有所帮助,除非出现严重的AE,否则可以继续进行有效治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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