3 Committee discussion

The appraisal committee considered evidence submitted by AbbVie, a review of this submission by the evidence review group (ERG), and responses from stakeholders. See the committee papers for full details of the evidence.

Decision problem

The company's decision problem is relevant to clinical practice

3.1 Risankizumab is licensed for treating active psoriatic arthritis in adults who have had an inadequate response or who have been intolerant to 1 or more disease-modifying antirheumatic drugs (DMARDs). The company's decision problem was narrower than risankizumab's marketing authorisation. It positioned risankizumab for people who also have moderate to severe psoriasis and have previously had 2 conventional and at least 1 biological DMARD. The proposed population was consistent with NICE's technology appraisal guidance on guselkumab. Risankizumab and guselkumab are both IL‑23 modulators. The company presented a comparison with guselkumab, which the committee considered was consistent with the criteria for a cost-comparison appraisal (see section 3.6). The committee noted that NICE has recommended many treatments other than guselkumab for psoriatic arthritis. But, because guselkumab is the only treatment recommended for this specific subgroup it is an appropriate comparator for a cost-comparison appraisal. The committee concluded that the company's decision problem was relevant to clinical practice.

Clinical effectiveness

Risankizumab is more effective than placebo

3.2 Risankizumab has been studied in 3 randomised controlled trials including a total of 1,592 adults with active psoriatic arthritis. These trials compared risankizumab with placebo. The KEEPsAKE 2 trial (n=443) is the focus of the company's evidence submission because 46.5% of participants had previously had a biological DMARD. In the KEEPsAKE 2 trial, risankizumab showed statistically significant improvements in primary and secondary endpoints compared with placebo: a higher proportion had an American College of Rheumatology (ACR) 20 response at 16 weeks and 24 weeks, and a higher proportion had a Psoriasis Area and Severity Index (PASI) 90 response at 24 weeks. The committee concluded that risankizumab was more effective than placebo.

The company's network meta-analyses are suitable for decision making

3.3 The company did a series of network meta-analyses (NMAs) on PASI response rates, ACR response rates and safety outcomes. These compared risankizumab with guselkumab. The ERG was satisfied with the search strategy, the methodological quality of the included trials and the methodology used for the NMAs. The committee accepted the ERG's view, concluding that the NMAs provided by the company were suitable for decision making.

Risankizumab provides similar ACR and PASI response rates to guselkumab

3.4 The NMAs showed no significant differences between risankizumab and guselkumab for any of the ACR (20, 50, 70) and PASI (50, 75, 90, 100) outcomes. Also, there were no significant differences in adverse events rates. The ERG advised that the lack of significant differences does not imply clinical equivalence and that the wide confidence intervals around the point estimates suggest uncertainty. The committee noted this uncertainty. But, it agreed that their effectiveness is likely to be comparable. This is because the point estimates were close to 1 (or 0) for the main efficacy outcomes at 24 weeks and the drugs have the same mechanism of action.

The trial results are generalisable to the population in the company's decision problem

3.5 The ERG highlighted several limitations with the NMA. The company positioned risankizumab for also treating moderate to severe psoriasis in people who have had 2 conventional DMARDs and at least 1 biological DMARD. A pre-specified subgroup of the trial had all previously had a biological DMARD. However, in this subgroup only 51.0% had also had 2 conventional DMARDs. In addition, only a small proportion of the previous biological DMARD subgroup had moderate to severe psoriasis (the exact figures are considered confidential by the company and cannot be reported here). However, the committee recalled that when appraising guselkumab it had accepted the assumption that efficacy specific to people who had a biological DMARD was generalisable to that of people who also had 2 conventional DMARDS. Also, that modelling was appropriate regardless of disease severity. The committee agreed that the trial results were generalisable to the population in the company's decision problem.

Cost comparison

It is appropriate to assess response to risankizumab at 16 weeks

3.6 NICE's technology appraisal guidance on guselkumab recommends that response to treatment should be assessed from 16 weeks and stopped at 24 weeks if there is an inadequate Psoriatic Arthritis Response Criteria (PsARC) response. The summary of product characteristics for guselkumab specifies considering stopping treatment if no response is shown at 24 weeks. In its base case, the company modelled assessing PsARC response at 24 weeks for both treatments, aligned with the recommendation for guselkumab. However, the summary of product characteristics for risankizumab states that 'consideration should be given to discontinuing treatment in patients who have shown no response after 16 weeks of treatment'. The company also submitted a scenario modelling response assessment at 16 weeks. The committee recalled that there was strong clinical support in the appraisal of guselkumab for assessing response at 16 weeks. Also, that this is more aligned with clinical practice of using other biologic therapies for this condition. The committee considered it was appropriate to assess response to risankizumab at 16 weeks, in line with the summary of product characteristics.

The total costs associated with risankizumab are similar to or lower than those associated with guselkumab

3.7 The company presented a cost-comparison analysis that modelled the total costs of risankizumab and guselkumab over 5 years. The base case assumes that the only difference between the 2 treatment options arises from costs associated with drug acquisition. Additional scenario analyses explored the impact of variable drug administration and monitoring costs. It also assumed clinical equivalence between the 2 treatment options, based on evidence from the NMA outlined in section 3.3. The base case assumed treatment response was assessed at 24 weeks and applied a 16.5% annual probability of discontinuing treatment after initial assessment of response, for both risankizumab and guselkumab. This was in line with the modelling for the guselkumab appraisal for this indication. A scenario explored the impact of assessing response at 16 weeks. Taking into account the patient access scheme discounts, the total costs associated with risankizumab were similar to or lower than those associated with guselkumab. This was whether response was assessed at 16 weeks or 24 weeks (the exact results cannot be reported here because the discounts are confidential).

Clinicians should take into account factors that may affect PsARC and PASI and make any clinical adjustments needed

3.9 The committee noted that some people may have physical, sensory or learning disabilities or communication difficulties that could affect their responses to components of the PsARC. It concluded that this should be taken into account when using the PsARC. The committee was also aware that the PASI might underestimate disease severity in people with darker skin. The committee concluded that, when using the PASI, healthcare professionals should take into account skin colour and how this could affect the PASI score, and make the clinical adjustments they consider appropriate.

  • National Institute for Health and Care Excellence (NICE)