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Omalizumab for the Treatment of Severe Persistent Allergic Asthma in Children Aged 6–11 Years

A NICE Single Technology Appraisal

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Abstract

Following a licence extension to include those aged 6–11 years, the National Institute for Health and Clinical Excellence (NICE) invited the manufacturer of omalizumab (Novartis Pharmaceuticals UK) to submit evidence for the clinical and cost effectiveness of this drug for patients with severe persistent allergic asthma in this age bracket. NICE had previously considered the use of omalizumab in patients aged 12 years and over. The Centre for Reviews and Dissemination (CRD) and the Centre for Health Economics (CHE) at the University of York were commissioned as the Evidence Review Group (ERG) to critically appraise the evidence presented by the manufacturer. This article summarizes that review of the evidence, the deliberations of the NICE Appraisal Committee and the resulting NICE guidance.

The ERG critically reviewed the evidence presented in the manufacturer’s submission and identified areas requiring clarification, for which the manufacturer provided additional evidence. The relevant patient population was patients aged 6–11 years of age with severe persistent allergic immunoglobulin E-mediated asthma whose condition remained uncontrolled despite best standard care with high-dose inhaled corticosteroids and a long-acting inhaled β2-agonist. The main clinical effectiveness data were derived from a pre-planned subgroup analysis of a single randomized controlled trial comparing omalizumab plus standard therapy against standard therapy alone. At a 52-week follow-up, the only outcome to show a statistically significant benefit of omalizumab compared with placebo was the number of exacerbations defined as ‘clinically significant’ [CS] (relative risk [RR] 0.504; 95% CI 0.350, 0.725; p<0.001). At the ERG’s request, the manufacturer provided analyses stratified by baseline exacerbation rate, which indicated the effect of omalizumab on CS exacerbations was statistically significant only for those children with ≥3 exacerbations as baseline. The ERG identified a number of issues relating to the clinical effectiveness results: it was unclear whether the pre-planned subgroup analysis had sufficient power; the definition of CS exacerbation was less severe than that used in UK clinical practice; and the method for imputing exacerbations for those who withdrew from treatment may have underestimated the exacerbation rate.

The incremental cost-effectiveness ratio based on the manufacturer’s results was considerably above the threshold range stated in the NICE Guide to the Methods of Technology Appraisal. The ERG identified numerous issues relating to the cost-effectiveness results, which included the following: the 10-year time horizon for treatment may exceed that in clinical practice; the assumption of constant exacerbation rates over a lifetime given that adolescence is expected to impact on the severity of asthma; and whether it is appropriate to use health-related quality-of-life data collected in adults for children.

The ERG concluded that omalizumab appears to reduce CS exacerbations but there was no evidence of improvement in daily symptoms, CS severe (CSS) exacerbations or hospitalization rates. The main driver of cost effectiveness was the reduction in asthma-related mortality associated with a reduction in CSS exacerbations. As the number of CSS exacerbations avoided was low, as is asthma-related mortality in children, the potential small gain in QALYs associated with omalizumab was not sufficient to compensate for the high treatment cost even under the most favourable scenario analyses. The Appraisal Committee recommended that omalizumab should not be routinely provided for the treatment of severe persistent allergic asthma in children aged 6–11 years.

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Acknowledgements

This project was funded by the National Institute for Health Research (NIHR) Health Technology Assessment Programme (project number 09/98/01) and will be published as part of a compendium of ERG articles in Health Technology Assessment. See the HTA programme website (http://www.hta.ac.uk) for further project information. This summary of the ERG report was compiled after the Appraisal Committee’s review and incorporates additional information and comment from the authors on the STA process and iterations of the NICE guidance not covered by the HTA report. This summary has not been externally peer reviewed by PharmacoEconomics.

The views and opinions expressed herein are those of the authors and do not necessarily reflect those of NICE or the Department of Health. The authors have no conflicts of interest that are directly relevant to the content of this summary. They would like to thank Jonathan Minton for his assistance during the production of the ERG report.

This work is Crown copyright (UK).

Author contributions:

Jane Burch: Researcher responsible for reviewing the clinical evidence submitted, and the writing of the manuscript.

Susan Griffin: Researcher responsible for reviewing the cost-effectiveness evidence submitted and provided comments on drafts of the manuscript.

Claire McKenna: Contributed to the review of cost-effectiveness evidence and provided comments on drafts of the manuscript.

Simon Walker: Contributed to the review of cost-effectiveness evidence and provided comments on drafts of the manuscript.

James Paton: Provided clinical advice throughout the project and comments on drafts of the manuscript.

Kath Wright: Reviewed the search strategies, conducted additional searches, and provided comments on drafts of the manuscript.

Nerys Woolacott: Took overall managerial responsibility for the project, contributed to all aspects of the review of the evidence submitted, and provided comments on drafts of the manuscript.

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Authors and Affiliations

  1. Centre for Reviews and Dissemination (CRD), University of York, Heslington, York, YO10 5DD, UK

    Jane Burch, Kath Wright & Nerys Woolacott

  2. Centre for Health Economics (CHE), University of York, York, UK

    Susan Griffin, Claire McKenna & Simon Walker

  3. Royal Hospital for Sick Children, Glasgow, UK

    James Paton

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  1. Jane Burch
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Correspondence to Jane Burch.

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Burch, J., Griffin, S., McKenna, C. et al. Omalizumab for the Treatment of Severe Persistent Allergic Asthma in Children Aged 6–11 Years. PharmacoEconomics 30, 991–1004 (2012). https://doi.org/10.2165/11597160-000000000-00000

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