Dermata Therapeutics has reported positive topline data from the Phase Ib clinical trial where its product candidate, DMT310, was assessed to treat subjects with mild-to-moderate psoriasis.
Possessing mechanical and chemical mechanisms of action, DMT310 is a multifactorial drug obtained naturally from a peculiar freshwater sponge and processed into a powder.
The powder is combined with a fluidising agent just before the application to the target area.
The multicentre, single-arm, open-label, proof of concept, 12-week target lesion Phase Ib trial analysed the safety, tolerability and efficacy of DMT310 given once a week in 30 subjects.
These patients had mild-to-moderate psoriatic plaque spreading over 2%-30% of body surface area.
Findings showed that at week eight, 29.6% of the subjects who received the DMT310 treatment attained a Physician’s Global Assessment (PGA) score of 0 or 1.
How well do you really know your competitors?
Access the most comprehensive Company Profiles on the market, powered by GlobalData. Save hours of research. Gain competitive edge.
Thank you!
Your download email will arrive shortly
Not ready to buy yet? Download a free sample
We are confident about the unique quality of our Company Profiles. However, we want you to make the most beneficial decision for your business, so we offer a free sample that you can download by submitting the below form
By GlobalDataApproximately 25.9% of the subjects had a total Psoriasis Area Severity Index (PASI) score of 0 or 1 at week eight.
At the same time period, DMT310 offered a 19.6% decline from baseline in pruritis for the target lesion.
Furthermore, DMT310 was found to be safe with just three adverse events (AEs) observed in the trial.
Of these three AEs, two were associated with DMT310 while no serious adverse events (SAEs) were noted.
Dermata Development senior vice-president Christopher Nardo said: “Importantly, the treatment effect and tolerability observed in this Phase Ib target lesion study provides support for exploring a treatment regimen with more frequent than once-weekly applications, improved application techniques, or more drug per application site, which could be more effective for moderate psoriasis patients with thicker psoriatic plaques.
“Therefore, we have initiated additional work in an ex vivo skin model to evaluate dosing frequency and product application to better inform the clinical trial design for a future Phase II psoriasis study.”