Skyrizi

Psoriatic Arthritis (PsA)

The safety and efficacy of Skyrizi were evaluated in 1407 subjects in 2 randomized, double-blind, placebo-controlled studies (964 in PsA-1 [NCT03675308] and 443 in PsA-2 [NCT03671148]) in patients 18 years and older with active psoriatic arthritis (PsA).

Patients in these studies had a diagnosis of PsA for at least 6 months based on the Classification Criteria for Psoriatic Arthritis (CASPAR), a median duration of PsA of 4.9 years at baseline, ≥ 5 tender joints and ≥ 5 swollen joints, and active plaque psoriasis or psoriatic nail disease at baseline.

In PsA-1, all subjects had a previous inadequate response or intolerance to non-biologic DMARD therapy and were biologic naïve. In PsA-2, 53.5% of subjects had a previous inadequate response or intolerance to non-biologic DMARD therapy, and 46.5% of subjects had a previous inadequate response or intolerance to biologic therapy. In both studies, subjects were randomly assigned to receive Skyrizi 150 mg or placebo at Weeks 0, 4, and 16. Starting from Week 28, all subjects received Skyrizi every 12 weeks. Both studies included a long-term extension for up to an additional 204 weeks. Regarding use of concomitant medications, 59.6% of subjects were receiving concomitant methotrexate (MTX), 11.6% were receiving concomitant non-biologic DMARDs other than MTX, and 28.9% were receiving SKYRIZI monotherapy. 

For both studies, the primary endpoint was the proportion of subjects who achieved an American College of Rheumatology (ACR) 20 response at Week 24.

In Study PsA-1, treatment with Skyrizi achieved the following improvements in ACR responses compared with placebo, respectively:

• ACR20 Response 

• Week 16: 56.3% vs 33.4% (treatment difference, 23.1%; 95% CI, 16.8-29.4; multiplicity-controlled P ≤.001)

• Week 24: 57.3% vs 33.5% (treatment difference, 24.0%; 95% CI, 18-30; multiplicity-controlled P ≤.001)

• ACR50 Response

• Week 16: 26.4% vs 11.1% (treatment difference, 15.4%; 95% CI, 10.6-20.2)

• Week 24: 33.4% vs 11.3% (treatment difference, 22.2%; 95% CI, 17.3-27.2)

• ACR70 Response 

• Week 16: 11.8% vs 2.7% (treatment difference, 9.2%; 95% CI, 6.1-12.4)

• Week 24: 15.3% vs 4.7% (treatment difference, 10.5%; 95% CI, 6.9-14.2)

In Study PsA-2, treatment with Skyrizi achieved the following improvements in ACR responses compared with placebo, respectively:

• ACR20 Response 

• Week 16: 48.3% vs 25.3% (treatment difference, 22.6%; 95% CI, 13.9-31.2; multiplicity-controlled P ≤.001)

• Week 24: 51.3% vs 26.5% (treatment difference, 24.5%; 95% CI, 15.9-33.0; multiplicity-controlled P ≤.001)

• ACR50 Response 

• Week 16: 20.3% vs 6.8% (treatment difference, 13.5%; 95% CI, 7.3-19.7)

• Week 24: 26.3% vs 9.3% (treatment difference, 16.6%; 95% CI, 9.7-23.6)

• ACR70 Response 

• Week 16: 11.2% vs 3.4% (treatment difference, 7.8%; 95% CI, 3.0-12.6)

• Week 24: 12.0% vs 5.9% (treatment difference, 6.0%; 95% CI, 0.8-11.3)

In Studies PsA-1 and PsA-2, treatment with Skyrizi had a mean change from baseline in ACR components compared with placebo, respectively:

• Number of Swollen Joints (0-66)

• Week 16: -7.7 and -8.0 vs -5.5 and -5.4

• Week 24: -8.7 and -9.1 vs -6.7 and -6.5

• Number of Tender Joints (0-68)

• Week 16: -10.7 and -11.3 vs -6.3 and -6.0

• Week 24: -12.0 and -13.0 vs -7.9 and -8.3

• Patient’s Assessment of Pain

• Week 16: -18.4 and -14.4 vs -8.6 and -5.7

• Week 24: -21.4 and -15.3 vs -10.9 and -8.7

• Patient’s Global Assessment 

• Week 16: -19.4 and -17.0 vs -10.2 and -4.9

• Physician’s Global Assessment 

• Week 16: -31.1 and -32.7 vs -18.3 and -19.0

• Week 24: -34.8 and -35.5 vs -22.2 and -21.3

• Health Assessment Questionnaire - Disability Index (HAQ-DI)

• Week 16: -0.3 and -0.2 vs -0.1 and -0.1

• Week 24: -0.3 and -0.2 vs -0.1 and -0.1

• High sensitivity C-reactive protein (hs-CRP) mg/L 

• Week 16: -4.8 and -2.1 vs -0.3 and -0.1

• Week 24: -4.3 and -1.8 vs -0.2 and -0.5

Treatment with Skyrizi resulted in improvement in dactylitis and enthesitis in patients with pre-existing dactylitis or enthesitis. In patients with coexistent plaque psoriasis receiving Skyrizi, the skin lesions of psoriasis improved with treatment, relative to placebo, as measured by the Psoriasis Area Severity Index (PASI 90) at Week 24.

Physical Function: In both studies, patients treated with Skyrizi showed statistically significant improvement from baseline in physical function compared with placebo as assessed by HAQ-DI at Week 24. The mean difference (95% CI) from placebo in HAQ-DI change from baseline at Week 24 was -0.20 (-0.26, -0.14) in study PsA-1 and -0.16 (-0.26, -0.07) in study PsA-2.

In both studies, a greater proportion of subjects achieved a reduction of at least 0.35 in HAQ-DI score from baseline in the Skyrizi group compared with placebo at Week 24.

Other Health Related Outcomes: In both studies, general health status was assessed by the 36-Item Short Form Health Survey (SF36 V2). Fatigue was assessed by Functional Assessment of Chronic Illness Therapy Fatigue Scale (FACIT-Fatigue).

In both studies at Week 24, patients treated with Skyrizi showed improvements in the SF-36 physical component summary scores compared with subjects who received placebo. There were also numerical improvements in patients treated with Skyrizi in physical functioning, role physical, bodily pain, general health, vitality, social functioning, mental health, role emotional domain scores and mental component summary scores in both studies at week 24 compared to placebo. In both studies at Week 24, patients treated with Skyrizi showed improvements in FACIT-Fatigue scores compared with subjects who received placebo.

For more trial data: see full labeling.

Crohn’s Disease

Induction Trials (Studies CD-1 and CD-2)

In two 12-week induction studies (CD-1; NCT03105128 and CD-2; NCT03104413), patients with moderately to severely active Crohn’s disease were randomly assigned to receive Skyrizi 600 mg, Skyrizi 1,200 mg, or placebo as an intravenous infusion at Week 0, Week 4, and Week 8. Moderately to severely active CD was defined as a Crohn’s Disease Activity Index (CDAI) of 220 to 450 and Simple Endoscopic Score for Crohn’s disease (SES-CD) ≥6 (or ≥4 for isolated ileal disease). Subjects with inadequate response, loss of response, or intolerance to oral aminosalicylates, corticosteroids, immunosuppressants, and/or biologic therapy were enrolled.

The coprimary endpoints for both studies were clinical remission and endoscopic response at Week 12. Secondary endpoints included clinical response and endoscopic remission. The Skyrizi 1,200 mg dosage did not demonstrate additional treatment benefit over the 600 mg dosage and is not a recommended regimen.

In Study CD-1, a greater proportion of patients treated with Skyrizi 600 mg achieved the following efficacy endpoints at week 12 compared with placebo, respectively:

• Clinical remission: 45% vs 25% (treatment difference 21%; 95% CI, 12-29; P <.001)

• Endoscopic response: 40% vs 12% (treatment difference 28%; 95% CI, 21-35; P <.001)

• Clinical response: 60% vs 37% (treatment difference 23%; 95% CI, 14-32; P <.001)

• Endoscopic remission: 24% vs 9% (treatment difference 15%; 95% CI, 9-21; P <.001)

In Study CD-2, a greater proportion of patients treated with Skyrizi 600 mg achieved the following efficacy endpoints at week 12 compared with placebo, respectively:

• Clinical remission: 42% vs 20% (treatment difference 22%; 95% CI, 13-31; P <.001)

• Endoscopic response: 29% vs 11% (treatment difference 18%; 95% CI, 10-25; P <.001)

• Clinical response: 60% vs 30% (treatment difference 29%; 95% CI, 20-39; P <.001)

• Endoscopic remission: 19% vs 4% (treatment difference 15%; 95% CI, 9-21; P <.001)

Onset of clinical response and clinical remission based on CDAI occurred as early as Week 4 in a greater proportion of patients treated with the Skyrizi 600 mg induction regimen compared to placebo.

Reductions in stool frequency and abdominal pain were observed in a greater proportion of patients treated with the Skyrizi 600 mg induction regimen compared to placebo. 

For more trial data: see full labeling.

Study CD-3

The maintenance study CD-3 evaluated 382 patients who achieved clinical response defined as a reduction in CDAI of at least 100 points from baseline after 12 weeks of induction treatment with intravenous Skyrizi in studies CD-1 and CD-2. Patients were randomly assigned to receive a maintenance regimen of Skyrizi 180 mg or Skyrizi 360 mg or placebo at Week 12 and every 8 weeks thereafter for up to an additional 52 weeks. The co-primary endpoints in CD-3 were clinical remission and endoscopic response at Week 52.

Results showed that treatment with Skyrizi 180mg and 360mg achieved the following efficacy endpoints at week 52 compared with placebo, respectively:

• Clinical remission: 61% (treatment difference, 17%; 95% CI, 6-28; P <.05) and 57% (treatment difference, 14%; 95% CI, 3-26; P <.05) vs 46%

• Endoscopic response: 50% (treatment difference, 30%; 95% CI, 20-39; P <.05) and 48% (treatment difference, 31%; 95% CI, 21-41; P <.05) vs 22%

Endoscopic remission was observed at Week 52 in 33% (44/135) of patients treated with the Skyrizi 180 mg maintenance regimen and 41% (48/117) of patients treated with the Skyrizi 360 mg maintenance regimen, compared to 13% (17/130) of patients treated with placebo. This endpoint was not statistically significant under the prespecified multiple testing procedure.

Plaque Psoriasis

Four multicenter, randomized, double-blind studies [PsO-1 (NCT02684370), PsO-2 (NCT02684357), PsO-3 (NCT02672852), and PsO-4 (NCT02694523)] enrolled 2109 patients 18 years of age and older with moderate to severe plaque psoriasis who had a body surface area (BSA) involvement of ≥10%, a static Physician’s Global Assessment (sPGA) score of ≥3 (“moderate”) in the overall assessment (plaque thickness/induration, erythema, and scaling) of psoriasis on a severity scale of 0 to 4, and a Psoriasis Area and Severity Index (PASI) score ≥12.

Studies PsO-1 and PsO-2: 997 patients were randomly assigned to receive either Skyrizi 150mg (n=598), placebo (n=200), or a biologic active control (n=199) at weeks 0, 4, and every 12 weeks thereafter. The coprimary endpoints were the proportion of patients who achieved an sPGA score of 0 “clear” or 1 “almost clear” and the proportion of patients who achieved at least a 90% reduction from baseline PASI (PASI 90) at week 16. Secondary endpoints included the proportion of patients who achieved PASI 100, sPGA 0, and Psoriasis Symptom Scale (PSS) 0 at week 16.

In the PsO-1 study, a greater proportion of patients in the Skyrizi treatment arm achieved the primary and secondary endpoints at week 16 vs those in the placebo arm, respectively:

• sPGA 0 or 1: 88% vs 8%

• PASI 90: 75% vs 5%

• sPGA 0: 37% vs 2%

• PASI 100: 36% vs 0%

In the PsO-2 study, a greater proportion of patients in the Skyrizi treatment arm achieved the primary and secondary endpoints at week 16 vs those in the placebo arm, respectively:

• sPGA 0 or 1: 84% vs 5%

• PASI 90: 75% vs 2%

• sPGA 0: 51% vs 3%

• PASI 100: 51% vs 2%

In both the PsO-1 and PsO-2 studies at week 52, patients treated with Skyrizi also achieved sPGA 0 (58% and 60%, respectively), PASI 90 (82% and 81%, respectively), and PASI 100 (56% and 60%, respectively). 

Moreover, in both studies, treatment with Skyrizi showed improvements in signs and symptoms related to pain, redness, itching and burning at week 16 compared to placebo as assessed by the PSS. In PsO-1 and PsO-2, about 30% of the subjects who received Skyrizi achieved PSS 0 (“none”) at Week 16 compared to 1% of the subjects who received placebo. 

Study PsO-3: 507 patients were randomly assigned to receive either Skyrizi (n=407) or placebo (n=100) at weeks 0, 4, and every 12 weeks thereafter. At Week 16, Skyrizi was superior to placebo on the co-primary endpoints of sPGA 0 or 1 (84% Skyrizi and 7% placebo) and PASI 90 (73% Skyrizi and 2% placebo). The respective response rates for Skyrizi and placebo at Week 16 were: sPGA 0 (46% Skyrizi and 1% placebo); PASI 100 (47% Skyrizi and 1% placebo); and PASI 75 (89% Skyrizi and 8% placebo). 

Maintenance and Durability of Response: In PsO-1 and PsO-2, among the subjects who received Skyrizi and had PASI 100 at Week 16, 80% (206/258) of the subjects who continued on Skyrizi had PASI 100 at Week 52. For PASI 90 responders at Week 16, 88% (398/450) of the patients had PASI 90 at Week 52. 

In PsO-3, patients who were originally on Skyrizi and had sPGA 0 or 1 at Week 28 were re-randomized to continue Skyrizi every 12 weeks or withdrawal of therapy. At Week 52, 87% (97/111) of the patients re-randomized to continue treatment with Skyrizi had sPGA 0 or 1 compared to 61% (138/225) who were re-randomized to withdrawal of Skyrizi. 

For more trial data: see full labeling.