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Biological therapies have made great progress for patients with psoriasis, including long-term safety and efficacy, longer dosing intervals and oral therapies.

Biological therapies have made tremendous progress for patients with psoriasis with many products now available. At IFPA 2024, Prof. Bruce Strober, MD, PhD, from Yale University, in Connecticut presented recent data on biologics, including long-term safety and efficacy, longer dosing intervals and oral therapies¹.

A recent large data set showed that bimekizumab is effective in scalp psoriasis. An analysis of 5 phase three trials showed that 84–88% of participants with plaque psoriasis receiving bimekizumab achieved scalp Investigator’s Global Assessment (IGA) of 0 depending on the dose regimen². Furthermore, a pooled analysis of the same five trials showed that oral candidiasis occurs at decreasing yearly rates, inflammatory bowel disease was rare, and no active tuberculosis events were reported over 4 years of therapy³.

Another recent long-term phase 3 study was LIMMItless (NCT03047395) of risankizumab versus placebo⁴. At 6 years, 86–87% of participants achieved great than or equal to 90% improvement in Psoriasis Area and Severity Index (PASI90), with participants achieving and maintaining response by week 52. In terms of safety, no active tuberculosis or systemic candidiasis was reported and only 1 case of ulcerative colitis (<0.1% of participants).

The multipart GUIDE trial (NCT03818035) is assessing guselkumab treatment in patients with a short disease duration of psoriasis (<2 years)⁵. Part three of the trial assesses withdrawal of guselkumab 100 mg every 8 weeks or every 16 weeks treatment in patients initially ‘super-responders’ (PASI score 0) and who maintained PASI scores of less than 3. Following guselkumab treatment withdrawal, patients with ultra-short disease duration (<15 months) maintained their response much longer than patients with longer disease duration (median 450 days vs 291 days; P<0.0001).

JNJ-77242113 is a novel, small peptide, oral IL-23 receptor antagonist. This agent was assessed in the dose-ranging, randomized, phase 2 FRONTIER 1 trial (NCT05223868) in patients with PASI scores of greater or equal to 12⁶. All assessed dose groups significantly improved disease activity compared with placebo. The 100 mg twice daily dose group of JNJ-77242113 led to significantly higher proportions of patients achieving PASI75 versus placebo at week 16 (78.6% vs 9.3%; P<0.001), as well as proportions of patients with PASI90 (59.5% vs 2.3%; P<0.001) and PASI100 (40.5% vs 0%; P<0.001). “This is probably the best response we’ve had with an oral formulation,” said Prof. Strober. AEs more commonly reported with JNJ-77242113 included nasopharyngitis, diarrhea, and cough. Furthermore, a similar dose-ranging study FRONTIER 2 (NCT05364554) showed that 76.2% of patients receiving JNJ-77242113 100 mg twice daily achieved PASI75 at week 52, demonstrating maintenance of response with longer treatment⁷.

Prof. Storber concluded that earlier intervention in patients with lower body surface area can offer long durations of therapy for responders. “It’s probably better to start intervening earlier because the therapies are relatively safe now,” said Prof. Strober. “I think in the next 3 to 5 years we will be dosing biologics 6 to 12 months with the same efficacy as we see with the current products.” Finally, we will also see “better orals or oral biologics for patients who demand oral therapies.”

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