N07 JAKne: JAK inhibitor associated acne, a real-life single-center experience

Journal of Crohn's and Colitis Pub Date : 2024-01-01 DOI:10.1093/ecco-jcc/jjad212.1379

E. De Dycker, S. Vermeire, M. Ferrante, T. Lambrechts, A. Paps, P. Geens, E. Loddewijkx, J. Sabino, T. Hillary, B. Verstockt

{"title":"N07 JAKne: JAK inhibitor associated acne, a real-life single-center experience","authors":"E. De Dycker, S. Vermeire, M. Ferrante, T. Lambrechts, A. Paps, P. Geens, E. Loddewijkx, J. Sabino, T. Hillary, B. Verstockt","doi":"10.1093/ecco-jcc/jjad212.1379","DOIUrl":null,"url":null,"abstract":"\n \n \n Three Janus kinase (JAK) inhibitors, tofacitinib (TFC), filgotinib (FIL) and upadacitinib (UPA), have been approved for treatment of Crohn’s disease (CD) and/or ulcerative colitis (UC). During the IBD registrational trials, acne was reported as adverse event (AE) in 5-7% of UPA treated patients, but not in the FIL and TFC programs. Hence, we assessed the prevalence of JAK inhibitor associated acne in a real-life cohort.\n \n \n \n All patients initiating JAK inhibitors for active moderate-to-severe CD or UC at our center were included. Patients were prospectively monitored at prespecified timepoints, and specifically assessed for AEs including acne. Affected patients completed a visual analogue scale (VAS) to assess the impact of acne on their quality of life. All pictures of skin lesions were assessed by a dermatologist specialized in inflammatory skin diseases.\n \n \n \n In total, 46 patients initiated TFC, 40 FIL and 79 UPA. None of the TFC or FIL treated patients reported new onset of acne. Instead, 17 (21.5%) patients (9 CD, 8 UC; median [IQR] age 28.2 [25.2-45.0]; 47.1% female) spontaneously reported acne during UPA therapy. Most (89.5%) reported new onset of acne, while 2 (10.5%) mentioned a deterioration of existing acne during UPA induction. Previous acne during adolescence was reported by 46.2%. Lesions were present in the face (82.3%), back (23.5%), chest (23.5%) and scalp (11.8%). The acne phenotype included inflammatory papules in all patients, but also pustules (66.7%), nodules (33.3%), cysts (11.1%) and comedones (11.1%) were observed. A median VAS score of 5.5 [5.0-7.0] highlighted the impact on the patient’s quality of life, though no patient interrupted UPA due to acne. Six (35.2%) patients were referred to a dermatologist for acne. Most patients (82.4%) received topical skin therapy during UPA induction based on a standard operation procedure approved by the dermatologist and communicated via the IBD nurses. Three patients (17.6%) received antibiotics during UPA induction because of acne. During UPA maintenance, 5 patients (29.4%) reported resolution of skin problems with only 1 requiring continued skin therapy. Ten patients (58.7%) continued topical skin therapy during maintenance, with 4 of them requiring continued antibiotic treatment for at least 3 months. A single patient was deescalated from UPA 30mg to 15mg QD because of severe acne, with little improvement.\n \n \n \n In this real-world experience, JAK inhibitor associated acne was uniquely linked to UPA, occurring in one fifth of patients. This is more prevalent than observed in the registrational trials. Awareness and patient education are therefore important, as well as early referral to the dermatologist for appropriate treatment.\n","PeriodicalId":15453,"journal":{"name":"Journal of Crohn's and Colitis","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2024-01-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Journal of Crohn's and Colitis","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.1093/ecco-jcc/jjad212.1379","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"","JCRName":"","Score":null,"Total":0}

引用次数: 0

Abstract

Three Janus kinase (JAK) inhibitors, tofacitinib (TFC), filgotinib (FIL) and upadacitinib (UPA), have been approved for treatment of Crohn’s disease (CD) and/or ulcerative colitis (UC). During the IBD registrational trials, acne was reported as adverse event (AE) in 5-7% of UPA treated patients, but not in the FIL and TFC programs. Hence, we assessed the prevalence of JAK inhibitor associated acne in a real-life cohort. All patients initiating JAK inhibitors for active moderate-to-severe CD or UC at our center were included. Patients were prospectively monitored at prespecified timepoints, and specifically assessed for AEs including acne. Affected patients completed a visual analogue scale (VAS) to assess the impact of acne on their quality of life. All pictures of skin lesions were assessed by a dermatologist specialized in inflammatory skin diseases. In total, 46 patients initiated TFC, 40 FIL and 79 UPA. None of the TFC or FIL treated patients reported new onset of acne. Instead, 17 (21.5%) patients (9 CD, 8 UC; median [IQR] age 28.2 [25.2-45.0]; 47.1% female) spontaneously reported acne during UPA therapy. Most (89.5%) reported new onset of acne, while 2 (10.5%) mentioned a deterioration of existing acne during UPA induction. Previous acne during adolescence was reported by 46.2%. Lesions were present in the face (82.3%), back (23.5%), chest (23.5%) and scalp (11.8%). The acne phenotype included inflammatory papules in all patients, but also pustules (66.7%), nodules (33.3%), cysts (11.1%) and comedones (11.1%) were observed. A median VAS score of 5.5 [5.0-7.0] highlighted the impact on the patient’s quality of life, though no patient interrupted UPA due to acne. Six (35.2%) patients were referred to a dermatologist for acne. Most patients (82.4%) received topical skin therapy during UPA induction based on a standard operation procedure approved by the dermatologist and communicated via the IBD nurses. Three patients (17.6%) received antibiotics during UPA induction because of acne. During UPA maintenance, 5 patients (29.4%) reported resolution of skin problems with only 1 requiring continued skin therapy. Ten patients (58.7%) continued topical skin therapy during maintenance, with 4 of them requiring continued antibiotic treatment for at least 3 months. A single patient was deescalated from UPA 30mg to 15mg QD because of severe acne, with little improvement. In this real-world experience, JAK inhibitor associated acne was uniquely linked to UPA, occurring in one fifth of patients. This is more prevalent than observed in the registrational trials. Awareness and patient education are therefore important, as well as early referral to the dermatologist for appropriate treatment.

查看原文

微信好友朋友圈 QQ好友复制链接

本刊更多论文

N07 JAKne：与 JAK 抑制剂相关的痤疮，单个中心的真实体验

三种 Janus 激酶 (JAK) 抑制剂托法替尼 (TFC)、非尔戈替尼 (FIL) 和乌达替尼 (UPA) 已被批准用于治疗克罗恩病 (CD) 和/或溃疡性结肠炎 (UC)。在 IBD 注册试验期间，UPA 治疗患者中有 5%-7% 出现了痤疮不良反应（AE），但 FIL 和 TFC 项目中却没有出现痤疮不良反应。因此，我们评估了现实生活中队列中与 JAK 抑制剂相关的痤疮发生率。我们中心纳入了所有因活动性中重度 CD 或 UC 而开始使用 JAK 抑制剂的患者。在预先规定的时间点对患者进行前瞻性监测，并对包括痤疮在内的AEs进行专门评估。受影响的患者填写了视觉模拟量表（VAS），以评估痤疮对其生活质量的影响。所有皮损图片均由皮肤炎症专科医生进行评估。共有 46 名患者接受了 TFC 治疗，40 名患者接受了 FIL 治疗，79 名患者接受了 UPA 治疗。在接受 TFC 或 FIL 治疗的患者中，没有人报告新发痤疮。相反，17 名（21.5%）患者（9 名 CD，8 名 UC；中位数 [IQR] 年龄 28.2 [25.2-45.0]；47.1% 为女性）在 UPA 治疗期间自发报告出现痤疮。大多数人（89.5%）报告了新发痤疮，2 人（10.5%）提到在 UPA 诱导期间原有痤疮恶化。46.2%的患者表示在青春期曾出现过痤疮。皮损分布在面部（82.3%）、背部（23.5%）、胸部（23.5%）和头皮（11.8%）。所有患者的痤疮表型包括炎性丘疹，但也有脓疱（66.7%）、结节（33.3%）、囊肿（11.1%）和粉刺（11.1%）。虽然没有患者因为痤疮而中断 UPA，但 VAS 中位数评分 5.5 [5.0-7.0]凸显了对患者生活质量的影响。六名患者（35.2%）因痤疮转诊至皮肤科医生。大多数患者（82.4%）在 UPA 诱导期间根据皮肤科医生批准的标准操作程序接受了局部皮肤治疗，并通过 IBD 护士进行了沟通。三名患者（17.6%）因痤疮在 UPA 诱导期间接受了抗生素治疗。在 UPA 维护期间，5 名患者（29.4%）报告皮肤问题得到解决，只有 1 名患者需要继续接受皮肤治疗。10 名患者（58.7%）在维持治疗期间继续接受局部皮肤治疗，其中 4 人需要继续接受抗生素治疗至少 3 个月。一名患者因痤疮严重而将 UPA 30 毫克的剂量降至 15 毫克 QD，但改善甚微。在这一实际经验中，JAK 抑制剂相关痤疮与 UPA 有着独特的联系，有五分之一的患者会出现痤疮。这种情况比注册试验中观察到的更为普遍。因此，提高认识和患者教育以及及早转诊至皮肤科医生接受适当治疗非常重要。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

求助全文

约1分钟内获得全文去求助

来源期刊

Journal of Crohn's and Colitis

自引率

0.00%

发文量