Definium Therapeutics Inc (DFTX) Study result summary
Event summary combining transcript, slides, and related documents.
Study result summary
22 Jun, 2026Study design and methodology
Phase III EMERGE study was a randomized, double-blind, placebo-controlled trial evaluating a single 100 µg dose of DT120 ODT in adults with major depressive disorder (MDD) over 12 weeks, followed by a 40-week open-label extension (Part B).
149 participants aged 18–74 with DSM-5-confirmed MDD were enrolled; 84–85% completed Part A, with demographics representative of the MDD population and high baseline severity (MADRS 34.5).
Participants were tapered off background antidepressants and anxiolytics, with no concurrent psychotherapeutic intervention.
The primary endpoint was MADRS score at week six, assessed by blinded central raters; key secondary endpoints included MADRS and CGI-S changes at Weeks 1, 6, and 12.
Part B allowed up to four open-label doses over 40 weeks for those with moderate or worse symptoms, with interim analysis showing mean MADRS at entry of 26.5.
Efficacy results
DT120 ODT showed rapid, robust, and durable efficacy, with an 8.1-point placebo-adjusted improvement on MADRS at week six and 7.3 points at week 12 (p<0.0001).
Rapid onset observed: 14.2-point MADRS separation from placebo at week one (p<0.0001).
Response (≥50% MADRS reduction) at week six was 35–41% for DT120 vs 7–13% for placebo; remission (MADRS ≤12) was 24% for DT120 vs 3% for placebo.
Statistically and clinically significant improvements were observed on all primary and key secondary endpoints, including CGI-S.
Efficacy was consistent across key subgroups, including those with treatment-resistant depression and prior psychedelic exposure.
Safety and tolerability
DT120 ODT was generally well tolerated; 99% of adverse events were mild to moderate, transient, and resolved on dosing day.
No serious adverse events, no suicidality signal, and no study withdrawals due to adverse events.
Most common adverse events included illusion (64%), euphoric mood (29%), and nausea (27%), with perceptual, affective, and behavioral changes expected during dosing.
Treatment session duration was predictable: average time to clear end-of-session checklist was 5.8 hours, with all participants cleared by 8 hours.
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