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Benefit-Transfer: Practice and Prospects Workshop 22 November 2007

Benefit-Transfer: Practice and Prospects Workshop 22 November 2007 Applications of Benefit–Transfer in Health Kees van Gool Centre for Health Economics Research and Evaluation University of Technology Sydney. Outline. Setting the scene Economic evaluation and health care policy

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Benefit-Transfer: Practice and Prospects Workshop 22 November 2007

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  1. Benefit-Transfer: Practice and Prospects Workshop 22 November 2007 Applications of Benefit–Transfer in Health Kees van Gool Centre for Health Economics Research and Evaluation University of Technology Sydney

  2. Outline • Setting the scene • Economic evaluation and health care policy • Economic evaluation and benefit transfer in health • Examples: • Screening for cystic fibrosis • Health impact of noise • Cancer treatment protocols • Conclusions

  3. Setting the scene

  4. Economic evidence and health care policy • Evidence of use at a central level, e.g. • PBAC/MSAC in Australia • NICE in the UK • CDR in Canada • Very limited evidence of use at a local level (e.g. public hospitals)

  5. Central level use of economic evidence • Pharmaceutical Benefits Scheme (PBS): • Australia’s most famous example of economic evaluation use • Used to make decisions about which (new) drugs to list on the PBS and receive public subsidies. • Mandatory use of economic evidence since 1993 (world first) • Formal nexus between decision-making and economic evidence • Pharmaceutical Benefits Advisory Committee (PBAC) recommendation binds the Minister for Health: • Minister cannot list drugs that have been rejected by PBAC • Minister can reject drugs that have been recommended by PBAC

  6. Central level use of economic evidence • Applicants (drug companies) conduct economic evaluation based on guidelines published by PBAC • Focus on “how much it would cost to achieve additional health outcomes with the new therapy compared with the existing therapy that would be replaced” • Australian context • Use of randomised clinical control trial data, but: • Lack of resource data (estimation) • Insufficient duration (extrapolation) • Trial population differ from real population (application) • Non-patient-relevant outcomes of treatment (transformation) • Translation (akin to benefit-transfer)

  7. Central level use of economic evidence • Independent consultants check modeling • Department of Health re-checks • In 2006, PBAC made 187 decisions (137 positive recommendations) • PBAC administrative costs around $11m • $60,000 per decision • PBAC economic evidence not publicly available due to commercial-in-confidence

  8. Local level use of economic evidence • Hospitals and local health regions make many resource allocation decisions • Very little use of economic evidence at this level • Lack health economics expertise/resources at local level • Perception of bias in studies • Lack of relevance to local setting • Budget rigidities • Is the published economic evidence useful for decision makers?

  9. Some examples of current workExample IScreening for Cystic Fibrosis

  10. Economic evaluation of cystic fibrosis screening program • Cystic Fibrosis (CF) is one of the most common serious genetic disease in Caucasians • Incidence of 1 in 2500 and carrier frequency of 1 in 25. • In Australia, over 70 babies with CF are born mostly to parents with no known family history • No organized community based prenatal testing programs • Calls for community screening of CF carriers • Population screening strategies: • Preconception (before pregnancy) • Prenatal (during early pregnancy) • Neonatal (new born)

  11. Aims • Analyse the cost-effectiveness of a community-based cystic fibrosis (CF) carrier screening program • the cost of CF carrier screening per CF birth averted. • Use decision analysis techniques • Attempted to look at literature • Economic evidence • Transferability of existing evidences

  12. Results - Economic Evidence • 29 economic studies were included • North America (12), Europe(15), Asia/ Australia (2) • Only 14 studies focussed on preconceptional/ prenatal screening • Wide ranging Incremental Cost Effectiveness Ratio(ICER) • Cost per carrier couple detected ranged from US$33,504 to US$295,121 • Inconsistent net savings results (cost CF care minus cost of CF screening) • Literature offers decision makers with limited information and great uncertainty • How can we make better use of this evidence?

  13. Deconstructing the model (1)

  14. Deconstructing the model (2) • Set inputs • Carrier incidence (1/25 amongst Caucasians) • Carrier couple incidence (1/625 amongst Caucasians) • Foetus CF status (1/4 amongst CF+ carrier couples) • Behavioural inputs • Screening participation: • Preconception - 10% to 100% • Prenatal - 50% to 100% • 15 -25% refrained from having children (preconception) • 75-100% make use of prenatal diagnosis • 80- 95% therapeutic termination rates • Decisions like in vitro fertilization ignored • Therapeutic termination range from 30 – 100%

  15. Deconstructing the model (3) • Cost inputs • Pre-screening stage • Mass communication - US$35k (in school screening) to between US$297k - $562k (general population) • Screening stage • Cost of per test – US$28 to US$240 • Post-test stage • Counselling cost/carrier couple (US$17.2 to US$1188),CF foetal diagnosis(US$249 to US$2120),termination - US$206 to US$3486 and replacement (US$4,696) • Lifetime cost of care of CF patients • Range from US$329k to US$1.3m • Estimated in several ways (specific to age, severity & symptoms) and included different cost items (e.g. non-hospital costs)

  16. Deconstructing the model (3) • Identify fixed inputs • Identify behavioural inputs • Assess the likelihood of variation with local setting • Where necessary substitute using • Existing local evidence • New evidence where none exist • Use local cost data from existing sources and standard methods

  17. Example IIState of the art on the economics valuation of noiseproject undertaken for the Department of Environment and Climate Change NSW

  18. Project aims • Identify and assess methods for measuring the economic impact of noise pollution • Appraise the potential for these methods for measuring noise in NSW • Assess the applicability of empirical results of noise pollution to the NSW context • Here we focus on health

  19. Project framework • The nature of noise pollution • Multiple sources and impacts • Context specific • Some evidence uncertain, others clear • Some impacts well-known, others unknown • Multiple valuation techniques • Revealed preferences • Stated preferences • Physical linkages • Preferred for the purposes of measuring health impact

  20. Model deconstruction

  21. Empirical results: health costs • Total health impact is a function of: • noise level • noise distribution • prevalence of disease • attributable fraction • cost of disease • Health impact • Life years lost • WTP to avoid disease • Health care costs (cost of treatment/management) • Productivity costs (e.g. cost of days absent)

  22. Exposure functions • Noise can have an impact on: • Physiological responses including stress and annoyance • Sleep disturbance • Hearing loss • Mental health • Child health • Cardiovascular disease • Performance and learning in children

  23. Noise exposure functions • State of the evidence • Good evidence on ‘annoyance’, ‘sleep disturbance’ and ‘hearing loss’. • Some evidence on cardiovascular disease and child learning and performance • Little or no evidence on serious mental health and child health • Future prospects of better and more conclusive evidence of relationships

  24. Measuring the impact • Staatsen et al (2004) estimated the monetary values for each health impact associated with noise as the sum of: • WTP to avoid each type of episode of ill health. • health care costs of treatment when relevant; and • productivity loss.

  25. Empirical results: health costs Source: Staatsen et al (2004)

  26. Example IIIEconomic evaluation of Standard Cancer Treatment ProtocolsUNSW and UTSNHMRC Health Services Research Grant

  27. Cancer-related pharmaceutical spending in public hospitals • $127m through Section 100 – highly specialised drugs • $124m on drugs related to cancer separations • 52% related to chemotherapy • Average pharmaceutical cost per chemo separation: • 1996/97 = $165 • 2004/05 = $479

  28. The challenge in public hospitals • Capped budget; limited resources • Maximise health • Very little information • Very little effective coordination within/between hospitals • Community and provider expectations • Teaching hospitals need to be at the cutting edge • Clinical trials and Special Access Scheme

  29. The challenge for public hospitals (and PHI) • Many new drugs • Far more costly • Far more complex • Adoption decision • Cost-effective diffusion • Introduced into a dysfunctional decision-making system • Possible strategic behaviour by pharmaceutical companies •  CI-SCAT

  30. Cancer Institute– Standard Cancer Treatment protocols (NSW) • Online resource that lists over 450 protocols • Information on target patient group, how to administer the chemo drug, summary of evidence, dose calculation and side effects. • Developed by multidisciplinary reference groups www.cancerinstitute.org.au • But no economic evidence

  31. Aims of the project • Aim 1: Developing economic evidence for CI-SCaT clinical guidelines • similar to those produced for PBS funding • to present models that illustrate the costs and consequences of implementing cancer treatment guidelines • using existing data on cancer treatment pathways, as well as resource costs, to construct an economic “base case” against which new interventions can be compared.

  32. Aims of the project • Aim 2: Developing economic evidence applicable to local settings • work with local decision makers to adapt the decision analytic models to the particular context of their locality. • use local data to populate key model parameters • Models to set out the conditions necessary to ensure that a new treatment remains cost-effective in practice. • estimate the economic impact if prescribing patterns go beyond the intended patient groups, • if treatment is not halted once certain clinical indicators have been reached. • Aim 3: Have aims 1 and 2 had an impact?

  33. The challenge • 455 protocols (and counting); • Small budget, few health economists and five years. • Economic evidence to be • High quality • Timely • Relevant to local setting • Easily interpreted

  34. The approach • The decision context: • what type of chemotherapy to give • what additional (health) benefits can we expect at what additional cost? • Outcome: • survival but can also include quality of life • evidence from trials • Resource use: • Cost of the drug -  • Cost of administering – broad categories • Cost of managing side effects – general econometric model

  35. The approach • Model to be available on web • Updated as new evidence is released • Estimates of additional resources (e.g. number of chairs, nursing time) • Estimate of cost burden (e.g. federal government, PHI, public hospital) • Local users can adapt model to take into account: • Local population parameters • Local unit costs (e.g. wages) • Comparator • Alternative scenarios

  36. Conclusions • Health economists place too much emphasis on the results rather than the mechanics of the model. • Deconstruction would be useful – with more emphasis on making general models available. • CI-SCAT project aims to produce economic evidence that is: • Relevant and adaptable • High quality • Widely disseminated • Timely and regularly updated • Produced efficiently • Will availability of economic evidence have an impact on decision-making?

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