Abstract
Introduction
In pivotal phase 3 tralokinumab monotherapy (ECZTRA 1/2) and topical corticosteroid (TCS) combination (ECZTRA 3) trials in adults with moderate-to-severe atopic dermatitis (AD), tralokinumab significantly improved signs and symptoms of AD. Geographic region may impact treatment response due to potential differences in race and ethnicity, and based on findings in other therapy areas. Here, we evaluated the efficacy and safety of tralokinumab in the ECZTRA 1/2/3 North American population at week 16, as well as maintenance of responses over time, and compared these data side-by-side with those of the ECZTRA 1/2/3 non-North American population.
Methods
Primary endpoints were Investigator’s Global Assessment score of 0 or 1 (IGA 0/1; clear or almost clear) or at least 75% improvement in Eczema Area and Severity Index (EASI-75) at week 16. At week 16, tralokinumab-treated IGA 0/1 or EASI-75 responders were re-randomized 2:2:1 to tralokinumab 300 mg q2w, or q4w, or placebo (ECZTRA 1/2) and 1:1 to tralokinumab 300 mg q2w or q4w (ECZTRA 3).
Results
Overall, 559/1596 (35%) and 160/380 (42.1%) patients randomized in ECZTRA 1/2 and ECZTRA 3 were from North America, respectively. At week 16, IGA 0/1 and EASI-75 response rates were greater with tralokinumab versus placebo in ECZTRA 1/2 (IGA 0/1: 25.3% vs 15.1%; 95% confidence interval [CI] 3.0, 17.3; p = 0.012; EASI-75, 40.1% vs 19.4%; 95% CI 12.6, 28.7; p < 0.001) and ECZTRA 3 (IGA 0/1, 40.0% vs 25.9%; 95% CI − 0.5, 28.3; p = 0.074; EASI-75: 58.1% vs 37.0%; 95% CI 4.9, 37.0; p = 0.012) and tralokinumab was well tolerated in the North American population. Patients with IGA 0/1 or EASI-75 response at week 16 demonstrated sustained responses at week 52 and week 32 in ECZTRA 1/2 and ECZTRA 3, respectively. Similar findings were observed in the non-North American trial populations.
Conclusions
Tralokinumab, with or without TCS, displayed similar efficacy and safety in patients with moderate-to-severe AD across the North American population, and was comparable to the non-North American population.
Clinical Trial Registration
NCT03131648 (registered 27-Apr-2017); NCT03160885 (registered 19-May-2017); NCT03363854 (registered 6-Dec-2017).
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Why carry out this study? |
In three pivotal, multinational, phase 3 trials (ECZTRA 1, ECZTRA 2, and ECZTRA 3) in patients with moderate-to-severe atopic dermatitis, tralokinumab, a fully human monoclonal antibody, with or without topical corticosteroids, demonstrated a favorable safety profile and improved signs and symptoms of atopic dermatitis. |
Geographic region may influence treatment response in patients with atopic dermatitis; hence, regional analyses are important to identify whether treatment differences exist in clinical trial subpopulations. |
This post-hoc analysis evaluated the efficacy and safety of tralokinumab, with or without TCS, in the ECZTRA 1/2 and ECZTRA 3 North American population during the initial treatment period and maintenance of responses over time. |
What was learned from the study? |
Tralokinumab displayed similar efficacy and safety across the ECZTRA 1/2 and ECZTRA 3 North American population, comparable to that of the non-North American population (all patients in ECZTRA 1/2 and ECZTRA 3, excluding patients from North America). |
This post-hoc analysis provides important region-specific evidence of the therapeutic efficacy of tralokinumab monotherapy and combination topical corticosteroid therapy, which could strengthen clinical decision-making and benefit patients with moderate-to-severe atopic dermatitis from North America. |
Introduction
Atopic dermatitis is a chronic inflammatory skin disease that displays a high degree of clinical heterogeneity [1, 2]. Generally, studies investigating safety and efficacy of treatments for atopic dermatitis are analyzed at the multinational level [3,4,5]. However, clinical presentations of atopic dermatitis are known to be influenced by multiple factors, including race, ethnicity, and geographic region, all of which may also impact treatment response [6,7,8]. Additionally, regional differences in treatment outcomes have been reported for other conditions, including metabolic and autoimmune diseases, such as type 2 diabetes and multiple sclerosis, respectively [9, 10]. Analysis of efficacy and safety by region is, therefore, necessary to identify whether treatment differences exist in clinical trial subpopulations and for making better informed, region-specific clinical decisions for patients.
Tralokinumab is a first-in-class, fully human immunoglobulin G4 monoclonal antibody that specifically binds with high affinity to interleukin (IL)-13, thus neutralizing it and inhibiting its signaling capabilities [11]. Having recently been approved in the EU, UK, US, and Canada, tralokinumab is a targeted treatment option that can provide long-term efficacy and safety for adults with moderate-to-severe atopic dermatitis [12,13,14,15].
In recent pivotal, multinational, phase 3 tralokinumab monotherapy (ECZTRA 1, NCT03131648; ECZTRA 2, NCT03160885) and topical corticosteroid (TCS) combination therapy (ECZTRA 3, NCT03363854) trials in adult patients with moderate-to-severe atopic dermatitis, significantly more tralokinumab-treated patients achieved the primary endpoints of Investigator’s Global Assessment score of 0 or 1 (IGA 0/1; clear or almost clear) or at least 75% improvement in Eczema Area and Severity Index (EASI-75) at week 16 [16, 17].
The objective of this post-hoc analysis was to evaluate the efficacy and safety of tralokinumab 300 mg every 2 weeks (q2w), with or without TCS, in the ECZTRA 1/2 and ECZTRA 3 North American subpopulations at week 16 and maintenance of response over time. Equivalent data are provided for the ECZTRA 1/2 and ECZTRA 3 non-North American populations in the electronic supplementary material [ESM] to facilitate side-by-side comparisons of outcomes in the North American trial populations with the non-North American trial populations.
Methods
Studies
Three multinational, double-blind, randomized, placebo-controlled, phase 3 trials of tralokinumab, ECZTRA 1, ECZTRA 2, and ECZTRA 3, were included in the subanalysis. Detailed ECZTRA 1/2 and ECZTRA 3 trial designs, endpoints, and results for the primary study populations were reported previously [16, 17]. Briefly, patients were stratified by region and baseline disease severity and randomized 3:1 (ECZTRA 1/2) to receive subcutaneous tralokinumab 300 mg or placebo q2w, and 2:1 (ECZTRA 3) to subcutaneous tralokinumab 300 mg plus TCS as needed or placebo plus TCS as needed q2w for an initial treatment period of 16 weeks. All patients randomized to tralokinumab and placebo received a 600 mg loading dose of tralokinumab or placebo, respectively, on Day 0. After the initial 16-week treatment period, tralokinumab-treated patients who achieved clinical response, defined as an IGA 0/1 or EASI-75 response at Week 16, were re-randomized 2:2:1 to tralokinumab 300 mg q2w or q4w, or placebo (in ECZTRA 1/2) and 1:1 to tralokinumab 300 mg q2w or q4w (in ECZTRA 3) for a maintenance treatment period of 36 weeks in ECZTRA 1/2 or 16 weeks in ECZTRA 3.
In ECZTRA 3, all patients were instructed to apply a thin layer of TCS (mometasone furoate 0.1% cream; Europe Class 3 [potent]; US Class 4 [mid-strength], supplied at each visit in kit sizes 180–200 g q2w) once daily to active lesions, as needed. To measure the amount of TCS used, patients were instructed to return used and unused TCS tubes at each trial visit. To control intolerable atopic dermatitis symptoms, rescue medication use was permitted at the discretion of the investigator from Day 0. In ECZTRA 1/2, TCS, topical calcineurin inhibitors (TCI), and systemic treatments were considered rescue; in ECZTRA 3, higher potency TCS (Europe Class > 3; US Class < 4) and systemic treatment were considered rescue. The ECZTRA 1, 2, and 3 studies were conducted in accordance with the ethical principles derived from international guidelines including the Declaration of Helsinki and Council for International Organizations of Medical Sciences International Ethical Guidelines and in compliance with International Council for Harmonisation guidelines for Good Clinical Practice. The clinical trials were approved by institutional review boards or ethics committees at each study site and followed the Consolidated Standards of Reporting Trials reporting guideline. All participants provided informed consent to participate in the trials.
Study Population
Detailed inclusion and exclusion criteria have been described previously [16, 17]. Patients were ≥ 18 years of age, with diagnosed atopic dermatitis for ≥ 1 year, and an inadequate response to topical medications < 1 year prior to screening. Patients were required to have an IGA score of ≥ 3, EASI ≥ 12 at screening and ≥ 16 at baseline, involvement of ≥ 10% body surface area at screening and baseline, and worst daily pruritus numeric rating scale (NRS) average score of ≥ 4 during the week prior to baseline.
Endpoints and Post-Hoc Analysis
The primary endpoints were IGA score of 0 (clear) or 1 (almost clear) or at least 75% improvement in EASI (EASI-75) at week 16 [16, 17]. Secondary endpoints included: change from baseline to week 16 in SCORing Atopic Dermatitis (SCORAD), Dermatology Life Quality Index (DLQI), and weekly average worst daily pruritus NRS score, as well as proportions of patients achieving ≥ 4-point reduction of weekly average worst daily pruritus NRS and at least 90% improvement in EASI (EASI-90). Maintenance endpoints at week 52 (in ECZTRA 1/2) and week 32 (in ECZTRA 3) were IGA 0/1 in patients with IGA 0/1 at week 16 and EASI-75 in patients with EASI-75 at week 16. These analyses were performed post hoc for the North American trial subpopulations. Equivalent analyses were performed for the non-North American trial populations to facilitate side-by-side comparisons of the North American and non-North American trial populations.
Statistical Analyses
Post-hoc analyses were based on the ECZTRA 1, 2, and 3 North American populations and were considered exploratory; no adjustments for multiplicity testing were made, hence, p-values obtained for these analyses are nominal. ECZTRA 1 and ECZTRA 2 study data were pooled for the North American subanalysis. For binary endpoints, the difference in response rates between treatment groups was analyzed using the Cochran–Mantel–Haenszel test, stratified by baseline IGA and study identification for ECZTRA 1 and ECZTRA 2, and by baseline IGA for ECZTRA 3. Patients receiving rescue medication, including TCS in ECZTRA 1/2, prior to week 16 or with missing data were considered non-responders.
For the pooled ECZTRA 1/2 data and ECZTRA 3 data, continuous endpoints were assessed using a linear mixed model for repeated measures, including baseline IGA and treatment-by-week interaction as factors and interaction between week and baseline value as covariates for ECZTRA 1/2 and ECZTRA 3 as well as interactions between week and study identification for ECZTRA 1/2. An unstructured covariance matrix was used to model within-patient variation. Data collected after permanent discontinuation of investigational medicinal product or after initiation of rescue medication were excluded from the analysis.
Adverse events (AEs) were assessed at baseline and each subsequent visit until completion of the trial. Descriptive statistics were used to present baseline demographics, baseline disease characteristics, and safety assessments.
Side-by-side comparison was used to compare the efficacy and safety of tralokinumab in the ECZTRA 1/2 and ECZTRA 3 North American populations with that in the non-North American populations.
Results
Patients
Overall, 1596 and 380 patients were randomized in ECZTRA 1/2 and ECZTRA 3, respectively, of whom 559 (35%) and 160 (42.1%) patients were from North America, respectively. The North American population in ECZTRA 1/2 and ECZTRA 3 had similar baseline disease characteristics and demographics, although there were some variations compared with the non-North American population (Table 1 and Table S1, see ESM). Across treatment groups, the median baseline body surface area involvement and proportion of patients with severe atopic dermatitis (IGA 4) were lower in the North American population (ECZTRA 1/2: 38–39% and 40.7–40.8%; ECZTRA 3: 33–36% and 37.7–38.9%) compared with the non-North American population (ECZTRA 1/2: 57–60% and 54.1–56.2%; ECZTRA 3, 50–51% and 51.7–53.4%). In the ECZTRA 1/2 and ECZTRA 3 North American population, median duration of atopic dermatitis was 25–26 years and 24–25 years and median EASI was 24.2–24.9 and 21.6–24.9, respectively, across treatment groups. The ECZTRA 1/2 and ECZTRA 3 North American population was more racially diverse than the non-North American population, with ~ 30–52% of patients from ethnic minority groups across treatment groups (ECZTRA 1/2: ~ 19–24% black/African American, ~ 21% Asian; ECZTRA 3: ~ 18% black/African American, ~ 12–33% Asian).
Primary Outcomes of the ECZTRA 1/2 and ECZTRA 3 North American Population
At week 16, a greater proportion of tralokinumab-treated patients in ECZTRA 1/2 (25.3% vs 15.1%; difference 10.2%; 95% confidence interval [CI] 3.0, 17.3; p = 0.012), and numerically greater proportion of patients in ECZTRA 3 (40.0% vs 25.9%; difference 13.9%; 95% CI − 0.5, 28.3; p = 0.074) achieved IGA 0/1 compared with those who received placebo (Fig. 1a). Similarly, a higher proportion of tralokinumab-treated patients achieved EASI-75 compared with placebo in ECZTRA 1/2 (40.1% vs 19.4%; difference 20.6%; 95% CI 12.6, 28.7; p < 0.001) and ECZTRA 3 (58.1% vs 37.0%; difference 21.0%; 95% CI 4.9, 37.0; p = 0.012) (Fig. 1b).
In the ECZTRA 3 North American population, cumulative TCS use was approximately 50% lower at weeks 15–16 in patients receiving tralokinumab compared with placebo (geometric mean 60.7 g vs 118.5 g; p = 0.012) (Fig. 2), which could account for the high placebo response at week 16 in ECZTRA 3; this needs to be considered when comparing other week 16 endpoints in this trial.
A summary of tralokinumab efficacy in the ECZTRA 1/2 and ECZTRA 3 non-North American population at week 16 can be found in Table S2 (see ESM).
Secondary Outcomes of the ECZTRA 1/2 and ECZTRA 3 North American Population
EASI-90 was achieved by a greater proportion of tralokinumab-treated patients in ECZTRA 1/2 (23.6% vs 7.9%; difference 15.6%; 95% CI 9.6, 21.6; p < 0.001) and numerically greater proportion of tralokinumab-treated patients in ECZTRA 3 (32.4% vs 22.2%; difference 10.1%; 95% CI − 4.3, 24.5; p = 0.18) versus those who received placebo at week 16 (Fig. 3). The adjusted mean change from baseline to Week 16 in SCORAD (standard error [SE]) was greater with tralokinumab versus placebo in ECZTRA 1/2 (− 29.0 [1.08] vs − 18.1 [2.03]; difference –10.9; 95% CI − 15.4, − 6.4; p < 0.001) and ECZTRA 3 (–38.6 [1.98] vs − 23.0 [2.77]; difference − 15.6; 95% CI − 22.4, − 8.9; p < 0.001) (Fig. 4a). Similarly, adjusted mean change from baseline to week 16 in DLQI (SE) was greater with tralokinumab versus placebo in ECZTRA 1/2 (− 9.0 [0.35] vs − 5.9 [0.66]; difference − 3.1; 95% CI − 4.6, − 1.7; p < 0.001) and ECZTRA 3 (− 11.5 [0.61] vs − 7.6 [0.86]; difference − 3.9; 95% CI − 6.0, − 1.9; p < 0.001) (Fig. 4b).
In the initial 16-week treatment period, tralokinumab-treated patients achieved a greater adjusted mean percentage change from baseline in weekly average worst daily pruritus NRS (SE) versus those who received placebo in ECZTRA 1/2 (− 38.7 [1.82] vs − 24.5 [3.41]; difference − 14.1; 95% CI − 21.7, − 6.5; p < 0.001) and ECZTRA 3 (− 55.0 [3.36] vs − 32.4 [4.70]; difference − 22.6; 95% CI − 34.1, − 11.2; p < 0.001) (Fig. 4c). Additionally, a greater proportion of patients in the tralokinumab group in ECZTRA 1/2 (28.0% vs 16.3%; difference 11.8%; 95% CI 4.3, 19.4; p = 0.006) and numerically greater proportion of patients in ECZTRA 3 (42.3% vs 31.5%; difference 10.8%; 95% CI − 4.9, − 26.6; p = 0.19) achieved a ≥ 4-point reduction in weekly average worst daily pruritus NRS versus those in the placebo group (Fig. 5). Notably, the placebo group in ECZTRA 3 used twice as much of the supplied TCS at weeks 15–16 compared with the tralokinumab group (Fig. 2).
Rescue Medication Use in the ECZTRA 1/2 and ECZTRA 3 North American Population
During the initial 16-week treatment period, tralokinumab-treated patients used less rescue medication compared with those who received placebo in ECZTRA 1/2 (17.7% vs 32.9%). TCS was the most commonly used rescue medication in ECZTRA 1/2. In ECZTRA 3, where an increase in TCS potency or systemic therapy were considered rescue, tralokinumab-treated patients used less rescue medication compared with placebo (4.7% vs 9.3%) during the initial treatment period (Table 2). Higher potency TCS was the most commonly used rescue medication in ECZTRA 3. A smaller proportion of patients in the tralokinumab group used immunosuppressants as rescue medication compared with those in the placebo group in ECZTRA 1/2 (0.7% vs 4.3%) and ECZTRA 3 (0% vs 3.7%) (Table 2).
Rescue medication use in the ECZTRA 1/2 and ECZTRA 3 non-North American population was comparable to the ECZTRA 1/2 and ECZTRA 3 North American population, with lower rescue medication use in the tralokinumab arm compared with the placebo arm (Table S3, see ESM).
Maintenance Outcomes in the ECZTRA 1/2 and ECZTRA 3 North American Population
In tralokinumab-treated patients with IGA 0/1 at week 16 in the ECZTRA 1/2 North American population, IGA 0/1 was maintained at week 52 by 58.1% of patients with continued tralokinumab q2w and 40.5% of patients re-randomized to tralokinumab q4w versus 38.1% of patients re-randomized to placebo (Fig. 6a). Similarly, in tralokinumab-treated patients with EASI-75 at week 16, EASI-75 was maintained at week 52 by 59.7% with continued tralokinumab q2w and 58.5% of patients re-randomized to tralokinumab q4w, compared with 34.4% of patients re-randomized to placebo (Fig. 6b).
In week 16 tralokinumab responders in the ECZTRA 3 North American population, IGA 0/1 response was maintained at week 32 by 81.8% and 75.0% and EASI-75 response was maintained by 89.7% and 88.5% of patients receiving tralokinumab q2w and q4w, respectively (Fig. 6a and b).
Efficacy outcomes in the ECZTRA 1/2 and ECZTRA 3 non-North American population were comparable with the North American population during the maintenance treatment period (Table S4, see ESM); a slightly lower response was observed in the placebo arm in the ECZTRA 1/2 non-North American and North American populations, possibly due to a small number of patients.
Safety in the ECZTRA 1/2 and ECZTRA 3 North American Population
The overall AE rate was comparable between the tralokinumab and placebo groups during the initial 16-week treatment period in the ECZTRA 1/2 and ECZTRA 3 North American population (Table 3). The majority of AEs were mild or moderate in severity, with ~ 50% resolved or resolving at the end of the treatment period. Of the most frequently reported AEs (> 5% in any treatment groups), viral upper respiratory tract infection (ECZTRA 1/2: 10.5% vs 9.4%; ECZTRA 3: 8.6% vs 5.6%) and injection-site reaction (ECZTRA 1/2: 4.8% vs 0.7%; ECZTRA 3: 11.4% vs 0%) occurred more frequently with tralokinumab versus placebo, and dermatitis atopic (ECZTRA 1/2: 7.2% vs 21.6%; ECZTRA 3: 1.9% vs 7.4%) occurred less frequently with tralokinumab versus placebo.
In the initial 16-week treatment period, conjunctivitis occurred more often with tralokinumab versus placebo (ECZTRA 1/2: 2.4% vs 1.4%; ECZTRA 3: 2.9% vs 1.9%) (Table 3). All cases of conjunctivitis were mild or moderate in severity and most resolved at the end of the initial treatment period. No cases of keratitis or keratoconjunctivitis were reported (Table 3). Skin infections requiring systemic treatment occurred less frequently with tralokinumab compared with placebo in ECZTRA 1/2 (2.4% vs 6.5%) and ECZTRA 3 (1.9% vs 9.3%) (Table 3).
No marked differences in rates of serious AEs were observed between tralokinumab and placebo in the ECZTRA 1/2 (1.9% vs 2.9%) and ECZTRA 3 (0% vs 1.9%) North American population (Table 3).
In the maintenance treatment period, a slightly higher rate of AEs was reported with tralokinumab q2w in the ECZTRA 1/2 and ECZTRA 3 North American population than in the initial treatment period, although event severity and outcome with tralokinumab q2w was comparable to the initial treatment period (Table 4) and may be an artifact of the small number of patients analyzed.
Safety in the ECZTRA 1/2 and ECZTRA 3 non-North American population during the initial and maintenance treatment periods are summarized in Table S5 and Table S6 (see ESM).
Discussion
This is the first phase 3 trial post-hoc analysis evaluating the therapeutic efficacy of an anti-IL-13 biologic, used with or without TCS as needed, in a North American subpopulation of patients with moderate-to-severe atopic dermatitis. Tralokinumab showed greater improvement compared with placebo in all primary and secondary endpoints at week 16 in the ECZTRA 1/2 North American population and most primary and secondary endpoints at week 16 in the ECZTRA 3 North American population. In addition, IGA 0/1 and EASI-75 were sustained with tralokinumab at week 52 (in ECZTRA 1/2) and at week 32 (in ECZTRA 3). These results are similar to those observed in the ECZTRA 1/2 and ECZTRA 3 non-North American population (Table S2 and Table S4, see ESM). While direct comparison is not possible due to lack of head-to-head data, at week 16, 40% and 58.1% of the North American population in ECZTRA 3 achieved IGA 0/1 and EASI-75 with tralokinumab plus TCS as needed, respectively, which is similar to week 16 dupilumab plus TCS IGA 0/1 (39%) and EASI-75 (69%) response rates in the LIBERTY AD CHRONOS study [18]. However, compared with LIBERTY AD CHRONOS, placebo response rates were greater in the ECZTRA 3 North American population. This may be due to a number of factors, including: (1) a higher proportion of patients with moderate atopic dermatitis (IGA 3) at baseline; (2) the nature of the ECZTRA 3 study, where all patients had continued access to TCS; and (3) the greater amount of TCS use in patients receiving placebo compared with tralokinumab.
During the initial treatment period, rescue medication use was ~ 50% lower in tralokinumab-treated patients compared with those who received placebo in the ECZTRA 1/2 and ECZTRA 3 North American population. Of note, a considerably smaller proportion of the ECZTRA 1/2 North American population used rescue medications compared with the non-North American population (Table S3, see ESM). Overall, rescue medication use was low in the ECZTRA 3 North American and non-North American populations, possibly due to continued access to TCS. Greater tralokinumab responses were observed in the North American population in ECZTRA 3 compared with ECZTRA 1/2 at week 16, also likely due to TCS use as needed as an adjunct to treatment with tralokinumab. These ECZTRA 3 data reflect how moderate-to-severe atopic dermatitis might be treated in real-world settings, i.e., with a biologic combined with TCS [17].
Tralokinumab, with or without TCS, was well tolerated in the ECZTRA 1/2 and ECZTRA 3 North American population, with an overall safety profile consistent with the non-North American population (Table S5 and Table S6, see ESM). Of note, the proportion of patients experiencing ≥ 1 AE was lower in the North American population compared with the non-North American population. This may be explained by the greater proportion of patients with moderate disease, who are less likely to experience flares and skin infections compared to patients with severe disease [19, 20]. Additionally, regardless of treatment groups, conjunctivitis occurred with lower frequency in the ECZTRA 1/2 and ECZTRA 3 North American population compared with the non-North American population. This may reflect the lower proportion of patients in the North American population with severe disease at baseline, which has been identified as a risk factor for conjunctivitis in an analysis of five tralokinumab trials in adult patients with moderate-to-severe atopic dermatitis [21].
Limitations of this study include the small North American population sample sizes and multiplicity testing; only analyses included in the pre-specified ECZTRA 1/2 and ECZTRA 3 testing hierarchy were considered statistically significant. Although this post-hoc analysis of the North American population was exploratory in nature, differences were observed between treatment groups for most primary and secondary outcomes, comparable to the primary study population, where all primary and secondary endpoints were met [16, 17]. Of note, there was a difference between the proportion of ethnic minorities in the ECZTRA 1/2 and ECZTRA 3 North American population compared with the non-North American population. Approximately 30–52% of patients had skin of color in the ECZTRA 1/2 and ECZTRA 3 North American population compared with approximately 5–25% in the non-North American population across treatment groups. This is an important finding and represents a strength of this North American subanalysis, providing safety and efficacy data across several ethnicities in three large phase 3 programs.
Conclusions
Tralokinumab, with or without TCS, displayed similar efficacy and safety in patients with moderate-to-severe atopic dermatitis across the ECZTRA 1/2 and ECZTRA 3 North American population, comparable to that of the non-North American population. Tralokinumab, with or without TCS, was well tolerated in ethnically diverse North American populations, suggesting no special treatment considerations may be required for this subpopulation. Confirmation of the region-specific therapeutic efficacy and safety of tralokinumab may strengthen clinical decision-making, thereby benefiting patients from North America with moderate-to-severe atopic dermatitis.
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Acknowledgements
Funding
The ECZTRA 1/2 and ECZTRA 3 trials were sponsored by LEO Pharma A/S, Ballerup, Denmark. The sponsor of these studies will fund the mandatory Rapid Service Fee required for the publication of this manuscript in Dermatology and Therapy.
Medical Writing/Editorial Assistance
Medical writing and editorial support were provided by Henna Potigadoo, MSc, and Jade Moores, MSc, from Complete HealthVizion, funded by LEO Pharma.
Authorship
All named authors meet the International Committee of Medical Journal (ICMJE) criteria for authorship for this article, take responsibility for the integrity of the work as a whole, and have given their approval for this version to be published.
Author Contributions
Conceptualization: AB (equal), MG (equal), NB (equal), RGL (equal), SS (equal), JZ (equal), AK (equal), AA (equal), JIS (equal); Investigation: AB (equal), MG (equal), NB (equal), RGL (equal), SS (equal), JZ (equal), AK (equal), AA (equal), JIS (equal); Data curation: AK (lead); Formal analysis: AK (lead), SS (supporting); Methodology: AK (equal), SS (equal), JZ (equal); Visualization: AB (equal), MG (equal), NB (equal), RGL (equal), SS (equal), JZ (equal), AK (equal), AA (equal), JIS (equal); Writing – original draft: AB (equal), MG (equal), NB (equal), RGL (equal), SS (equal), JZ (equal), AK (equal), AA (equal), JIS (equal); Writing – review & editing: AB (equal), MG (equal), NB (equal), RGL (equal), SS (equal), JZ (equal), AK (equal), AA (equal), JIS (equal)
Prior Presentation
Part of the data in this manuscript has been presented at the Fall Clinical 2020 Dermatology Conference, Las Vegas, NV, USA, October 29–November 1, 2020 (https://doi.org/10.25251/skin.4.supp.97) and the American Academy of Dermatology Annual Meeting, San Francisco, CA, USA, March 19–23, 2021 (https://doi.org/10.1016/j.jaad.2021.06.726).
Disclosures
Andrew Blauvelt has served as a scientific adviser and/or clinical study investigator for AbbVie, Abcentra, Aligos, Almirall, Amgen, Arcutis, Arena, Aslan, Athenex, Boehringer Ingelheim, Bristol-Myers Squibb, Dermavant, Eli Lilly, Evommune, Forte, Galderma, Incyte, Janssen, Landos, LEO Pharma, Novartis, Pfizer, Rapt, Regeneron, Sanofi Genzyme, Sun Pharma, UCB Pharma, and Xencor. Melinda Gooderham is or has been an investigator, adviser, and/or speaker for AbbVie, Akros, Amgen, Arcutis, Boehringer Ingelheim, Bristol-Myers Squibb, Celgene, Coherus BioSciences, Dermavant, Dermira, Eli Lilly, Galderma, GlaxoSmithKline, Janssen, Kyowa Kirin, LEO Pharma, Medimmune, Merck, Novartis, Pfizer, Regeneron Pharmaceuticals, Inc., Roche, Sanofi Genzyme, Sun Pharma, UCB, and Valeant/Bausch. Neal Bhatia reports disclosures related to Almirall, Bristol-Myers Squibb, EPI Health, Incyte, J&J, LaRoche Posay, LEO Pharma, Pfizer, and Regeneron/Sanofi. Richard G. Langley has received honoraria as an advisory board member from AbbVie, Amgen, Boehringer Ingelheim, Celgene, Eli Lilly, LEO Pharma, Merck, Novartis, Pfizer, and UCB Pharma, and as a speaker from AbbVie, Amgen, Celgene, LEO Pharma, Merck, Novartis, and Pfizer. Shannon Schneider, and Azra Kurbasic are employees of LEO Pharma. John Zoidis is a former employee of LEO Pharma. April Armstrong reports grants from Bristol-Myers Squibb, Dermavant, Dermira, Eli Lilly, Galderma, Janssen-Ortho, Inc., Kyowa Hakko Kirin, LEO Pharma, Pfizer, and UCB Pharma; and has received honoraria from AbbVie, Boehringer Ingelheim/Parexel, Bristol-Myers Squibb, Dermavant, Eli Lilly, Janssen Pharmaceuticals, Inc., LEO Pharma, Modernizing Medicine, Novartis, Ortho Dermatologics, Pfizer, Regeneron Pharmaceuticals, Sanofi Genzyme, and Sun Pharma; and has acted as a speaker for AbbVie, Regeneron, and Sanofi Genzyme. Jonathan I. Silverberg reports personal fees from AbbVie, AnaptysBio, Arena, Asana, Bluefin, Boehringer Ingelheim, Celgene, Dermavant, Dermira, DS Biopharma Kiniksa, Eli Lilly, LEO Pharma, Luna, Menlo, Novartis, Pfizer, Realm, Regeneron, and Sanofi‐Genzyme, and grants and personal fees from Galderma and GlaxoSmithKline outside the submitted work.
Compliance with Ethics Guidelines
The ECZTRA 1, 2, and 3 studies were conducted in accordance with the ethical principles derived from international guidelines including the Declaration of Helsinki and Council for International Organizations of Medical Sciences International Ethical Guidelines and in compliance with International Council for Harmonisation guidelines for Good Clinical Practice. The clinical trials were approved by institutional review boards or ethics committees at each study site and followed the Consolidated Standards of Reporting Trials reporting guideline. All participants provided informed consent to participate in the trials.
Data Availability
Data will be made available upon request to the study sponsor, following review by the external Patient and Scientific Review Board.
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Blauvelt, A., Gooderham, M., Bhatia, N. et al. Tralokinumab Efficacy and Safety, with or without Topical Corticosteroids, in North American Adults with Moderate-to-Severe Atopic Dermatitis: A Subanalysis of Phase 3 Trials ECZTRA 1, 2, and 3. Dermatol Ther (Heidelb) 12, 2499–2516 (2022). https://doi.org/10.1007/s13555-022-00805-y
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DOI: https://doi.org/10.1007/s13555-022-00805-y