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Efficacy outcomes from PSO-1

SOTYKTU was studied in two global, Phase 3, randomised, multi-arm clinical studies^1,2

Key eligibility criteria^1,3

Adults with moderate-to-severe plaque psoriasis + PASI ≥12, sPGA ≥3, BSA ≥10%
Stratified by geographic region, body weight, and prior biologic use

Selected exclusion criteria^1,3

Prior treatment with SOTYKTU or apremilast
History or evidence of active infection, including latent or active TB
Other forms of psoriasis

POETYK PSO-1¹

A chart comparing Sotyktu vs. placebo at Week 16 of the POETYK PSO-1 study

Adapted from Armstrong A et al. 2023.

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Co-primary endpoints at Week 16 (vs. placebo)^1,3

PASI 75
sPGA 0/1

Selected secondary endpoints^1,3

sPGA 0/1 at Week 16, 24 and 52
sPGA 0 at Week 16
PASI 75 at Week 16, 24 and 52
PASI 90 at Week 16, 24 and 52
PASI 100 at Week 16
ss-PGA 0/1 at Week 16
PSSD symptom score at Week 16
DLQI 0/1 at Week 16

This is a selection of secondary endpoints from PSO-1

baseline characteristics

*Apremilast was titrated from 10 mg QD to 30 mg BID over the first 5 days of dosing¹
BID, twice daily; BSA, Body Surface Area; DLQI, Dermatology Life Quality Index; PASI, Psoriasis Area and Severity Index; PSSD, Psoriasis Symptoms and Signs Diary; QD, once daily; sPGA, static Physician’s Global Assessment; ssPGA, scalp-specific Physician's Global Assessment.

SOTYKTU demonstrated superior efficacy vs. placebo (at 16 weeks) and across key secondary
endpoints in the PSO-1 study^1,4

A graph showing Sotyktu vs. placebo (at 16 weeks) and across key secondary endpoints in the PSO-1 study

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Co-primary endpoints¹

PASI 75 at Week 16 vs. placebo
sPGA 0/1 at Week 16 vs. placebo

A table breaking down the data generated through the POETYK PSO-2 study

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Selected secondary endpoints^1,3

sPGA 0/1 at Week 16, 24 and 52
sPGA 0 at Week 16
PASI 75 at Week 16, 24 and 52
PASI 90 at Week 16, 24 and 52
PASI 100 at Week 16
Scalp-specific PGA 0/1 at Week 16
PSSD symptom score at Week 16
DLQI 0/1 at Week 16

*p≤0.0001 for comparison between SOTYKTU and placebo or SOTYKTU and apremilast.^1,4
^†p<0.001 for comparison between SOTYKTU and apremilast.^1,4
^‡Includes patients with baseline Scalp Specific PGA score of ≥3.^1,4
Missing data were imputed using NRI method; patients who discontinued treatment or the study prior to the endpoint or had missing data were counted as non-responders.
DLQI, Dermatology Life Quality Index; NRI, non-responder imputation; PASI, Psoriasis Area and Severity Index; PGA, Physician’s Global Assessment; PSSD, Psoriasis Symptoms and Signs; SE, standard error; sPGA, static Physician’s Global Assessment.

SOTYKTU demonstrated superior efficacy vs. placebo at Week 16 (co-primary endpoint)^1,4

PSO-1 co-primary endpoints: PASI 75 response and sPGA 0/1 response rates were superior vs. placebo at Week 16^1,4,5

PASI 75

sPGA 0/1

Adapted from Armstrong A et al. 2023, SOTYKTU SmPC & SOTYKTU EPAR.
PSO-1: SOTYKTU (n=332), apremilast (n=168), placebo (n=166)¹

Missing data were imputed using NRI method.
PASI 75 and sPGA were co-primary endpoints in the Phase 3 POETYK study. PASI 75 was defined as ≥75% reduction from baseline PASI.
NRI, no-responder imputation; PASI, Psoriasis Area and Severity Index; sPGA, static Physician’s Global Assessment.

SOTYKTU demonstrated superior efficacy vs. apremilast at Week 24 (secondary endpoint)^1,4

PSO-1 secondary endpoint: PASI 75 response and sPGA 0/1 response rates were significantly improved vs. apremilast at Week 24^1,4,5

PASI 75

A graph showing Sotyktu efficacy vs. apremilast at Week 24 of the trial (secondary endpoint)

sPGA 0/1

Adapted from Armstrong A et al. 2023, SOTYKTU SmPC & SOTYKTU EPAR.
PSO-1: SOTYKTU (n=332), apremilast (n=168), placebo (n=166)¹

SOTYKTU demonstrated superior efficacy vs. placebo at Week 16 (co-primary endpoint),
and vs. apremilast at Week 24 (secondary endpoint)^1,4

PSO-1: maximum PASI 75 response was achieved by Week 24 and maintained through Week 52^1,4,5

PASI 75

A graph showing Sotyktu efficacy vs. placebo at Week 16 (co-primary endpoint), and vs. apremilast at Week 24 (secondary endpoint)

Adapted from Armstrong A et al. 2023, SOTYKTU SmPC & SOTYKTU EPAR.
PSO-1: SOTYKTU (n=332), apremilast (n=168), placebo (n=166)¹

An icon representing pinch to zoom Pinch & zoom to explore

PSO-1: sPGA 0/1 respones rates continued to improve through Week 24 and were maintained through to Week 52^1,4,5

sPGA 0/1

Adapted from Armstrong A et al. 2023, SOTYKTU SmPC & SOTYKTU EPAR.
PSO-1: SOTYKTU (n=332), apremilast (n=168), placebo (n=166)¹

An icon representing pinch to zoom Pinch & zoom to explore

*p≤0.001 for comparison between SOTYKTU and placebo or SOTYKTU and apremilast.^1,4
^†p<0.001 for comparison between SOTYKTU and apremilast.^1,4
Missing data were imputed using NRI method.
PASI 75 and sPGA were co-primary endpoints in the Phase 3 POETYK study. PASI 75 was defined as ≥75% reduction from baseline PASI.
NRI, no-responder imputation; PASI, Psoriasis Area and Severity Index; sPGA, static Physician’s Global Assessment.

References

Armstrong A et al. J Am Acad Dermatol. 2023;88(1):29–39. Plus supplementary material.
Strober B et al. J Am Acad Dermatol. 2023;88(1):40–51. Plus supplementary material.
Clinicaltrials.gov. Effectiveness and Safety of BMS-986165 Compared to Placebo and Active Comparator in Participants with Psoriasis (POETYK-PSO-1). NCT03624127. Available at
https://clinicaltrials.gov/ct2/show/NCT03624127?term=poetyk&draw=2&rank=2 (Accessed August 2023).
SOTYKTU. Summary of Product Characteristics
SOTYKTU. European Product Assessment Report (EPAR). 26 January 2023. Available at https://www.ema.europa.eu/en/documents/assessment-report/sotyktu-epar-public-assessment-report_en.pdf (Accessed August 2023).