Table 2.
Clinical trial | |||||||
---|---|---|---|---|---|---|---|
Authors, year | Study type | No. of prt | Study design (study groups) | Study period | Efficacy | Safety | Ref |
Papp et al., 2017 |
Phase II, multicentre, randomized, dose-ranging trial Double-blind within risankizumab dose groups and single-blind (patients) with regard to drug |
116 |
1)Single 18-mg SC dose of risankizumab at week 0 2)90-mg dose of risankizumab at weeks 0, 4, and 16 3)180-mg dose of risankizumab at weeks 0, 4, and 16 4)Ustekinumab 45 mg or 90 mg depending on body weight at weeks 0, 4, and 16 |
48 weeks |
Week 12: PASI90 73% in 90-mg risankizumab, 81% in the 180-mg risankizumab versus 40% in ustekinumab. At least PASI75 was achieved in 63% in the 18-mg risankizumab, 98% in the 90-mg, and 88% in the 180-mg, as compared to 72% in ustekinumab Week 24: At least PASI75 was achieved in 53% of 18-mg risankizumab, 90% in the 90-mg, 88% in the 180-mg, compared to 70% in the ustekinumab |
In the 18-mg and 90-mg risankizumab and the ustekinumab group 12%, 15%, and 8%, respectively had serious AEs, including 2 BCCs and 1 major cardiovascular adverse event. No serious AEs in the 180-mg risankizumab group were found | 61 |
Gordon et al., 2018 |
Replicate phase III, randomized, placebo-controlled, and active comparator-controlled trial UltIMMa-1 and UltIMMa-2 |
997 |
1)150 mg risankizumab at weeks 0, 4, 16, 28, and 40 2)Ustekinumab based on weight (45 mg or 90 mg) at weeks 0, 4, 16, 28, and 40 3)Placebo at weeks 0 and 4 → 150 mg risankizumab at weeks 16, 28, and 40 |
52 weeks |
Week 16: UltIMMa-1: PASI90 was achieved by 75.3% risankizumab group, 4.9% placebo group, and 42% of the ustekinumab group UltIMMa-2: PASI90 was achieved by 74.8% risankizumab group, 2% placebo group, and 47.5% of the ustekinumab group UltIMMa-1: sPGA 0 or 1 was achieved by 87.7% risankizumab group, 7.8% placebo, and 63% ustekinumab group UltIMMa-2: sPGA 0 or 1 was achieved by 83.7% risankizumab group, 5.1% placebo, and 61.6% ustekinumab group |
Treatment-related AEs in UltIMMa-1 and UltIMMa-2 in risankizumab group were found in 49.7% and in 45.6%. Serious AEs were reported in 2.3% of patients on risankizumab in UltIMMa-1 and in 2% in UltIMMa-2 | 21 |
Ohtsuki et al., 2019 |
Phase II / III, randomized, double-blinded, placebo-controlled trial SustalMM |
171 Japanese |
1)75 mg risankizumab weeks 0, 4, 16, 28, and 40 2)150 mg risankizumab weeks 0, 4, 16, 28, and 40 3)Placebo weeks 0 and 4 → 75 mg risankizumab weeks 16, 28, and 40 4)Placebo weeks 0 and 4 → 150 mg risankizumab weeks 16, 28, and 40 |
52 weeks |
Week 16: Risankizumab 75 and 150 mg superior versus placebo for PASI90 (75.9%, 74.5%, and 1.7%, respectively) (p < 0.001). PASI75 for risankizumab 75 and 150 mg were significantly higher than placebo (89.7%, 94.5%, and 8.6%, respectively) sPGA score of 0 or 1 was achieved by 86.2% and 92.7% versus 10.3% for risankizumab 75, 150 mg versus placebo Week 52: PASI90 and PASI100 were achieved by 86.2% and 43.1% in risankizumab 75 mg; 92.7% and 41.8% in the risankizumab 150 mg |
The safety profile was consistent with previous trials, no new or unexpected safety events were found | 72 |
Reich et al., 2019 |
Phase III, randomized, double-blind, active-comparator-controlled trial IMMvent |
605 |
1)Risankizumab 150 mg week 0 and 4 2)Adalimumab 80 mg at randomization, then 40 every 2 weeks until week 15 Week 16: 1)Patients remained in risankizumab group (150 mg at week 16 and 28) 2)Adalimumab intermediate responders → re-randomized to continue 40 mg adalimumab every other week or switch to risankizumab 150 mg (week 16, 20, and 32). Responders to adalimumab (PASI90) remained on adalimumab every other week |
44 weeks |
Week 16: A significantly higher proportion of patients who were assigned to risankizumab achieved PASI90 and sPGA scores of clear or almost clear compared to adalimumab (72% versus 47% and 84% versus 60%, respectively) Week 44: Among adalimumab intermediate responders a larger proportion of patients that were rerandomized to risankizumab achieved PASI90, and PASI 100 |
In part A AEs occurred in 56% on risankizumab and 57% on adalimumab, with serious AE in 3% of risankizumab and 3% of adalimumab. The most frequently reported were viral upper respiratory tract infection, upper respiratory tract infection, and headache | 63 |
Blauvelt et al., 2020 |
Phase III, randomized, double-blind, placebo-controlled trial IMMhance |
507 |
1)Risankizumab 150 mg at weeks 0 and 4 2)Placebo at weeks 0 and 4 Week 16: All patients received risankizumab 150 mg Week 28: 1)Patients with risankizumab that achieved an sPGA of 0/1 were rerandomized to risankizumab or placebo every 12 weeks 2)Patients with an inadequate response to initial therapy received open-label risankizumab 150 mg every 12 weeks |
104 weeks |
Week 16: 73.2% patients in the risankizumab group achieved PASI90 versus 2% in placebo. 83.5% receiving risankizumab versus 7% receiving placebo achieved sPGA 0/1 scores Week 52: sPGA score of 0/1 was achieved by 87.4% of risankizumab versus 61.3% receiving placebo Week 104: the sPGA score of 0/1 was achieved by 81.1% receiving risankizumab versus 7.1% receiving placebo |
Rates of treatment-related AEs were similar between risankizumab and placebo group (45.7% and 49%) in part A and remained stable over time | 62 |
Warren et al., 2020 |
Phase III, multicentre, open-label, efficacy assessor-blinded, active-comparator trial IMMerge |
327 |
1)Risankizumab 150 mg at week 0, 4, and every 12 weeks 2)Secukinumab 300 mg at weeks 0, 1, 2, 3, 4, and every 4 weeks |
52 weeks |
Week 16: Risankizumab was noninferior to secukinumab in proportion of patients achieving PASI90 (73.8% versus 65.6%) Week 52: PASI90 Risankizumab was superior to secukinumab (86.6% versus 57.1%, p < 0.001) PASI 100, sPGA 0/1, and PASI75 demonstrated superiority for risankizumab (p < 0.001) |
AEs were reported in 71.3% of patients treated with risankizumab vs. 71.2% with secukinumab. Serious AEs were found in 5.5% and 3.7% with risankizumab and secukinumab, respectively Most common AEs with risankizumab were nasopharynhitis, upper respiratory tract infection, headache, arthralgia, diarrhoea, and bronchitis |
64 |
Papp et al., 2021 |
Phase II, multicenter OLE trial Patients already treated in the 48-week, phase 2, double-blind, active comparator trial were included (Papp et al. 2017) |
110 |
1)Risankizumab 90 mg every 12 weeks for at least 48 weeks If at week 12 < PASI90 was found → Risankizumab 150 mg every 12 weeks |
48 weeks | 74.1% achieved PASI90, whereas 98.1%, 91.7%, 53.7%, and 67.6% achieved PASI50, PASI75, PASI100, and sPGA 0/1, respectively | 77.3% patients reported AEs. The most frequent were nasopharyngitis (17.3%), upper respiratory tract infection (13.6%), and arthralgia (10%) | 71 |
Thaçi et al., 2021 | Phase III, randomized, active-controlled, open-label study | 120 |
1)Risankizumab 150 mg at weeks 0, 4, and 16 2)FAEs 30 QD from week 0 to week 2, then up to 240 mg, TID from week 3 to week 24 if PASI90 was not achieved |
24 |
Week 24: PASI90 achieved by 83.3% of risankizumab group vs. 10% receiving FAEs PASI50 was achieved by 100% of risankizumab vs. 53.3% of FAEs |
Serious AEs were reported by 3.51% of FAEs group and 1.67 of risankizumab group | 65 |
Real world experience | |||||||
Authors, year | Study type | No. of prt | Study design | Study period | Efficacy | Safety | Ref |
Megna et al., 2020 | Single-centre, retrospective study | 8 | Risankizumab at labelled dosage | 16 weeks | Baseline mean PASI and BSA were 11.9 ± 5.5, and 22.9 ± 13.1, respectively. Week 16: 3.3 ± 1.7 and 7.5 ± 5 (p < 0.001 and p < 0.01), respectively. Mean baseline NAPSI reduced from 18.0 ± 8.5 to 7 ± 1.4. Palmo-plantar and scalp area showed a reduction of 67.5% and 99.9% | No AEs were reported | 68 |
Bonifati et al., 2020 | Prospective, real-world study | 12 (9 guselkumab and 3 risankizumab) |
1)Risankizumab at labelled dosage 2)Guselkumab at labelled dosage |
24 weeks |
PASI and PGA decreased significantly through the 24 weeks of treatment Week 12: all sites involved at baseline were free from psoriasis in 6 patients |
No AEs were reported | 73 |
Reddy et al., 2020 | Observational, single-centre, retrospective study | 41 |
1)Risankizumab at labelled dosage after failing guselkumab 2)Risankizumab + apremilast at labelled dosage after failing guselkumab 3)Risankizumab at labelled dosage without prior switch from guselkumab |
Risankizumab after failing guselkumab 21.6 ± 10.4 weeks Risankizumab without guselkumab 18 ± 15.2 weeks |
In the guselkumab failures BSA decreased from 28.5 to 5.9 with a 79.3% average decrease In the group without guselkumab treatment BSA decreased from 49.8 to 7.8 for an 84.3% decrease |
NR | 67 |
Hansel et al., 2020 | Real-life multicenter study | 57 | Risankizumab at labelled dosage | 16 weeks | 49.1% reached PASI100, PASI90 was achieved by 63.2%, and PASI75 by 86% | 1 patient experienced an upper respiratory tract infection | 66 |
Kromer et al., 2020 | Case report | 1, 45-year-old woman | Risankizumab at labelled dosage | 28 weeks | PASI at week 0: 12.8, week 11: 4.8, week 16: 3.8, and week 28:2.2 | NR | 74 |
Ruiz-Villaverde et al. 2020 | Case report | 1, 47-year-old male | Risankizumab at labelled dosage | 56 weeks | Week 8: PASI 0, BSA 0, and sPGA 8 | None | 75 |
Tsuchida et al. 2021 | Case report | 1, 37-year-old man with recurrent colonic diverticulitis | Risankizumab at labelled dosage | 48 weeks | PASI100 after a year of treatment | NR | 69 |
Abbreviations: AEs, adverse events; BCC, basal cell carcinomas; FAEs: fumaric acid esters; PASI, Psoriasis Area Severity Index; prt, participants; QD, once a day; ref, reference; SC, subcutaneous; sPGA, static Physician Global Assessment; TID, three times a day (TID)