Department of Dermatology, Watford General Hospital, Watford, U.K.
Department of Paediatric Dermatology, Great Ormond Street Hospital for Children, London, WC1N 3JH, U.K.
Br J Dermatol. 2018 Mar;178(3):659-662. doi: 10.1111/bjd.16046. Epub 2017 Dec 3.
To assess the efficacy and safety of crisaborole ointment, a phosphodiesterase 4 inhibitor, for the treatment of mild or moderate atopic dermatitis (AD) in two phase III studies (AD-301 and AD-302).
Two identically designed multicentre, double-blind randomized controlled trials were conducted in the U.S.A. Participants were randomized 2 : 1 to receive crisaborole or vehicle treatment. In total 47 and 42 investigational centres were identified for AD-301 and AD-302, respectively.
Inclusion criteria were identified as age ≥ 2 years, clinical diagnosis of AD (as per the Hanifin and Rajka criteria), ≥ 5% body surface area involvement, and baseline Investigator's Static Global Assessment (ISGA) mild or moderate. Exclusion criteria included previous use of biologics or systemic corticosteroids (within the last 28 days) or a topical calcineurin inhibitor/corticosteroid (within the last 14 days), and active skin infection.
Participants were instructed to apply the study drug twice daily to all lesions identified at baseline, and all new lesions identified after day 1 (with weekly review of application instructions). Bland emollients were permitted to be used on skin not treated with the study drug.
The primary outcome was defined as ISGA clear or almost clear at day 29, with a 2-grade or more improvement from baseline.
Secondary outcomes included the proportion of patients with an ISGA score of clear or almost clear at day 29, and time to success in ISGA score. Additional outcomes included pruritus severity and signs of AD (erythema, exudation, excoriation, induration/papulation and lichenification), and were measured on a 4-point scale (none, mild, moderate, severe). Adverse events were also recorded.
More participants in the crisaborole-treated group achieved ISGA scores of clear or almost clear with ≥ 2-grade improvement than in the vehicle-treated group (AD-301, 32·8% vs. 25·4%, P = 0·38; AD-302, 31·4% vs. 18·0%, P < 0·001). Greater percentages of clear and almost clear scores were observed in the treatment groups (51·7% vs. 40·6%, P = 0·005; 48·5% vs. 29·7%; P < 0·001), as well as earlier success in ISGA score and improvement in pruritus (P ≤ 0·001). No serious treatment-related adverse events were identified.
Based on the study results, the authors suggest that crisaborole is a safe treatment that improves disease severity, pruritus and clinical signs associated with AD.
评估磷酸二酯酶 4 抑制剂吡美莫司乳膏治疗轻中度特应性皮炎(AD)的疗效和安全性,两项 III 期研究(AD-301 和 AD-302)对此进行了评估。
这两项在美国开展的多中心、双盲、随机对照试验设计相同。参与者按 2:1 的比例随机接受吡美莫司或赋形剂治疗。AD-301 和 AD-302 分别确定了 47 个和 42 个研究中心。
纳入标准为年龄≥2 岁、临床诊断为 AD(根据 Hanifin 和 Rajka 标准)、≥5%的体表面积受累以及基线时研究者静态总体评估(ISGA)为轻度或中度。排除标准包括在过去 28 天内使用过生物制剂或全身性皮质类固醇、在过去 14 天内使用过局部钙调磷酸酶抑制剂/皮质类固醇以及存在活动性皮肤感染。
参与者被指示每天两次将研究药物涂抹于基线时所有识别出的病变以及第 1 天以后新出现的所有病变(每周审查一次用药说明)。可以使用无刺激性的软膏涂抹未用研究药物治疗的皮肤。
主要结局定义为第 29 天 ISGA 达到清除或几乎清除,与基线相比改善≥2 级。
与赋形剂治疗组相比,更多接受吡美莫司治疗的患者在第 29 天达到 ISGA 评分清除或几乎清除且改善≥2 级(AD-301:32.8% vs. 25.4%,P=0.38;AD-302:31.4% vs. 18.0%,P<0.001)。治疗组中观察到更清除和几乎清除的评分比例更高(51.7% vs. 40.6%,P=0.005;48.5% vs. 29.7%,P<0.001),ISGA 评分的成功更早,瘙痒也得到改善(P≤0.001)。未发现与治疗相关的严重不良事件。
基于研究结果,作者认为吡美莫司是一种安全的治疗方法,可改善 AD 相关疾病严重程度、瘙痒和临床体征。
