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Is an Orphan Drug’s Cost-Effectiveness Associated with US Health Plan Coverage Restrictiveness?

Author

Listed:
  • James D. Chambers

    (Tufts Medical Center)

  • Nikoletta M. Margaretos

    (Tufts Medical Center)

  • Daniel E. Enright

    (Tufts Medical Center)

  • Rosa Wang

    (Daiichi Sankyo, Inc.)

  • Xin Ye

    (Daiichi Sankyo, Inc.)

Abstract

Background and Objectives Orphan drugs’ high prices raise questions about whether their costs are worth their benefits. We examined the association between an orphan drug’s cost-effectiveness and health plan coverage restrictiveness. Methods We analyzed a dataset of US commercial health plan coverage decisions (information current as of 2019) for orphan drugs (n = 3298). We used multi-level random-effect logistic regression to examine the association between orphan drug cost-effectiveness and coverage restrictiveness. We identified cost-effectiveness estimates from the Tufts Medical Center Cost-Effectiveness Analysis Registry, and from the Institute for Clinical and Economic Review’s value assessments. We included only cost-effectiveness studies not funded by product manufacturers. We included the following independent variables: cancer indication, availability of alternatives, pediatric population, number of years since US Food and Drug Administration (FDA) approval, disease prevalence, annual cost, additional non-orphan indication, safety, and inclusion in a FDA expedited review program. Results Plans restricted drug coverage in 29.7% (n = 981) of decisions. Plans were more likely to restrict drugs with incremental cost-effectiveness ratios of $50,000–$175,000 per quality-adjusted life-year [QALY] (odds ratio = 1.855, p $500,000 per QALY/dominated (odds ratio = 2.032, p

Suggested Citation

  • James D. Chambers & Nikoletta M. Margaretos & Daniel E. Enright & Rosa Wang & Xin Ye, 2022. "Is an Orphan Drug’s Cost-Effectiveness Associated with US Health Plan Coverage Restrictiveness?," PharmacoEconomics, Springer, vol. 40(2), pages 225-232, February.
  • Handle: RePEc:spr:pharme:v:40:y:2022:i:2:d:10.1007_s40273-021-01096-5
    DOI: 10.1007/s40273-021-01096-5
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