A randomised, controlled, parallel-group, phase 2a trial (NCT03754309) investigated the non-depleting anti-OX40 ligand antibody amlitelimab for the treatment of moderate-to-severe AD [1]. “By blocking the interaction of antigen-presenting cells and T cells rather high up in the immune cascade, amlitelimab has the benefit of impacting not only type 2 pathways but also other immune axes, in particular Th17, Th22, and Th1 pathways, that have all been implicated in AD in particular in chronic-lesional stages,” Prof. Stephan Weidinger (University Hospital Schleswig-Holstein, Germany) explained the special features of the study drug. The current study defined the number of treatment-emergent adverse events (AE) and efficacy as determined by % change from baseline in the Eczema Area and Severity Index (EASI) score at week 16 as co-primary endpoints.
The 88 treated adult participants with AD were all withdrawn from their topical medication, including corticosteroids, 14 days before baseline. They were randomised to either amlitelimab high dose (i.e. 500 mg loading/250 mg every 4 weeks), low dose (i.e. 200 mg loading/100 mg every 4 weeks), or placebo. “In patients who achieved an Investigator’s Global Assessment (IGA) of 0/1 [representing clear or almost clear skin] at week 16, in addition to safety, efficacy measures were taken to investigate the durability of response,” Prof. Weidinger pointed out.
The mean proportion of affected body surface area was around 50% and the mean EASI score was about 30. The safety endpoint was met, as the rate of treatment-emergent AEs was similar between active arms and placebo. “When AEs are ranked in system organ class by frequency, it is not surprising to see infections as the most frequently reported events. There was no meaningful imbalance between amlitelimab and placebo, and the most commonly seen events were nasopharyngitis, folliculitis, and upper respiratory tract infections,” stated Prof. Weidinger.
Durable response for several months without treatment
As for efficacy in terms of percentage EASI change from baseline, the onset of action was apparent as early as day 15 and continued to increase. “Even with rather strong placebo responses, both doses were statistically significantly superior over placebo at week 12, when the last dose was applied, and amlitelimab low dose also demonstrated superiority at week 16, so 4 weeks after the last dose,” Prof. Weidinger stressed. The proportions of patients with a clinically meaningful ≥4-point itch reduction in the numeric rating scale were 57.9% (low dose) and 62.5% (high dose) compared with 38.1% in the placebo group. Furthermore, the results for achieving IGA 0/1 were significantly greater for both high-dose and low-dose amlitelimab compared with placebo at days 57, 85, and 113 (P<0.001 for all time points). “Interestingly, in around 70% of patients, this excellent response was maintained over time until day 253, so it was maintained for several months without treatment. This could indicate a long and sustained response following the last dose, opening up the opportunity of extended dosing,” Prof. Weidinger remarked.
He summarised that the novel, non-depleting, anti-OX40 ligand monoclonal antibody amlitelimab demonstrated robust efficacy in the treatment of moderate-to-severe AD with an acceptable and unremarkable safety profile. A phase 2b dose-ranging study is being planned.
- Weidinger S. A phase 2a study of KY1005, a novel non-depleting anti-OX40 ligand (OX40L) mAb in patients with moderate to severe AD. D1T01.3A, EADV Congress 2021, 29 Sept–2 Oct.
Copyright ©2021 Medicom Medical Publishers
Posted on
Previous Article
« Superior EASI scores after switch from dupilumab to upadacitinib Next Article
Women with breast cancer at increased risk for developing atrial fibrillation »
« Superior EASI scores after switch from dupilumab to upadacitinib Next Article
Women with breast cancer at increased risk for developing atrial fibrillation »
Table of Contents: EADV 2021
Featured articles
Letter from the Editor
Long-term disease control in AD could be in reach with anti-OX40 antibody KHK4083
Late-Breaking News
Targeting OX40 in the treatment of atopic dermatitis meets expectations
Superior EASI scores after switch from dupilumab to upadacitinib
CSU: Novel agent targeting Bruton’s tyrosine kinase leads to disease control
Novel JAK3/TEC blocker leads to maintained re-pigmentation in vitiligo
TYK2 inhibitor deucravacitinib shows impressive long-term response in psoriasis
Tapinarof cream for psoriasis leads to high clearance rates and remittive effect
CSU: Ligelizumab likely safe and effective for adolescents
Long-term disease control in AD could be in reach with anti-OX40 antibody KHK4083
Topical JAK1/JAK2 inhibitor effective in vitiligo
Abrocitinib demonstrates fast itch control and skin clearance in atopic dermatitis
AD patients with stable response fare well with a monthly dose of tralokinumab
Opioid receptor agonist difelikefalin disappoints in AD
Atopic Dermatitis: State of the Art
Upadacitinib beats dupilumab in different body regions
Efficacious 2-year AD control with IL-13 inhibitor tralokinumab
Ruxolitinib cream: a safe treatment for elderly AD patients
Novel and upcoming targeted AD treatment
Psoriasis: What's New?
Existing and upcoming small molecules in psoriasis
Treating psoriasis during pregnancies
A patient-related approach to freedom of disease
Ixekizumab superior to secukinumab in real-world psoriasis study
Nail psoriasis: An important target to be treated
Grand debate: Is psoriasis a systemic or skin-only disease?
Spotlight on Alopecia Areata
JAK1/2: A promising novel treatment target in alopecia areata
Alopecia areata: encouraging response rates with JAK3/TEC inhibition
Related Articles
November 18, 2021
Nail psoriasis: An important target to be treated
November 18, 2021
Efficacious 2-year AD control with IL-13 inhibitor tralokinumab
© 2024 Medicom Medical Publishers. All rights reserved. Terms and Conditions | Privacy Policy
HEAD OFFICE
Laarderhoogtweg 25
1101 EB Amsterdam
The Netherlands
T: +31 85 4012 560
E: publishers@medicom-publishers.com