Impact of Oral Abrocitinib Monotherapy on Patient‑Reported Symptoms and Quality of Life in Adolescents and Adults with Moderate‑to‑Severe Atopic Dermatitis: A Pooled Analysis of Patient‑Reported Outcomes
Abstract
Background Atopic dermatitis imparts a substantial patient burden, including itch, sleep disturbance, and decreased health- related quality of life.Objective This analysis evaluated changes in patient-reported outcomes of disease-specific signs/symptoms and health- related quality of life in adult and adolescent patients with moderate-to-severe atopic dermatitis treated with once-daily oral abrocitinib 200-mg or 100-mg monotherapy.Methods Pooled data from one phase IIb (NCT02780167) and two phase III (NCT03349060, JADE MONO-1; NCT03575871, JADE MONO-2) monotherapy trials in adult and adolescent patients with moderate-to-severe atopic der- matitis were analyzed. Patient-reported outcome assessments included: global severity, itch, and multi-item measures that assess other signs and symptoms of atopic dermatitis. Additional patient-reported outcome assessments measured depression, anxiety, fatigue, disease-specific and general health-related quality of life, and work and general productivity among employed patients. Results Overall, 942 patients were included in this analysis. Improvements were observed from the first post-baseline assessment to week 12 across all patient-reported outcomes, including Patient Global Assessment (PtGA) score of 0/1 (35.5%, 19.8%, and 5.9% for 200 mg, 100 mg, and placebo, respectively), ≥ 4-point improvement in Night Time Itch Scale (NTIS; 57.0%, 42.7%, and 12.7%), change from baseline in Patient-Oriented Eczema Measure (POEM) score (− 11.4, − 8.2, and – 3.4), 1-point improvement in Pruritus and Symptoms Assessment for Atopic Dermatitis (PSAAD; 75.2%, 65.1%, and 33.5%), Hospital Anxiety and Depression Scales (HADS) anxiety (− 2.0, − 1.7, and − 1.0) and depression (− 1.7, − 1.3, and − 0.1). Conclusions Abrocitinib monotherapy improved disease-specific signs/symptoms and health-related quality of life across multiple domains as reported by adult and adolescent patients with moderate-to-severe atopic dermatitis, complementing clinician-reported efficacy and safety outcomes.
Clinical Trial Registration NCT02780167 (registered 23 May, 2016), NCT03349060 (registered 21 November, 2017), NCT03575871 (registered 3 July, 2018).
1.Introduction
Atopic dermatitis (AD) is a chronic, relapsing, inflam- matory skin condition with a high disease and comorbid- ity burden that affects up to 20% of children and 5–10% of adults worldwide [1–5]. Moderate-to-severe AD nega- tively affects patient health-related quality of life (HRQoL),impacting patients, their finances, families, and society in general [6–8]. Pruritus is the most common and bothersome symptom of AD [4, 9] and is associated with sleep distur- bance [10], which additionally may lead to psychological comorbidities, including anxiety, depression, and fatigue [11–16]. Atopic dermatitis is also associated with a higher work absentee rate, causing substantial direct and indirect costs [17]abrocitinib modulates the signaling pathways of several key cytokines involved in the pathogenesis of AD and pruritus [18]. Monotherapy with once-daily oral abrocitinib showed significant efficacy in three phase II/III placebo-controlled trials in adolescents and adults with moderate-to-severe AD [19–21]. A phase IIb trial in adults with moderate-to- severe AD showed that abrocitinib was safe and effective in reducing signs and symptoms of AD based on Investigator’s Global Assessment (IGA) response (clear [0] or almost clear[1] with ≥ 2-grade improvement) and change in Eczema Area and Severity Index (EASI) score from baseline [19]. In JADE MONO-1, significantly greater proportions of abroc- itinib-treated (200 mg or 100 mg) patients than placebo- treated patients achieved IGA response (43.8% and 23.7% vs 7.9%; p < 0.0001 and p < 0.005, respectively) and/or ≥ 75% improvement in EASI (EASI-75) response (62.7% and 39.7% vs 11.8%; p < 0.0001 for both) [20]. Likewise, in JADE MONO-2, greater proportions of abrotine-treated (200 mg or 100 mg) than placebo-treated patients achieved IGA response (38.1%, 28.4% vs 9.1%; p < 0.001) and/or EASI-75 response (61.0%, 44.5% vs 10.4%; p < 0.0001)
[21].
Although it is important to establish efficacy and safety for new treatments, clinician-reported outcome assessments do not capture the full extent of treatment benefits experi- enced by patients; therefore, it is important to report the clinically relevant and complementary data captured by patient-reported outcome (PRO) assessments from clinical trials [22, 23]. Hence, to generate a comprehensive assess- ment of the effect of a treatment on AD, the Harmonising Outcome Measures for Eczema and the More Than Skin Deep initiatives have recommended that clinical trials in AD include assessments of patient-reported symptoms, particu- larly Patient-Oriented Eczema Measure (POEM) and Pru- ritus Numerical Rating Scale (Pruritus-NRS)/Peak Pruritus Numerical Rating Scale (PP-NRS), and HRQoL, particularly the Dermatology Life Quality Index (DLQI), alongside cli- nician-evaluated endpoints and long-term disease control, as core outcome measures [24, 25]. Here, we present a pooled analysis from the placebo-controlled phase IIb and III stud- ies of the effect of abrocitinib monotherapy on PRO meas- ures in adolescents and adults with moderate-to-severe AD.
2.Methods
All three studies included in this pooled analysis were simi- larly designed, international, multicenter, randomized, dou- ble-blind, placebo-controlled, parallel-group trials (Table 1 of the Electronic Supplementary Material [ESM]). The phase IIb study (NCT02780167) was conducted between April 2016 and April 2017 in Australia, Canada, Germany, Hun- gary, and the USA [19]. JADE MONO-1 (NCT03349060)
was a phase III trial conducted between December 2017 and March 2019 in Australia, Canada, Europe, and the USA [20]. JADE MONO-2 (NCT03575871) was a phase III trial con- ducted between June 2018 and August 2019 in Australia, Canada, China, Europe, Japan, South Korea, and the USA [21].All studies had similar eligibility criteria (described pre- viously [19–21]). Briefly, eligible patients were either 18–75 years of age (phase IIb) or ≥ 12 years of age (phase III) with moderate-to-severe AD (IGA ≥ 3, EASI [26] score ≥12 [phase IIb] or ≥ 16 [phase III], affected percentage of body surface area ≥ 10, PP-NRS [27] (used with permission of Regeneron Pharmaceuticals, Inc. and Sanofi) score ≥ 4 [PP- NRS4; phase III only], and inadequate response to treatment with topical corticosteroids or topical calcineurin inhibitors given for ≥ 4 weeks, a history of topical AD treatments considered medically inadvisable, or a history of systemic therapies for AD. Exclusion criteria were medical history of conditions associated with thrombocytopenia, coagulopathy, or platelet dysfunction; prior systemic JAK inhibitor use; systemic corticosteroid use within 4 weeks of study initia- tion; and treatment with dupilumab within 6 weeks of study initiation. The phase III studies also excluded patients with suicidal ideation associated with actual intent and method or plan in the past year (Columbia Suicide Severity Rat- ing Scale [C-SSRS] [28] items 4 and 5), history of suicidal behaviors in the past 5 years (any CSSRS suicidal behavior item in the past 5 years), lifetime history of serious or recur- rent suicidal behavior (Suicidal Behaviors Questionnaire- Revised [29] total score ≥ 8), clinically significant depres- sion (Patient Health Questionnaire-8 [30] total score ≥ 15), or any other major psychiatric disorder that might require exclusion in the opinion of the investigator. Use of topical medicated therapies for AD (topical corticosteroids, topical calcineurin inhibitors, tars, antibiotic creams, topical anti- histamines) and rescue medication (e.g., oral corticoster- oids) was not permitted, but patients were allowed to use oral antihistamines and/or topical nonmedicated emollients during the studies.
In the phase IIb study, patients were randomly assigned 1:1:1:1:1 to receive once-daily oral abrocitinib 200 mg, abrocitinib 100 mg, abrocitinib 30 mg, abrocitinib 10 mg, or matching placebo for 12 weeks. In the phase III studies, patients were randomly assigned 2:2:1 (stratified by baseline disease severity [IGA 3 or 4] and age group [12 to < 18 years or ≥ 18 years]) to receive once-daily oral abrocitinib 200 mg, abrocitinib 100 mg, or matching placebo for 12 weeks. This analysis includes patients randomly assigned to receive abrocitinib 200 mg, abrocitinib 100 mg, or placebo.Patient-reported outcome assessments in all three stud- ies included proportions of patients achieving a ≥ 4-point improvement in itch score (PP-NRS and Pruritus-NRS) [27, 31]. Other PRO assessments included in all studies were: Patient Global Assessment (PtGA) [32, 33] clear or almost clear with a ≥ 2-point improvement; Pruritus and Symptoms Assessment for Atopic Dermatitis (PSAAD [33]) total score; change from baseline in POEM [35–37] total score; distributions of patients across DLQI [38] and Children’s Dermatol- ogy Life Quality Index (CDLQI [39]) band descriptors; and change from baseline in Hospital Anxiety and Depression Scale (HADS) [40, 41] depression and/or anxiety subscale scores and, among patients with respective baseline sub- scale scores ≥ 8, proportions of patients achieving subscale scores < 8.
Several additional PRO endpoints were assessed in JADE MONO-1/MONO-2, including change from baseline in the Short Form-36 Health Survey, Version 2, Acute (SF-36v2)[42] mental and physical component summary scores and domain scores (for patients aged ≥ 18 years only), EuroQol 5-Dimension 5-Level Scale (EQ-5D-5L) [43] or EuroQol 5-Dimension Youth Scale (EQ-5D-Y) [44] index score, and Functional Assessment of Chronic Illness Therapy Fatigue Scale (FACIT-F) [45] score or Pediatric FACIT-F (Peds- FACIT-F) [46] score as well as the proportion of patients achieving FACIT-F/Peds-FACIT-F < 30 at week 12 (among patients with FACIT-F/Peds-FACIT-F ≥ 30 at baseline).JADE MONO-2 assessed two additional PRO endpoints: change from baseline in Work Productivity and Activity Impairment Questionnaire–Atopic Dermatitis, Version 2.0 (WPAI-AD) [47] score (for patients aged ≥ 18 years only) and the proportion of patients and time to achieve a ≥ 4-point improvement in Night Time Itch Scale (NTIS) score for severity of worst itching due to AD during the previous night’s sleep. More detailed descriptions of each PRO assessment are summarized in Table 1.Binary endpoints were analyzed using the Cochran–Man- tel–Haenszel test adjusted by randomization strata. Miss- ing responses for patients who permanently discontinued the study were defined as non-responders at all subsequent visits. Continuous endpoints were analyzed based on the observed data using mixed-model repeated measures with fixed factors of treatment, week, treatment-by-week interac- tion, study, baseline disease severity, age category, and base- line value and unstructured covariance matrix or compound symmetry covariance matrix.
3.Results
Overall, 942 patients were included in this pooled analysis. Baseline disease characteristics were similar across treat- ment groups and across three included studies (Table 2 and Supplementary Table 2 of the ESM). The total population reported moderate-to-severe signs and symptoms of AD per mean POEM total score (Table 3). Furthermore, 62.7% of patients had moderate AD and 37.3% had severe AD per IGA; this distribution was 43.7% and 48.7%, respectively, per PtGA (Table 3). Finally, the patients reported considera- ble symptoms of anxiety or depression per HADS subscores and a very large effect of AD on their quality of life (QoL) based on mean DLQI and CDLQI total scores (Table 3).Mean (standard deviation [SD]) Pruritus-NRS (phase IIb)/PP- NRS scores (phase III; 200 mg, 100 mg, and placebo) were 7.0 (1.9), 7.1 (1.9), and 7.0 (1.9) at baseline and 2.9 (2.6), 3.9(2.7), 5.4 (2.6) at week 12, respectively. Pooled proportions of patients achieving a ≥ 4-point improvement in itch severity based on Pruritus-NRS/PP-NRS score were greater starting at the first post-baseline assessment (week 2) for abrocitinib 200AD atopic dermatitis, CDLQI Children’s Dermatology Life Quality Index, DLQI Dermatology Life Quality Index, EQ-5D-5L EuroQol 5-Dimen- sion 5-Level Scale, EQ-5D-Y EuroQol 5-Dimension Youth Scale, FACIT-F Functional Assessment of Chronic Illness Therapy Fatigue Scale, HADS Hospital Anxiety and Depression Scale, NTIS Night Time Itch Scale, Peds-FACIT-F Pediatric Functional Assessment of Chronic Ill- ness Therapy Fatigue Scale, POEM Patient Oriented Eczema Measure, PP-NRS Peak Pruritus Numerical Rating Scale, Pruritus-NRS Pruritus Numerical Rating Scale, PSAAD Pruritus and Symptoms Assessment for Atopic Dermatitis, PtGA Patient Global Assessment, QoL quality of life, SF-36v2 Short Form-36 Health Survey, Version 2, Acute, WPAI-AD Work Productivity and Activity Impairment Questionnaire–Atopic Der- matitis, Version 2.0mg and 100 mg compared with placebo. At week 2, 44.2% (200 mg), 24.9% (100 mg), and 5.8% (placebo) of patients achieved a ≥ 4-point improvement (i.e., response criteria in phase III studies).
Proportions achieving a ≥ 4-point improvement in Pruritus-NRS/PP-NRS at weeks 4, 8, and 12 were, respectively,57.5%, 59.2%, and 57.3% for 200 mg, 35.7%, 39.7%, and 42.9%for 100 mg, and 12.3%, 14.3%, and 16.5% for placebo. Simi- larly, a significant proportion of patients achieved an itch-free or virtually itch-free status (i.e., PP-NRS 0/1) at week 12 with abrocitinib 200 mg or 100 mg (36.6% and 23.4%, respectively) compared with placebo (5.3%). The median (95% confidence interval [CI]) time to achieve a ≥4-point improvement in Pruri- tus-NRS/PP-NRS was significantly shorter for abrocitinib 200 mg (15 days [13–29]) and abrocitinib 100 mg (57 days [30–64]) vs placebo (112 days [92–not estimable]).Mean (SD) NTIS scores (200 mg, 100 mg, and placebo) were 6.8 (1.9), 6.8 (2.0), and 6.2 (2.1) at baseline and 2.2(2.3), 3.2 (2.8), and 4.8 (3.0) at week 12, respectively. A higher proportion of patients receiving abrocitinib (100 or 200 mg) experienced a ≥ 4-point improvement in the sever- ity of night-time itch (Fig. 1a). The differences in the pro- portion of patients who achieved NTIS response at week 12 vs placebo for abrocitinib 200 mg and 100 mg were 44.6% (95% CI 33.0–56.1; p < 0.0001) and 29.8% (95% CI18.3–41.4; p < 0.0001), respectively. The median (95% CI) time to achieve a ≥ 4-point improvement in the NTIS score was significantly shorter for abrocitinib 200 mg (29 days[14–33]) and abrocitinib 100 mg (57 days [30–81]) vs pla- cebo (116 days [89–116]; p < 0.0001 for both). Mean (SD) PSAAD scores (200 mg, 100 mg, and placebo) were 5.3 (2.1), 5.3 (2.2), and 5.3 (2.0) at baseline and 2.0 (2.1), 2.8(2.1), and 4.3 (2.4) at week 12, respectively. Overall, > 50% of patients treated with abrocitinib reported experiencing a clinically important response in pruritus and symptoms as measured by PSAAD (≥ 1-point improvement) starting at week 2 and continuing through week 12; the proportions of responders were greater for both doses of abrocitinib than placebo at all time points (Fig. 1b).
As measured with PtGA, the proportions of patients with moderate AD (200 mg, 100 mg, and placebo) were 46.6%, 38.5%, and 48.1% at base- line and 22.7%, 32.8%, and 31.6% at week 12, respectively. The proportions of patients with severe AD (200 mg, 100 mg, and placebo) were 46.3%, 53.1%, and 45.2% at base- line and 7.1%, 12.4%, and 23.9% at week 12, respectively. In the overall monotherapy pool, both doses of abrocitinib improved overall disease severity as rated by patients (PtGA) starting at the first post-baseline assessment (week 2) and continuing through the end of treatment (Fig. 1c). Mean (SD) POEM scores (200 mg, 100 mg, and placebo) were 19.8 (5.8), 20.2 (6.2), and 19.9 (5.8) at baseline and 8.9(7.5), 12.0 (7.8), and 16.4 (7.1) at week 12, respectively.Compared with placebo-treated patients, abrocitinib-treated patients reported marked reductions in the frequency of symptoms via POEM throughout the study (Fig. 1d).Mean HADS depression subscale scores (200 mg, 100 mg, and placebo) were 4.2 (3.8), 4.3 (4.0), and 4.5 (3.6) at base-line and 2.4 (3.0), 2.7 (3.2), and 4.0 (3.9) at week 12, respec- tively. Mean HADS anxiety subscale scores (200 mg, 100 mg, and placebo) were 5.8 (4.0), 6.0 (4.3), and 6.6 (4.0) atbaseline and 3.8 (3.7), 4.1 (3.7), and 4.9 (4.0) at week 12, respectively.Decreases from baseline in HADS depression and anxiety subscale scores were greater for abrocitinib-treated patients at all time points (Fig. 2). Among adults with baseline HADS depression score ≥ 8, 32 of 53 patients (60.4%), 28of 60 patients (46.7%), and 9 of 33 patients (27.3%) in the 200-mg, 100-mg, and placebo groups, respectively, achieved HADS depression scores < 8 at week 12. Among adults with baseline HADS anxiety scores ≥ 8, 53 of 98 patients (54.1%), 48 of 100 patients (48.0%), and 17 of 67 patients (25.4%) in the 200-mg, 100-mg, and placebo groups, respec- tively, achieved HADS anxiety score < 8 at week 12.clear with a ≥ 2-point improvement, and d a change from baseline in the Patient-Oriented Eczema Measure (POEM) total score. CI confidence interval, LSM least-squares mean. a≥ 1-point improvement is the clinically important response for the PSAAD total scoreMean FACIT-F scores (200 mg, 100 mg, and placebo) were 38.3 (10.6), 37.4 (11.8), and 37.9 (10.2) at baseline and41.9 (8.9), 40.6 (10.4), and 37.4 (12.1) at week 12, respectively. For adult patients, the least-squares mean change (95% CI) from baseline to week 12 in FACIT-F scores was 3.9 (2.9–4.9) in the abrocitinib 200-mg group and 2.9 (1.9–3.9) in the abrocitinib 100-mg group compared with0.6 (–2.2 to 0.9) in the placebo group. In adolescent patients, mean Peds-FACIT-F scores (200 mg, 100 mg, and placebo) were 37.1 (7.7), 36.2 (9.0), and 35.8 (7.8) at baseline and 39.8 (6.4), 37.9 (9.0), and 37.7 (7.9) at week 12. Least- squares mean change (95% CI) from baseline to week 12 in Peds-FACIT-F was 3.0 (1.3–4.7) in the abrocitinib 200-mg group and 1.4 (– 0.3 to 3.1) in the abrocitinib 100-mg group vs 1.5 (– 1.1 to 4.0) in the placebo group. Among patients with FACIT-F/Peds-FACIT-F ≥ 30 at baseline (i.e., severe fatigue; n = 224 for abrocitinib 200 mg, n = 209 for abroci- tinib 100 mg, n = 93 for placebo), 10 (4.5%), 14 (6.7%), and 13 (14.0%), respectively, achieved FACIT-F/Peds-FACIT- F < 30 at week 12.Mean EQ-5D-5L index scores (200 mg, 100 mg, and pla- cebo) were 0.80 (0.14), 0.79 (0.15), and 0.78 (0.15) at base-line and 0.9 (0.1), 0.9 (0.1), and 0.8 (0.2) at week 12, respec- tively. For adult patients, both abrocitinib doses improved EQ-5D-5L index scores compared with placebo (Fig. 3a). Mean EQ-5D-Y index scores (200 mg, 100 mg, and placebo) were 0.65 (0.32), 0.66 (0.36), and 0.63 (0.39) at baseline and0.9 (0.2), 0.8 (0.3), and 0.8 (0.3) at week 12, respectively. For adolescents, abrocitinib 200 mg improved EQ-5D-Y index scores compared with placebo (Fig. 3b).Mean SF-36v2 mental component summary scores (200 mg, 100 mg, and placebo) were 47.9 (10.7), 48.3 (10.8),and 48.6 (9.2) at baseline and 51.5 (9.4), 50.3 (10.3), and48.8 (9.7) at week 12, respectively. Mean SF-36v2 physical component summary scores (200 mg, 100 mg, and placebo) were 46.0 (8.0), 45.2 (9.0), and 46.0 (8.1) at baseline and 51.0 (7.5), 49.6 (7.6), and 46.8 (8.4) at week 12, respectively. Improvements from baseline to week 12 in SF-36v2 mental and physical component summary scores as well as all eight domain scores were greater for abrocitinib 200 mg and 100 mg than for placebo (Fig. 3c). Mean DLQI total scores (200 mg, 100 mg, and placebo) were 14.4 (6.6), 15.1 (7.1), and 14.3 (7.2) at baseline and 4.9 (5.6), 6.9 (6.2), and10.3 (7.9) at week 12, respectively. By week 12, abrocitinib- treated patients reported a greater shift in DLQI/CDLQI band descriptors toward no or a small impact on disease- specific QoL than placebo-treated patients (Fig. 4). Adult patients treated with abrocitinib 200 mg or 100 mg experi- enced improvement in all individual items of DLQI (effect on symptom severity, embarrassment or self-consciousness, daily activities, clothing, social/leisure activities, perfor- mance of sports, prevention of work/study, impairment of work/study, personal relationships, sex life, and burden of treatment) compared with patients treated with placebo fromweeks 2 to 12 (Fig. 1 of the ESM). In adolescent patients, mean CDLQI total scores (200 mg, 100 mg, and placebo) were 13.1 (5.5), 12.4 (6.4), and 12.5 (6.3) at baseline and4.3 (3.8), 6.4 (5.2), and 9.6 (5.2) at week 12, respectively. Adolescent patients treated with abrocitinib 200 mg or 100 mg experienced improvement in the individual items on CDLQI that address effects on symptom severity, embarrass- ment or self-consciousness, sleep, and burden of treatment compared with patients treated with placebo from weeks 2 to 12 (Fig. 2 of the ESM). Mean percentages of activ- ity impairment measured by WPAI-AD (200 mg, 100 mg, and placebo) were 43.0 (25.6), 41.0 (27.5), and 41.9 (27.2)at baseline and 20.5 (25.3), 22.7 (25.2), and 38.0 (28.6) at week 12, respectively. Employed abrocitinib-treated patients reported greater reductions from baseline to week 12 in the percentage of impairment while working and the percentage of overall work impairment compared with placebo-treated patients (Table 4). Likewise, abrocitinib-treated patients reported greater reductions in activity impairment from baseline to week 12 than placebo-treated patients (Table 4). 4.Discussion This pooled analysis from three placebo-controlled stud- ies showed that adults and adolescents with moderate-to- severe AD treated once daily with oral abrocitinib 200 mg or 100 mg monotherapy experienced clinically meaningful improvements in all domains of patient-reported disease- specific symptoms and HRQoL that were observed start- ing at the first post-baseline assessment (week 2) and sus- tained over a period of 12 weeks. These improvements were observed across a global measure (PtGA), single-symptom measures (Pruritus-NRS/PP-NRS, NTIS), and multi-item measures that included assessments of sleep disturbance, itch, skin pain, erythema, and other skin signs of ADVersion 2, Acute (SF-36v2) scores at week 12. CI confidence inter- val, LSM least-squares mean. aFor patients ≥ 18 years of age. bFor patients < 18 years of age(POEM, PSAAD). These improvements are supported by reduced depression, anxiety, and fatigue (HADS, FACIT-F, Peds-FACIT-F) as well as improved disease-specific (DLQI, CDLQI) and general HRQoL (EQ-5D-5L, EQ-5D-Y, SF-36v2) and improved work and general productivity among employed patients (WPAI-AD). The data generally show that abrocitinib treatment resulted in dose-dependent improve- ments, showing that a higher dose of abrocitinib is associated with greater improvements in PROs and HRQoL assess- ments, and greater proportions of patients benefit from the treatment in these outcomes. These results are consistent with previously reported trends in clinical efficacy outcomes in the individual studies included in this analysis and a pooled analysis of abrocitinib monotherapy studies focusing on itch relief [19–21, 48]. Finally, the changes from baseline reported in this study (POEM, EQ-5D-5L, and SF-36v2) were above meaningful changes previously reported in the literature [42, 49, 50].Starting at the first post-baseline assessment (week 2) and increasing to week 12, substantially greater proportions of patients treated with abrocitinib reported clear or almost clear skin via PtGA compared with placebo. Although the baseline disease severity in the total population differed by clinician (IGA) and patient (PtGA) assessment, the trend in improvement in disease severity was consistent with both assessments by week 12. Likewise, substantially greater pro- portions of abrocitinib-treated patients than placebo-treated patients reported “no impact” on QoL (DLQI/CDLQI band descriptors) at weeks 4 and 12, suggesting both abrocitinib doses improved disease-specific QoL compared with pla- cebo. These improvements in having little-to-no disease activity and impact are especially notable given the sever- ity of disease and impairment observed at baseline in this population.A recent systematic review and network meta-anal- ysis (which included only the phase IIb study data for abrocitinib) found that improvements in Pruritus-NRS/ PP-NRS, POEM, and DLQI scores for abrocitinib 200 mg were comparable to those observed for dupilumab [51]. The majority of improvement in itch with abrocitinib (proportion of patients achieving PP-NRS4 and PP-NRS score changes from baseline) was observed within the first 2 weeks of treat- ment [48]. In the context of other systemic treatments with more gradual improvements in itch (i.e., the majority of itch relief with dupilumab is observed over the first 4 weeks of treatment [52]), the short time to maximal itch relief with abrocitinib treatment is particularly beneficial to patients, especially during acute flares. The more rapid onset of itch relief with abrocitinib vs dupilumab has also been confirmed in JADE COMPARE, which compared short-term efficacy and safety data between abrocitinib and dupilumab treat- ments in patients with moderate-to-severe AD [53]. Other JAK inhibitors, such as baricitinib, have also shown a rapid and sustained itch relief [54]; however, because different itch metrics were used, comparing abrocitinib to baricitinib in the onset of itch relief is challenging. Immediate and sustained relief from itch has been identified as the most relevant benefit expected from new treatments based on a survey of individuals with eczema [25]. This rapid onset of itch relief is also reflected in early separation of abrocitinib from placebo in other measures of AD symptoms, psycho- logical burden, and QoL.As with any post hoc analysis, the strength of these resultsmay be limited. It is possible that improvements in itch could have led to improvements in sleep, hence decreasing fatigue and increasing productivity. Future studies will need to address the interdependency of itch and sleep improvement with QoL outcomes. The PRO instruments were adminis- tered at specific time points, influencing the time to detection of an improvement. In addition, differences in PRO instru- ments across studies resulted in smaller data sets for some of the endpoints. The exclusion of patients with suicidal idea- tion/behaviors or other psychiatric disorders from the phase III studies may limit the generalizability of these results to patients with depressive symptoms, which affect up to 20% of patients with AD (compared with ~15% of patients with- out AD) [55]. Last, these studies were relatively short (12 weeks); the long-term efficacy and safety of abrocitinib are being assessed in ongoing trials. 5.Conclusions The results of these analyses suggest that abrotine is effective for adult and adolescents with moderate-to-severe AD [19, 21]. These results of PRO assessments provide important information on the efficacy of abrotine from the patient perspective and complement clinician-reported efficacy and safety PF-04965842 outcomes.