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Speaker Invited Issue Panel Session New AntiAnti-Cancer Drugs Reimbursement Issues in Cancer Drugs: Do We Have To Pay For All Cancer Drugs? Are they as Valuable as we Think? Are they a Special Case? Kenneth R. Paterson MBChB, MBChB, FRCP, FFPM Prof Ken Paterson ISPOR - Prague Chair, Scottish Medicines Consortium Consultant Physician, Glasgow Royal Infirmary Glasgow, UK New AntiAnti-Cancer Medicines ► Considerable pent pent--up demand Patients Clinicians ► Much media interest “miracle drugs”, “life “life--saving treatment” ► Often political interest …especially if threat not to make drug available ► Legitimate interest from pharma Does some ‘Hype’ Matter? ► May raise false hopes ► Often fails to represent the downside of treatment ► May M distort di t t priority i it setting tti in i healthhealth h lth-care Use of ineffective therapy Failure to adopt new, effective therapy ► Subverts true evidenceevidence-based practice Keen to sell drug and boost share price/profile ► How good are new antianti-cancer drugs? Scottish Medicines Consortium ► Rapid health technology assessment of all new drugs – established 2002 Unique position in world newnew-drug HTA ► Manufacturer makes the case for use – Clinical effectiveness Cost Cost--effectiveness ► Cost Cost--utility analysis (cost per QALY) the preferred approach ► Analysis of QALYs only (not cost) Why QALYs? ► Can (should) capture all the benefits and adverse effects of the medicine in question Survival gain (or loss) Improvement p in quality q y of life from treatment Reduction in quality of life from adverse events Impact on quality of life of treatment protocol Appropriate modelling very sensitiven to change ► Allows comparison across (and within) disease areas 1 SMC and AntiAnti-Cancer Medicines ► 87 cancer medicines reviewed 38 for advanced/metastatic cancer 49 for earlier/adjuvant treatment ► Median M di QALY gain i (over ( currentt treatment) t t t) 0.26 for advanced cancer 0.37 for earlier/adjuvant treatment ► Mean QALY gain (over current treatment) 0.51 for both groups What does this Mean? ► Median ► Mean of the greatest healthhealth-gains are with really innovative drugs – Trastuzumab – 2.4 QALYs Nilotinib – 2.1 2 1 QALYs Lenalidomide – 1.8 QALYs ► Even if these are expensive, they offer good ‘value-for ‘valuefor--money’ ► Only ► 22 8 drugs (9%) offered ≥1 QALY drugs (25%) offered ≤0.2 QALY = 3 months at 70% of normal QoL Note NICE ‘end ‘end--ofof-life’ decision decision--making Is There No Good News – 2? ► Anti Anti--cancer offer no health gain (=me too!) 28% offer >0 – 0.1 QALY 25% offer >0 >0.1 1 – 0.5 0 5 QALY 13% offer >0.5 – 1.0 QALY 12% offer >1 QALY Median health gain (n = c. 300) = 0.1 QALY!! drugs are much like other drugs Musculoskeletal (11) – 0.66 QALY Infections (33) – 0.11 QALY Endocrine (24) – 0.07 0 07 QALY Cardiovascular (33) – 0.05 QALY CNS and pain (55) – 0.04 QALY ► New drugs in general are not as valuable as many would like to think! How Good are New Drugs? ► 22% health gain 8-9 months th with ith QoL Q L 70% Is There No Good NewsNews- 1? ► Some health gain 6 months with quality of life 70% of normal Caveats and Criticisms ► Health gain is as presented by pharma May overover-estimate true gain by a factor of 2!! SMC did not always accept the QALY given ► QALY may nott adequately d t l capture t b benefits fit Responder v nonnon-responder Problems with QoL assessment ► Clinical trial ≠ clinical practice ?possible to maximise benefit & minimise S/E 2 Special Cancer Issues - 1 ► Often scanty phase 3 clinical data regimens with polypoly-pharmacy make comparators hard to define ► Complex RCTs RCT often ft use comparators t diff differentt ffrom current Scottish practice May require indirect comparison ► Survival benefits often unclear Overall v ‘progression‘progression-free’ survival Extrapolation not clearclear-cut Conclusions medicines are rarely as valuable as they might like to appear ► Health Health--gain from many new cancer medicines is modest Special Cancer Issues - 2 ► Quality of life assessment difficult Impact of adverse events a problem ? revaluation of QoL near life’s end ? special benefit with low expectancy ► Increased niching by indication …more (ultra(ultra-)orphan drugs ►…with ► Rule expectations of “special case” of Rescue - a rule?? Scottish Medicines Consortium ► New www.scottishmedicines.org.uk …and often overover-stated in media etc ► Some innovative new drugs are breaking the mould ► Cancer medicines have only limited grounds to be a ‘special case’ QUESTIONS • Is there something ‘special’ about cancer that implies that it should be taken outside normal prioritization decisions and funded separately? • Should payers establish a minimum clinical hurdle for new cancer drugs to be seen as an advance to subsequently command a price premium - otherwise only similar acquisition costs to current standards? • Should payers automatically reject new risk sharing schemes unless fully transparent and all administrative costs considered? 3