• PSI One Day Meeting: Extrapolation

    Stevenage | Dates: 22 Nov, 2017
    Use of extrapolation techniques is playing an increasingly important role in the development of new medicines particularly with regard to special populations such as paediatrics and rare diseases. This meeting will include speakers from industry, academia and regulatory (including Rob Hemmings from MHRA).

    Speakers include:
    • Peter Milligan - Pfizer
    • Kristin Karlsson - Medical Products Agency, Sweden
    • Rob Hemmings - MHRA
    • Nicky Best - GSK
    • Dawn Edwards - GSK
    • Adrian Mander - MRC Biostatistics Unit, University of Cambridge
    • Lisa Hampson - AstraZeneca
    • Ian Wadsworth - Lancaster University
    Please click here to view the flyer.


    Rob Hemmings, MHRA

    Extrapolation; regulatory need, examples and emerging guidance.

    Abstract: Extrapolation is defined as ‘extending information and conclusions available from studies in one or more subgroups of the patient population (source population(s)), or in related conditions or with related medicinal products, to make inferences for another subgroup of the population (target population), or condition or product, thus reducing the amount of, or general need for, additional information (types of studies, design modifications, number of patients required) needed to reach conclusions for the target population, or condition or medicinal product’.  The talk will illustrate the potential need for, and benefits of, this concept in regulatory work with a primary focus on extrapolation from adults to children.  An overview of the EMA Reflection Paper on this topic will be presented and discussed, highlighting areas for further discussion and research.

    Ian Wadsworth, Lisa V. Hampson, Thomas Jaki and Graeme J. Sills

    Using historical data to inform extrapolation decisions in children

    When developing a new medicine for children, the potential to extrapolate from adult efficacy data is well recognised. However, significant assumptions about the similarity of adults and children are needed for extrapolations to be biologically plausible. One such assumption is that pharmacokinetic-pharmacodynamic (PK-PD) relationships are similar in these different groups. In this presentation, we consider how ‘source’ data available from historical trials completed in adults and adolescents treated with a test drug, can be used to quantify prior uncertainty about whether PK-PD relationships are similar in adults and younger children. A Bayesian multivariate meta-analytic model is used to synthesise the PK-PD data available from the historical trials which recruited adults and adolescents. The model adjusts for the biases that may arise since these existing data are not perfectly relevant to the comparison of interest, and we propose a strategy for eliciting expert prior opinion on the size of these external biases. From the fitted bias-adjusted meta-analytic model we derive prior distributions which quantify our uncertainty about the similarity of PK-PD relationships in adults and younger children. These prior distributions can then be used to calculate the probability of similar PK-PD relationships in adults and younger children which, in turn, may be used to inform decisions as to whether complete extrapolation of efficacy data from adults to children is currently justified, or whether additional data in children are needed to reduce uncertainty. Properties of the proposed methods are assessed using simulation, and their application to epilepsy drug development is considered.

    Clara Domínguez-Islas1, Adrian Mander1, Rebecca Turner2, Nicky Best3

    A Bayesian framework for extrapolation using mixture priors 

    1 MRC Biostatistics Unit, University of Cambridge, UK.

    2 MRC Clinical Trials Unit, University College London, UK.

    3 GlaxoSmithKline, UK.

    As defined by the European Medicines Agency (EMA), extrapolation refers to the extension of information and conclusions available from studies in a source population to make inferences in a target population, in order to reduce the amount of additional information needed to reach conclusions for the latter.  Bayesian inference seems to provide a natural framework to implement the extrapolation principle, as the information from the source population can be used as the prior beliefs for the target population. However, intrinsic to extrapolation principle, there is also the belief that the source and target populations, although similar enough to allow one of them to inform the other, are not exactly the same and important differences, not known a priori, might exist. Therefore, along with informative priors, we also need to incorporate a certain degree of scepticism. This could be achieved by the use of mixture priors.  Although mixture priors have been already proposed in different extrapolation contexts (bridging studies, historical controls, paediatric extrapolation), we identify some gaps in the research conducted and reported so far. In this presentation, we intend to further explore and better understand the potential of mixture priors to provide a quantitative framework for extrapolation. First we present the mixture prior model with special emphasis on the interpretation and type of inference that it allows, providing a connection with Bayesian model averaging. We then address some of the challenges that arise when constructing a mixture prior, including the choices to be made for each of the components of the model, as well as technical aspects of the estimation and computation. Finally, we discuss the frequentist operating characteristics of this approach and identify the trade-offs that come with the flexibility and robustness of the mixture priors. 

    Lisa V Hampson, Franz Koenig

    Use of frequentist and Bayesian approaches for extrapolating from adult efficacy data to design and interpret confirmatory trials in children

    New medicines for children should be subject to rigorous examination whilst taking steps to avoid unnecessary experimentation. Extrapolating from adult data can reduce uncertainty about a drug’s effects in younger patients meaning smaller trials may suffice.

    We consider how to design a confirmatory trial in children intended to compare the efficacy of a new drug, E, against control. Assuming that conduct of this trial is conditional on having demonstrated a significant beneficial effect in adults, we adopt a Bayesian approach to incorporate these adult data into the design and analysis of the paediatric trial. At each stage, inferences are made using all available data to update a Bayesian mixture model for prior opinion on the degree of similarities between adults and children. Using this framework, we propose designs for the paediatric trial which are specified by calibrating the sample size and final decision rule to: a) achieve a high frequentist power and high minimum (or average) Bayesian positive predictive value of a significant result in children; or b) ensure that a final decision to adopt (abandon) drug E in children is always associated with a minimum positive (negative) predictive value. Operating characteristics of our Bayesian designs are evaluated and compared with those of a recently proposed hybrid approach (Hlavin et al. Statistics in Medicine 2016; 35: 2117) where the sample size and significance level of a frequentist confirmatory trial in children are set to achieve a high frequentist power and high average positive predictive value of a significant result in children.

    Nicky Best, Dawn Edwards

    A case study using Bayesian methods to leverage existing clinical efficacy data in paediatric trials

    Recently there has been increased regulatory interest in partial extrapolation of adult efficacy information to paediatrics populations to reduce data collection requirements in children.  In this talk we will present a case study describing plans to use partial extrapolation of adult efficacy data from a phase III trial of an experimental drug in adolescents with a respiratory disease.  We will demonstrate how adult data on the treatment difference for the endpoint of interest can be included via an informative prior distribution to increase the probability of success of the study in adolescents and the precision of the estimated treatment difference. A method which incorporates dynamic borrowing will be used to define the level of extrapolation using a 2-step approach whereby information from the adult data is first incorporated into a prior distribution before being integrated with the data from the adolescent population. We propose a 3-component weighted robust mixture prior with the informative components based on (1) the adult efficacy data, (2) rescaled adult efficacy data to reflect the expected response for the adolescent population, and (3) a flat component to ensure that, in the event the adolescent and adult data are in clear conflict, the latter will have minimal influence on the posterior distribution of the treatment difference, thus also preventing excessive inflation of type 1 error. We will present results of a simulation study investigating operating characteristics for different choices of success criteria and prior weights.

    Peter Milligan

    Utilizing a Quantitative Framework to support Extrapolation

    Peter A Milligan on behalf of the EFPIA MID3 Workgroup 

    The 2016 white paper on Good Practices in Model-Informed Drug Discovery and Development: Practice, Application, and Documentation (1) defines Model Informed Drug Discovery and Development (MID3) as a ‘‘quantitative framework for prediction and extrapolation, centred on knowledge and inference generated from integrated models of compound, mechanism and disease level data and aimed at improving the quality, efficiency and cost effectiveness of decision making’’.

    MID3 in its simplest form embodies using ‘‘fit-for-purpose’’ mathematical models, implemented according to good practices, in order to enhance the extraction of inference from both existing information and data emanating from ongoing experiments. As the underpinning foundations for MID3 are based on robust scientific principles derived from pharmacological, physiological, and pathological processes (the domain sciences), MID3 can more effectively support translation across, and extrapolation beyond, the direct inference obtained from standard descriptive methods applied to experimental data.

    Conversion of the current knowledge captured within the ‘‘fit-for-purpose’’ model into inference requires a prediction based either on particular model parameter estimates or utilizing values generated through simulation. Predictions can either be interpolative or extrapolative with respect to available evidence and the intended purpose.

    Extrapolations beyond current experience often provide the greatest value to pharmaceutical companies. The recent EMA concept paper on The Extrapolation of Efficacy and Safety Data in Medicine Development (2) identified the approaches utilized in MID3 as part of the extrapolation concept and for inclusion in an extrapolation plan. The use of extrapolations emanating from an appropriate quantitative framework to bridge efficacy and safety in special populations was discussed in the 2011 joint workshop (3) with some of the resultant proposals subsequently published in greater detail (4). Replacement of direct experimental evidence (including all or part of a clinical trial) in a development program is conceptually ‘‘permissible’’ but considered to be of ‘‘high regulatory impact’’ (5) necessitating substantive a priori discussions with the regulatory agencies to characterize the context of use for any resultant extrapolations. 

    1. SF Marshall et al, CPT Pharmacometrics Syst. Pharmacol. (2016) 5, 93–122; doi:10.1002/psp4.12049
    2. EMA/EFPIA European Medicines Agency/European Federation of Pharmaceutical Industries and Associations workshop on the importance of dose finding and dose selection for the successful development, licensing and lifecycle management of medicinal products. http://www.ema.europa.eu/ema/index.jsp?curl5pages/news_and_events/events/2014/06/event_detail_000993.jsp&mid5WC0b01ac058004d5c3 (2014).
    3. EMA/EFPIA M&S workshop 2011. http://www.ema.europa.eu/ema/index.jsp?curl5pages/news_and_events/events/2011/07/event_detail_000440.jsp&mid5WC0-b01ac058004d5c3 (2011).
    4. Harnisch, L., Shepard, T., Pons, G., Della Pasqua, O. Modeling and Simulation as a Tool to Bridge Efficacy and Safety Data in Special Populations CPT: Pharmacometrics & Systems Pharmacology 2, e28 (2013).
    5. Manolis, E., Rohou, S., Hemmings, R., Salmonson, T., Karlsson, M. & Milligan, P.A. The role of modeling and simulation in development and registration of medicinal products: output from the EFPIA/EMA Modeling and Simulation Workshop. CPT Pharmacometrics Syst. Pharmacol. 2, e31 (2013).

    Registration on or before 22nd October
    PSI Member  £120 (plus VAT)
    Non-Member  £160 (plus VAT)
    Academic   £60 (plus VAT) 
    Registration after 22nd October
    PSI Member  £160 (plus VAT)
    Non-Member  £220 (plus VAT)
    Academic  £90 (plus VAT)

    Registration is now closed.
  • European Statistical Meeting: Latest Trends in Health Technology Assessments

    Two Pancras Square | Dates: 28 Nov, 2017

    This 1-day scientific meeting will provide an update on latest trends in HTA, including: the Real-World Evidence Navigator tool created by the IMI GetReal project; the EUnetHTA Joint Action 3 initiative and methodology being researched; introduction to value-based frameworks and estimands in HTA.  Patient perspectives in HTA will be discussed including how to involve patients in HTA and latest methods in patient reported outcomes.  HTA related methodological considerations will be highlighted including approaches to handle treatment switching in HTA.  Industry HTA case studies will also be presented. 

    Speakers include well known representatives from academia, European regulatory bodies and industry. The day will end with a panel discussion.

    To download the flyer please click here.

    Outline of the Agenda

     09:30 Welcome
    Chrissie Fletcher (Amgen, Chair HTA SIG), William Malbecq (MSD)
     09:50 Session: Trends in HTA(1)

    Introducing the RWE Navigator - Heather Stegenga (NICE)

    EUnetHTA Joint Action 3 activities - Zoe Garrett (NICE)

     11:10 Coffee Break
     11:30 Session: HTA research and methods

    Adjusting for treatment switching in randomised controlled trials - Nick Latimer (University of Sheffield)

    Accumulated Industry experience in bridging regulatory and HTA research methodologies - William Malbecq, Kristel Vandormael (MSD)
     12:50  Lunch
     13:30 Session: Patient perspectives in HTA

    Involving the patient in HTA - Karen Facey (Evidence Based Health Policy Consultant)

    Benefit-Risk assessments in HTA - Shahrul Mt-Isa (MSD), Susan Talbot (Amgen)
     14:50 Coffee Break
     15:10 Session: Trends in HTA(2)

    Value-based frameworks - Jan McKendrick (PRMA Consulting)

    Estimands in HTA - Jason Wang (Celgene), Chrissie Fletcher (Amgen)

     16:30 Panel Discussion
     17:00 Summary and meeting close


    Fee includes lunch & refreshments.

    Registration on or before 14th October
    PSI Member  £100 (plus VAT)
    Non-Member  £140 (plus VAT)
    Academic  £70 (plus VAT)
    Registration after 14th October
    PSI Member  £120 (plus VAT)
    Non-Member  £160 (plus VAT)
    Academic  £90 (plus VAT)

    Please click here to register.
  • PSI Toxicology SIG Webinar

    Dates: 12 – 12 Dec, 2017

    The next PSI Toxicology SIG webinar is on the 12th December at 14:00 GMT.

    Thomas Jaki is presenting about “Optimal designs for non-compartmental PK studies”.

    In traditional PK/PD trials, pharmacokinetics (PK) is investigated in the satellite group of animals, and the pharmacodynamics (PD) is investigated in the study group of animals. The new blood sampling method of microsampling opens up the opportunity to investigate both PK and PD in the same animals. To avoid excessive burden on the animals from the required blood sampling, sparse sampling schemes are typically utilized. Motivated by this application, this talk introduces a procedure to choose an optimal sparse sampling scheme and sampling time points using non-compartmental methods but which can be applied to further settings beyond this. We discuss how robust designs can be obtained and we apply and evaluate the approach to a range of scenarios to give an example of how it may be implemented. The results are compared to optimal designs for model based PK.

    Registration for this webinar is free. Please click here to register.
  • A PSI Training Course on Missing Data

    Heathrow | Dates: 06 – 07 Mar, 2018
    The aim of this course is to provide participants with an understanding of missing data, its link with what is to be estimated in a study (the “estimand”), and statistical modelling approaches. The 2 day course includes workshops: participants will undertake a number of practical exercises on missing data in SAS. The course will provide participants the opportunity to gain insight into some of the more useful new methodologies for missing data, with a view to being at the service of the real scientific question of interest. Multiple imputation (MI) will be emphasised – due to this method’s flexibility.

    Attendees will require a laptop with access to SAS.

    The following topics will be covered:
    - History of research into missing data
    - Prevention of missing data and impact on study power
    - Missing Data and its relation to the estimand
    - Estimands and their models
    - Multiple imputation I: models for missing data
    - Weighting I: weighting for missing data
    - Multiple imputation II: methods for non-continuous endpoints
    - Weighting II: augmenting weighed data with model estimates
    - Composite endpoints
    - Case studies

    Course runs from:
    10:00 - 17:00 (registration from 09:00) on Day 1
    09:00 - 16:00 on Day 2


    Registration costs include lunch and refreshments. PSI are holding a limited number of hotel rooms until the 31st January 2018 which will be allocated on a first come first served basis.

    Registration BEFORE 31st January 2018 
     PSI Member  £495 plus VAT
     Non-Member  £590 plus VAT
     Registration AFTER 31st January 2018
     PSI Member  £595 plus VAT
     Non-Member  £690 plus VAT

    Please click here to register.
    Please click here to view the flyer.
  • PSI Toxicology SIG Workshop 2018

    Stockley Road | Dates: 24 – 25 Apr, 2018

    The Toxicology SIG provides a forum for statisticians working in regulatory and investigative toxicology to discuss issues and interact with one another. 

    This 1.5-day workshop will involve hopefully approximately 20 statisticians, focusing on discussions around “best practice” in the statistical analysis of various data types. 

    The cost will be £225 including VAT per delegate, inclusive of food and one night’s accommodation.  The workshop is being held at the Crowne Plaza Hotel, Heathrow. 

    The agenda and topics that will be discussed is yet to be finalised, but please get in touch with gareth.thomas@envigo.com if you have suggestions.  Full details will be circulated in the coming months.

    Registration Costs
     £225 incl VAT Inclusive of food and one night’s accommodation 

    Please click here to register.