Apogee Therapeutics (APGE) Study result summary
Event summary combining transcript, slides, and related documents.
Study result summary
23 Mar, 2026Study design and objectives
The phase II APEX Part A study was a 52-week, double-blind, placebo-controlled trial evaluating zumilokibart in adults with moderate-to-severe atopic dermatitis, focusing on maintenance and deepening of efficacy with every 3- or 6-month dosing after induction.
Patients were re-randomized at week 16 to receive maintenance dosing every 3 months (Q3M/Q12W) or every 6 months (Q6M/Q24W); placebo patients crossed over to active treatment.
Safety and efficacy were evaluated across all patients, regardless of initial response at week 16, and baseline demographics were consistent with AD trials.
The study design mirrored upadacitinib phase III trials and included a dose optimization component (Part B), with results expected in Q2 2026.
Patients crossing over from placebo to zumilokibart achieved similar efficacy by week 52.
Key efficacy results
At week 52, zumilokibart maintained EASI-75 response in 75% (Q3M) and 85% (Q6M) of patients; IGA 0/1 was maintained in 86% (Q3M) and 78% (Q6M).
Deepening of response was observed, with IGA 0/1 rates rising from 37% at week 16 to 52% (Q6M) and 72% (Q3M) at week 52, and EASI-75 rates increasing to 81% (Q6M) and 88% (Q3M).
EASI-100 (clear skin) was achieved in 19% (Q6M) and 41% (Q3M) at week 52; EASI and itch NRS reductions reached up to 88% and 77%, respectively, among EASI-75 responders.
Deepening of response was seen across all endpoints, including EASI-90 and EASI-100, with up to 36 percentage points improvement.
Responses continued to improve over time, including in patients who did not fully respond in the first 16 weeks.
Safety and tolerability
Zumilokibart was well tolerated over 52 weeks, with a safety profile consistent with the IL-13 class; 71.4% of patients reported at least one TEAE and 0.8% reported a serious TEAE.
Most common adverse events were non-infective conjunctivitis (13.4–20.2%), upper respiratory tract infection (12.6%), nasopharyngitis (9.2%), and atopic dermatitis.
Conjunctivitis occurred in 20.2% of patients, with less than 1% discontinuation; rates were similar to dupilumab and lebrikizumab.
Most conjunctivitis cases were short-lived (median 27.5 days), resolved within 90 days, and were unrelated to drug exposure.
No impact of anti-drug antibodies on PK, efficacy, or safety was observed.
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