Institute for Public Health, Medical Decision Making and Health Technology Assessment 1 Results of the PanEuropean Hepatitis C Project 3 rd Paris Hepatitis.

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Institute for Public Health, Medical Decision Making and Health Technology Assessment 1 Results of the PanEuropean Hepatitis C Project 3 rd Paris Hepatitis Conference January 2009

Institute for Public Health, Medical Decision Making and Health Technology Assessment 2 The Project Funding: In part funded by an unrestricted educational grant from pharmaceutical industry Intention: To have a third party policy institute examine the hepatitis C problem in Europe both from a medical and economic perspective. Geographical focus: 22 countries of the WHO- European region, including 18 EU countries (if possible, all countries of the WHO European region)

Institute for Public Health, Medical Decision Making and Health Technology Assessment 3 Parts and Research Questions of the Project 1.HCV-related burden of disease in Europe  Size of the problem? 2.Market uptake of state-of-the-art antiviral drugs (Peginterferons)  Inequality of health care services? 3.Long-term effectiveness and cost-effectiveness of antiviral therapy  Should we treat? 4.Long-term effectiveness and cost -effectiveness of screening  Should we screen?

Institute for Public Health, Medical Decision Making and Health Technology Assessment 4 Part 1: HCV-related burden of disease in Europe

Institute for Public Health, Medical Decision Making and Health Technology Assessment 5 Objectives To summarise presently available burden of disease data To calculate burden of disease estimates, where HCV specific data are missing. To identify areas, where better data are needed.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 6 Investigated Burden of Disease Indicators Incidence Prevalence Mortality DALYs (Disability adjusted live-years) Liver transplants

Institute for Public Health, Medical Decision Making and Health Technology Assessment 7 Key Findings: Incidence Quantifies new infections  Assessed by national surveillance (notifiable disease) At present, no uniform hepatitis C surveillance exists at the European level, and national surveillance data are not comparable due to differences in surveillance  Reliable incidence data are lacking NOTE: Incidence does not appropriately reflect the size of the hepatitis C problem, because it does not consider the many yet undetected infections contracted in the past.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 8 Key Findings: Prevalence Quantifies disease frequency in pop.  Key measure to quantify the size of the hepatitis C problem. Most complete HCV prevalence data for Europe are available from WHO. However, it is widely accepted that these are unreliable and need to be updated. Estimates communicated by national authorities tend to be higher but are less frequently available. Based on available data, 1.1–1.3% of the population in our 22 focus countries are infected (7.3–8.8 million). In the EU, based on conservative WHO data, 0.7% (3.5 million) are infected.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 9 Prevalence (WHO 1999) Source: WHO 1999 Data extracted from published studies and/or submitted to WHO by countries/areas

Institute for Public Health, Medical Decision Making and Health Technology Assessment 10 Key Findings: Mortality Main causes of death associated with HCV infection are end-stage liver cirrhosis and liver cancer. However, HCV-specific mortality data for these conditions are lacking. Therefore, HCV-related mortality was estimated from data of the WHO Global Burden of Disease study (GBD) via HCV attributable fractions. HCV-related deaths per year: WHO Europ. Reg.: 86,000 (HIV/AIDS ~ 40,000) EU: 55,000 (HIV/AIDS ~ 7,000)

Institute for Public Health, Medical Decision Making and Health Technology Assessment 11 Key Findings: DALYs Quantify years of ‘healthy’ life lost (Years of life lost from premature death + years of healthy life lost due to disability) DALYs for HCV-related cirrhosis and liver cancer are lacking.  Calculation from data of the WHO Global Burden of Disease study (GBD) via HCV attributable fractions. HCV-related DALYs lost per year: WHO Europ. Reg.: 1.2 million (HIV/AIDS ~ 1.4 million) EU: 0.6 million (HIV/AIDS ~ 0.3 million) 95% of the DALYs are accumulated by patients in advanced disease stages (cirrhosis or liver cancer).

Institute for Public Health, Medical Decision Making and Health Technology Assessment 12 Key Findings: Liver Transplant Europe-wide HCV-specific transplant data are lacking  Calculation from various data sources via HCV attributable fractions. HCV accounts for about 1/4 of the liver transplants in Europe, and therewith is a major cause for the already existent shortage of donor organs. Strong variation of HCV-related transplantation rates across Europe. (Range 0.002/ in Bulgaria to 0.563/ in Spain)

Institute for Public Health, Medical Decision Making and Health Technology Assessment 13 Conclusions Part 1 Hepatitis C is a major public health problem in the WHO European region, costing twice as many lives and about as many ‘healthy’ live years as HIV/AIDS. Burden of disease caused by advanced disease highlights the potential benefit of antiviral treatment. Varying transplantation and mortality rates suggest inequality of health care services across Europe. Most importantly, the lack of data indicates that hepatitis C still is a neglected disease. What is needed are PUBLIC AWARENESS, coordinated action plans, more and better data.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 14 Part 2: Market uptake of state-of-the-art antiviral drugs (Peginterferons)

Institute for Public Health, Medical Decision Making and Health Technology Assessment 15 Objectives To assess the market uptake of peginterferons in 21 countries of the WHO European region up to To convert sales data into numbers of patients treated and to compare prevalence-adjusted peginterferon treatment rates across countries. To find out whether there is unequal access to optimised therapy.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 16 Prevalence-adjusted Cumulative PegINF Treatment Rates Source: Calculated from IMS Health data and HCV prevalence rates derived from national sources

Institute for Public Health, Medical Decision Making and Health Technology Assessment 17 Conclusions Part 2 Peginterferon market uptake and treatment rates differed considerably across countries. Results indicate unequal access to optimised therapy across Europe. Reasons for unequal access are budget restrictions, and differences in screening and treatment policies.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 18 Part 3: Long-term effectiveness and cost-effectiveness of antiviral therapy

Institute for Public Health, Medical Decision Making and Health Technology Assessment 19 Objectives To systematically review the long-term effectiveness and cost-effectiveness of antiviral treatment (AVT) in patients with chronic hepatitis C. Emphasis was placed on the comparison of peginterferon/ribavirin treatment with interferon/ribavirin treatment, which was the previous standard of care.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 20 Key Findings: CE of AVT 21 studies comparing peginterferon/ribavirin versus interferon/ribavirin treatment were reviewed (16 in treatment-naïve patients, 5 in other patient groups). In treatment-naïve patients peginterferon/ribavirin therapy gained life years or quality- adjusted life years (QALYs). Costs per QALY gained ranged from <0 to 84,700 EUR/QALY (discounted). Results varied with length of treatment, genotype, liver histology, population characteristics and discount rate.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 21 Conclusions Part 3 Our review proves that peginterferon/ribavirin therapy of treatment-naïve patients with chronic hepatitis C without doubt is cost-effective (i.e. gains additional life- years and quality of life at acceptable cost). Evidence is only weak for special patient groups (e.g., co-infection with HIV or HBV, haemophilia, intravenous drug users, mild hepatitis, persistently normal ALT levels)

Institute for Public Health, Medical Decision Making and Health Technology Assessment 22 Part 4: Long-term effectiveness and cost-effectiveness of screening

Institute for Public Health, Medical Decision Making and Health Technology Assessment 23 Objectives To systematically review the long-term effectiveness and cost-effectiveness of screening for hepatitis C. Emphasis was placed on the influence of HCV- prevalence on the cost-effectiveness of screening.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 24 Key Findings: CE of Screening 10 studies evaluating the cost-effectiveness of hepatitis C screening were reviewed. Studies varied regarding target population, HCV prevalence, study perspective, discount rate, mode of screening and antiviral treatment. Compared to no screening and standard care, HCV screening and early treatment gained life years ( days) or QALYs. Costs per QALY gained ranged from 18,300 to 1,151,000 EUR/QALY (if screening was not domimated) For target groups with HCV prevalence >10% most studies reported ICER/ICUR < EUR. With lower prevalence, costs per QALY gained were much higher.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 25 ICER of Screening by Prevalence ICER: incremental cost-effectiveness ratio, HCV: hepatitis C virus, IFN: interferon, RBV: ribavirin, PegIFN: peginterferon.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 26 ICUR of Screening by Prevalence ICER: incremental cost-utility ratio, HCV: hepatitis C virus, IFN: interferon, RBV: ribavirin, PegIFN: peginterferon. §One point out of range: 1, Euro/QALY with 1% HCV prevalence, PegIFN+RBV.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 27 ICER of Screening by Prevalence ICER: incremental cost-effectiveness ratio, HCV: hepatitis C virus Screening with PegINF+RBV Treatment

Institute for Public Health, Medical Decision Making and Health Technology Assessment 28 ICUR of Screening by Prevalence ICER: incremental cost-effectiveness ratio, HCV: hepatitis C virus Screening with PegINF+RBV Treatment

Institute for Public Health, Medical Decision Making and Health Technology Assessment 29 Conclusions Part 4 HCV screening should focus on populations with elevated HCV prevalence in order to be cost-effective. High prevalence target groups could be selected based on risk factor profiles (e.g., history of blood transfusion, elevated ALT, IVDU, age, visit in hepatology wards) However, cost-effectiveness may not be the only decision criterion for the implementation of HCV screening. In view of the multitude of iatrogenic infections, aspects like fairness might be considered as well. Currently, many European countries plan to introduce national screening programs, but the question is whom to screen and how to screen.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 30 Hepatitis C Research Team Nikolai Mühlberger, D.V.M, M.P.H. 1 Gaby Sroczynski, M.P.H. 1 Beate Lettmeier 1 Ruth Schwarzer, M.A., M.P.H. 1 Eva Esteban M.P.H. 1 Annette Conrads-Frank, Ph.D. 3 Stefan Zeuzem, M.D. 2 Uwe Siebert, M.D., M.P.H., M.Sc., Sc.D. 1,3 1 Dept. of Public Health, Medical Decision Making and HTA, UMIT - University for Health Sciences, Medical Informatics and Technology 2 Department of Internal Medicine, Gastroenterology, Hepatology, Pneumology and Endocrinology, Johann Wolfgang Goethe-University, Frankfurt a.M. Germany 3 Institute for Technology Assessment, Massachusetts General Hospital, Harvard Medical School, Boston, MA, USA

Institute for Public Health, Medical Decision Making and Health Technology Assessment 31 Publications 1.Mühlberger N, Schwarzer R, Lettmeier B, Sroczynski G, Zeuzem S, Siebert U. HCV-related burden of disease in Europe: a systematic assessment of incidence, prevalence, morbidity, and mortality. BMC Public Health (in press) 2.Lettmeier B, Mühlberger N, Schwarzer R, Sroczynski G, Wright D, Zeuzem S, Siebert U. Market Uptake of New Antiviral Drugs for the Treatment of Hepatitis C. Journal of Hepatology 2008;49: Sroczynski G, Esteban E, Conrads-Frank A, Schwarzer R, Mühlberger N, Wright D, Zeuzem S, Siebert U. Long-term Effectiveness and Cost-Effectiveness of Screening for Hepatitis C Virus Infection. European Journal of Public Health (accepted for publication)

Institute for Public Health, Medical Decision Making and Health Technology Assessment 32 Appendix

Institute for Public Health, Medical Decision Making and Health Technology Assessment 33 Recommendations for better data I Surveillance: For outbreak detection, monitor new cases of acute Hep C, which most appropriately reflect changes in infection rates. For disease monitoring, also include newly detected cases of chronic Hep C and stratify Assess transmission routes and GTs (international differences) Prevalence: Provide representative country-, age- and genotype-specific data In addition, prevalence studies should assess the number of yet undetected cases and how many of those would be detected to late for AVT without screening Help to identify target groups for cost-effective screening

Institute for Public Health, Medical Decision Making and Health Technology Assessment 34 Recommendations for better data II Mortality: Specifically assess HCV-related mortality on death certificates and mortality statistics (including deaths due to HCV-related cirrhoses and liver cancer)  Benefit is questionable DALYs: Most complex BoD measure aiming at global between country comparison. Estimation requires consistent methodology and input data  Should remain a task of WHO Liver transplants: Reliable HCV-related transplant data could easily be generated by collecting little additional HCV-specific information  Task should be adopted by the Transplant Committee of the Council of Europe or the European Liver Transplant Registry.

Institute for Public Health, Medical Decision Making and Health Technology Assessment 35 Recommended Strategies Source: Esteban et al. Journal of Hepatology 48 (2008) 148–162

Institute for Public Health, Medical Decision Making and Health Technology Assessment 36 HCV-Genotype Distribution Source: Esteban et al. Journal of Hepatology 48 (2008) 148–162 GT 1a, 3a and 4  related to IDU GT 1b and 2  related to blood transfusion and unsafe medical procedures