Styliani Mastraftsi, MD, 5, Ionos Dragoumi str., 16121, Athens, Greece;
Acta Dermatovenerol Croat. 2023 Dec;31(3):162-164.
Data on switching between agents in patients with atopic dermatitis (AD) are scarce (1-3). We report the case of a patient with severe AD and inadequate response to upadacitinib who showed a complete response after switching to abrocitinib. A 23-year-old male patient with severe AD was enrolled in the Measure Up double-blind, placebo-controlled, phase 3 randomized clinical trial. At baseline, the Eczema Area Severity Index (EASI) was 50.6, the Investigator's Global Assessment (IGA) was 4, the affected Body Surface Area (BSA) was 80%, and the Worst Pruritus-Numeric Rating Scale (WP-NRS) was 10/10 (Figure 1). At week 124, the patient discontinued participation in the trial, while EASI was 9.2, IGA 3, BSA 20%, and WP-NRS 5/10 at the time. After one month off treatment, and while expecting unblinding, the patient again presented with exacerbation of AD, since EASI was 45.6, IGA 4, BSA 80%, and WP-NRS 10/10. At that point of time, access to both dupilumab and tralokinumab was not available in Greece, while upadacitinib was avoided due to inadequate patient satisfaction, partly due to recurrent ocular herpes simplex infections during the previous upadacitinib treatment. The patient was prescribed abrocitinib 200 mg daily. One month after initiation of therapy, the patient achieved complete control of the disease (EASI 0.0, IGA 0, BSA 0%, and WP-NRS 0/10) (Figure 2). This has been maintained with no reported adverse events after 12 months of continuous treatment. After unblinding, the patient was confirmed to have received 15 mg of upadacitinib daily during his participation in the clinical trial. When to switch agents in the treatment of patients with severe AD if the response is not adequate, and what agent to switch to, is an issue that is not clearly defined. Data available from the JADE EXTEND study concluded that patients failing to achieve efficacy outcomes with dupilumab can benefit from switching to both doses of abrocitinib (1). However, a number of patients in this study did not achieve efficacy outcomes even after treatment with 200 mg of abrocitinib. Furthermore, sub-population analysis of the JADE EXTEND study, evaluating difficult-to-achieve patient-oriented outcomes such as Patient Oriented Eczema Measure (POEM) ≤2 and Dermatology Life Quality Index (DLQI) ≤1, further emphasized that switching might be beneficial for a significant number of patients, but unmet need was still evident for some of them (4). The literature lacks data on switching between Janus kinase (JAK) inhibitors in AD. Treat-to-target might be different for early control of the disease, as baricitinib and upadacitinib were assessed at 16 weeks, while abrocitinib was assessed at 12 weeks in the pivotal studies. Regarding the present case, the different clinical response obtained cannot be clearly defined since abrocitinib and upadacitinib are both selective JAK1 inhibitors. Consequently, the targeted inflammatory pathways and the expected regulation of immune functionality could be similar. We may assume that the high dose of abrocitinib vs. the low dose of upadacitinib could have accounted for the improved response. However, it is impossible to assess whether clinical outcomes would have been comparable with the administration of the full dose of upadacitinib 30 mg daily or whether usage of a half-dose of abrocitinib 100 mg daily would have also resulted in inadequate response in the same patient. Switching within the same class of treatment agents has also been a heavily-debated issue for psoriasis for many years; however, recent data suggest that switching between interleukin (IL)-17A antagonists may be of benefit to some patients, although the underlying mechanism of action is still under investigation (5,6). Treatment modification in inadequate response could include: up-dosing, adding classical treatments like methotrexate to the JAK inhibitor, switching to monoclonals, or switching to another JAK inhibitor, taking into account published metanalyses of the efficacy of novel agents. Consequently, there is an unmet need to determine an algorithmic step-by-step approach of treat-to-target and switching or adding treatment in the current landscape of AD therapy. Different policies of reimbursement in different countries, along with a lack of comparative studies, may complicate adding such recommendations to existing treatment guidelines.
关于特应性皮炎(AD)患者在不同药物之间转换的数据很少见(1-3)。我们报告了一例对乌帕替尼治疗反应不佳的严重 AD 患者,在转换为阿布昔替尼后完全缓解的病例。
一名 23 岁的男性严重 AD 患者参加了 Measure Up 双盲、安慰剂对照、3 期随机临床试验。基线时,湿疹面积严重指数(EASI)为 50.6,研究者整体评估(IGA)为 4,受累体表面积(BSA)为 80%,最严重瘙痒数字评分量表(WP-NRS)为 10/10(图 1)。第 124 周时,患者停止参与试验,此时 EASI 为 9.2,IGA 为 3,BSA 为 20%,WP-NRS 为 5/10。停药一个月后,在期待揭盲的同时,患者再次出现 AD 加重,此时 EASI 为 45.6,IGA 为 4,BSA 为 80%,WP-NRS 为 10/10。当时,在希腊,无法获得度普利尤单抗和特利鲁单抗,而乌帕替尼由于患者满意度不高而被避免使用,部分原因是在之前的乌帕替尼治疗过程中反复出现单纯疱疹病毒感染。患者开始每日服用阿布昔替尼 200mg。治疗开始一个月后,患者疾病完全得到控制(EASI 0.0,IGA 0,BSA 0%,WP-NRS 0/10)(图 2)。在连续治疗 12 个月后,没有报告不良事件。揭盲后,确认患者在参加临床试验期间每日接受 15mg 乌帕替尼治疗。如果治疗反应不佳,何时转换药物以及转换为哪种药物是一个尚未明确界定的问题。JADE EXTEND 研究的可用数据得出结论,对度普利尤单抗治疗反应不佳的患者,改用阿布昔替尼两种剂量可能会受益(1)。然而,该研究中的许多患者即使接受 200mg 阿布昔替尼治疗也未能达到疗效终点。此外,JADE EXTEND 研究的亚组分析评估了难以达到的患者导向的疗效终点,如患者导向的湿疹量表(POEM)≤2 和皮肤病生活质量指数(DLQI)≤1,进一步强调转换可能对大量患者有益,但对其中一些患者仍存在未满足的需求(4)。文献中缺乏 AD 中 JAK 抑制剂之间转换的数据。针对疾病早期控制的治疗目标可能有所不同,因为巴瑞替尼和乌帕替尼在 16 周时进行评估,而阿布昔替尼在关键研究中在 12 周时进行评估。就目前的情况而言,由于阿布昔替尼和乌帕替尼均为选择性 JAK1 抑制剂,因此获得的不同临床反应尚不清楚。针对疾病早期控制的治疗目标可能有所不同,因为巴瑞替尼和乌帕替尼在 16 周时进行评估,而阿布昔替尼在关键研究中在 12 周时进行评估。就目前的情况而言,由于阿布昔替尼和乌帕替尼均为选择性 JAK1 抑制剂,因此获得的不同临床反应尚不清楚。针对疾病早期控制的治疗目标可能有所不同,因为巴瑞替尼和乌帕替尼在 16 周时进行评估,而阿布昔替尼在关键研究中在 12 周时进行评估。就目前的情况而言,由于阿布昔替尼和乌帕替尼均为选择性 JAK1 抑制剂,因此获得的不同临床反应尚不清楚。我们可以假设阿布昔替尼的高剂量与乌帕替尼的低剂量相比可能会导致反应改善。然而,我们无法评估如果患者使用 30mg 乌帕替尼的全剂量或使用 100mg 阿布昔替尼的半剂量,临床结果是否会具有可比性,因为在相同患者中也可能出现反应不佳。在许多年内,同一类治疗药物之间的转换也是银屑病的一个激烈争论的问题;然而,最近的数据表明,IL-17A 拮抗剂之间的转换可能对一些患者有益,尽管其作用机制仍在研究中(5,6)。对治疗反应不佳的治疗调整可能包括:增加剂量、在 JAK 抑制剂中加入经典治疗方法,如甲氨蝶呤、转换为单克隆抗体或转换为另一种 JAK 抑制剂,同时考虑新型药物疗效的已发表荟萃分析。因此,在 AD 治疗的当前格局下,需要确定一种针对治疗目标和转换或添加治疗的明确分步方法,这一需求尚未得到满足。不同国家的报销政策不同,再加上缺乏比较研究,这可能会使在现有治疗指南中添加此类建议变得复杂。
