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Diseños adaptativos y otros diseños innovadores. El punto de vista de los reguladores .

Diseños adaptativos y otros diseños innovadores. El punto de vista de los reguladores. Ferran Torres Hospital Clínic Barcelona / Universitat Autònoma Barcelona. EMA: Scientific Advice Working Party (SAWP) Biostatistics Working Party (BSWP). Documentation. Disclaimer

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Diseños adaptativos y otros diseños innovadores. El punto de vista de los reguladores .

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  1. Diseños adaptativos y otros diseños innovadores.El punto de vista de los reguladores. • Ferran Torres • Hospital Clínic Barcelona / Universitat Autònoma Barcelona. • EMA: • Scientific Advice Working Party (SAWP) • Biostatistics Working Party (BSWP). Ferran.Torres@uab.es

  2. Documentation Disclaimer The views expressed are those of the speaker and not necessarily those of the AEMPS or EMEA http://ferran.torres.name/docencia/amife Ferran.Torres@uab.es

  3. Hoy nos hablará un regulador Ferran.Torres@uab.es

  4. Ferran.Torres@uab.es

  5. Ferran.Torres@uab.es

  6. The idea of adaptive design • Allow for mid-trial design modifications based on information from in- and outside the trial without compromising on the false positive error rate. • The option to modify the design of an ongoing clinical trial is intuitively appealing • to improve the performance of the running trial • to correct misjudgments in assumptions • Only adaptive designs (if carefully planned and conducted) guarantee a strict type I error control in case of design modifications in on-going clinical trials Ferran.Torres@uab.es

  7. Issues of flexibility • Early stopping (futility, early rejection) • Selection of treatments • Modification of the total sample size • Treatment allocation ratios • Modification of statistical analysis (Choosing “optimal” scores …) • Insertion or skipping of interim analyses • Population (change of inclusion/exclusion criteria, subgroups) • Changing goals (non-inferiority →superiority) • Modification of endpoints • Adaptive dose-finding . . . Writing amendments for “online” design modifications will not be solution in general! An amendment will not ensure that the type I error is controlled! Ferran.Torres@uab.es

  8. Common issues in regulatory discussions on adaptive designs White space or thinking time? Independent replication Dose Type I error control Exploratory studies Totality of evidence for regulatory decision making: comprehensive planning, compare strategies Multiple adaptations Ferran.Torres@uab.es

  9. EMEA Reflection Paper Key principles • A minimal prerequisite is the control of the pre-specified type I error • Post hoc changes to the design of an already ongoing phase III trial are not recommended • If design changes are anticipated the number of design modifications should be limited Ferran.Torres@uab.es

  10. Challenges • Justification • Pre-specification • Bias, integrity of the trial • Heterogeneity • Confidentiality/firewalls • Operational flexibility, substantial amendments • Procedures for monitoring, decision-making • Impact on conduct and regulatory acceptance Early phases of drug development v. phase III Ferran.Torres@uab.es

  11. SAWP & BSWP • SAWP: • Multidisciplinary group of 28 experts (complementary scientific competences) • 11 annual meetings • Advice to sponsors on all aspects of drug development: • quality, non clinical, clinical • non-product related issues (e.g. on new statistical approach or validation of a scale) • qualification of biomarkers • Biostatistics Working Party: • 10 members (plus observers) • 3 F2F annual meetings + 10 TC Ferran.Torres@uab.es

  12. European Regulatory Activities “adaptive” and/or “flexible” in SA letters • Internal discussions and external networking • Reflection paper published Oct 2007 • Consultation period March – Sept 2006 http://www.emea.europa.eu/pdfs/human/ewp/245902enadopted.pdf • EMEA / EFPIA workshops on adaptive designs • 14th Dec 2007 http://www.emea.europa.eu/pdfs/conferenceflyers/report_adaptivedesigns.pdf • 2nd April 2009 ??? Which came first the chicken or the egg? Ferran.Torres@uab.es

  13. Survey of SAWP procedures • Broad range of therapeutic indications – including anti-fungal, HIV, uveitis, anti-biotic, Type II diabetes, colorectal cancer, glioblastoma, multiple sclerosis, NSCLC … • About one-third are orphan drugs. • Vast majority were as confirmatory studies (not surprising as this is the most common topic for SAWP advice) including numerous requests for adaptive designs as single pivotal trials • Adaptive designs in pure phase II trials, phase II/III, phase III • Most common proposals are sample size re-estimation, seamless phase II/III designs with treatment (dose) selection or both together Ferran.Torres@uab.es

  14. Survey of SAWP procedures Summary findings • Tendency to keep the number of interim analysis as small as possible • 1 interim analysis: ~65% , 2 interim analysis ~29% • Adaptations should be limited to one interim analysis • Timing of interim results • Adaptations should be based on a reasonable amount of data. Too early interim analysis are discouraged (e.g., survival data might be too pre-mature) • n=2 proposals of adaptive designs with the option to change the statistical analysis methodology at interim(e.g., switch from Cox proportional hazards model to parametric Weibull model) • There is a wide range on other questions concerning adaptive designs Ferran.Torres@uab.es

  15. Survey of SAWP procedures Key findings • In ~20-25% there were concerns regarding type I error control. • treatment selection (!!!) • sample size reassessment • no adjustment at all • type I error only simulated although methods with strict type I error would be available • Not endorsing adaptive design without strict type I error control is • not due to a negative position towards adaptive designs per se • but due to a positive position towards the importance of type I error control in clinical trials. Ferran.Torres@uab.es

  16. For Discussion No ‘white space’ / thinking time Sponsor risk Maintenance of homogenous trial / Assessment of heterogeneity Uncontroversial Dose selection framework Phase II data already available Unequivocal Type I error control No sponsor involvement (though senior personnel informed) Non-adaptive pivotal study also available Summary of design features Ferran.Torres@uab.es

  17. Areas still controversial • Adaptive designs as single pivotal study • Population (inclusion / exclusion criteria) • Change to primary endpoint based on internal information discouraged • Sponsor involvement • Strictly limited involvement has been cautiously accepted, in particular if not single pivotal study • “sponsor involvement discouraged” remains current standard • Informative adaptations in open-label trials Design adaptations with limited or no experience Ferran.Torres@uab.es

  18. Conclusions (1/2) • Flexible designs are an excellent tool to deal with unexpected findings But… • Design modifications should be justified and pre-specified • Address control of the type I error, estimates for the treatment effect • In late phase trials flexibility should be used care- and thoughtfully to maintain integrity and persuasiveness of the results • Too early looks may be strongly misleading Ferran.Torres@uab.es

  19. Conclusions (2/2) • Homogeneity of different stages (e.g., treatment effect before and after adaptive interim analysis) • Integrity and interpretation must be preserved • Need for operational flexibility / rigorous procedures, firewalls • Promote use of adaptive designs where appropriate: • Exploratory studies • Difficult experimental situations • Confirmatory studies where efficiency gains do not compromise basis for regulatory decision or present unacceptable ‘risk’ to trial / trial programme. • Further consideration to be given to unresolved issues Ferran.Torres@uab.es

  20. References • Reflection Paper on Methodological Issues in Confirmatory Clinical Trials planned with an adaptive design(CHMP/EWP/2459/02) • Points to Consider on Multiplicity issues in Clinical Trials (CPMP/EWP/908/99) • Points to Consider on Application with 1.) Meta-analyses and 2.) One Pivotal study (CPMP/2330/99) • Points to Consider on Switching between Superiority and Non-inferiority  (CPMP/EWP/482/99) • Points to Consider on Choice of the Non-Inferiority Margin (CPMP/EWP/2158/99) • Guideline on Data Monitoring Committees (CHMP/EWP/5872/03) • Statistical Principles for Clinical Trials. ICHE9. (CPMP/ICH/363/96) • FDA: Adaptive Design Clinical Trials for Drugs and Biologics(Draft feb-2010) Ferran.Torres@uab.es

  21. Gracias por su atención!! http://ferran.torres.name/docencia/amife Ferran.Torres@uab.es 21 Ferran.Torres@uab.es

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