Considerations for Improving Supervision of Clinical Practice From an Exploratory Case Study
Statistical considerations in exploratory studies · Session 2: Statistical considerations in...
Transcript of Statistical considerations in exploratory studies · Session 2: Statistical considerations in...
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SME workshop: Statistical perspectives in regulatory clinical development programmes Session 2: Statistical considerations in exploratory studies Presenter: Dr Byron Jones Executive Director Statistical Methodology and Consulting Novartis Pharma AG Basel Switzerland
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SME workshop: Statistical perspectives in regulatory clinical development programmes Session 2: Statistical considerations in exploratory studies I am speaking today on behalf of EFSPI, and any views or opinions expressed in this presentation are personal, and should not be attributed to my employer, Novartis Pharma, AG.
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Acknowledgements: Bjoern Bornkamp, Frank Bretz, Ieuan Jones, Roland Fisch, Heinz Schmidli, Oliver Sander, Parasar Pal.
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Contents
• Introduction to drug development • Pharmacokinetics(PK)/Pharmacodynamics(PD) • Phase I dose escalation • Phase II proof-of-concept • Phase II dose finding • Adaptive dose finding designs • Predictive power • [Modelling and simulation are scattered throughout]
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Drug Development Path A well defined but complicated journey
• Drug development follows a well-defined path: – Drug discovery and preclinical development – Clinical development
• Phase I, II, & III clinical trials – Regulatory application and registration
• Approval by health authorities from different countries
– Post-Approval / Marketing • Phase IV clinical trials
• Drug development – very complex, with a high risk of failure
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An Overview of Drug Development From research to registration
Safety Proof of concept Efficacy / PK / Dose finding
~ 11-15 years
Research Development
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An Overview of Drug Development From research to registration: high risk
Safety Proof of concept Efficacy / PK / Dose finding
~ 11-15 years
Research Development
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10 high attrition rate
10K compounds
1 drug to market
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An Overview of Drug Development From research to registration
Phase Sample size per study
Length per study
Study population
Objective
I First in human/PK
6 – 20 Weeks – Months
Healthy volunteers
Safety, pharmacokinetics & pharmacodynamics; determining maximum tolerated dose (MTD)
II First in patients
50 – 200
Months Patients Proof of concept; dose finding
III Submission
200 – 10,000
Months – Years
Patients Confirmatory
IV Post approval
Broad range
Broad range
Patients Post marketing Health Authority commitments; health economics; pharmacovigilance
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An Overview of Drug Development Early Phase Trials
Phase Sample size per study
Length per study
Study population
Objective
I First in human
6 – 20 Weeks – Months
Healthy volunteers
Safety, pharmacokinetics & pharmacodynamics; determining maximum tolerated dose (MTD)
II First in patients
50 – 200
Months Patients Proof of concept; dose finding
III Submission
200 – 10,000
Months – Years
Patients Confirmatory
IV Post approval
Broad range
Broad range
Patients, Market
Post marketing Health Authority commitments; health economics; pharmacovigilance
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An Overview of Drug Development Phase I trials
Safety Proof of concept Efficacy / PK / Dose finding
~ 11-15 years
Research Development
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• First studies of drug in humans • Pharmacokinetics (PK) & Pharmacodynamics (PD) • Maximum Tolerated Dose (MTD)
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Phase I trials pharmacokinetics and pharmacodynamics
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Pharmacokinetics “What does the body do with the drug?”
Pharmacokinetics is the study of
• Absorption: How the drug gets absorbed into the blood
• Distribution: How the drug is distributed in the body when it has reached the blood
• Metabolism: How the drug is changed in the body
• Excretion: How the drug is excreted/eliminated from the body
To answer these questions, samples of blood, urine, feces, etc., are taken from healthy volunteers or patients over a set time period and the concentrations of drug in these are measured.
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Example drug-concentration vs time plot concentrations in blood for each patient can be plotted
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Simple one-compartment model model to explain shape of plot can be proposed
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Stomach
Blood
Dose
absorption
excretion
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Simple one-compartment model model to explain shape of plot can be proposed
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Stomach
Blood
Dose
absorption
excretion
rate=ka
rate=ke
concentration in stomach =
C1(t)
concentration in blood = C2(t)
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One compartment model model for concentration of drug in blood
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Typical drug-concentration plots After multiple oral doses
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Typical drug-concentration plots After multiple oral doses
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steady state
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Single Ascending Dose (SAD) study How to choose a dose to take forward into clinical trials
First-in-Human (FIH) study healthy male (or female) subjects low number of subjects (limit risks) single doses: cohorts of subjects go from low doses to
high doses, in an ascending fashion, up to the maximum tolerated dose (MTD)
each dose may be given to a different cohort of subjects
blinded Evaluate safety and tolerability before increasing dose to
next level so adaptive in nature
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Single Ascending Dose (SAD) design
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Stopping rule based on number of SAEs -> MTD ? Stop
Cohort (8 subjects, 6 active, 2 placebo)
increasing dose
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Single Ascending Dose (SAD) designs
• Choice of starting dose – FDA
– EMA
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Single Ascending Dose (SAD) design
• Subjects in a cohort are assessed for safety and tolerability before dose is increased
• Safety: adverse events
• Study can be stopped at any time
• Secondary objective is to evaluate PK
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Multiple Ascending Dose (MAD) design How to choose a dose to take forward into clinical trials
• Started once MTD of single dose is established • Healthy subjects will typically take a dose of the drug
daily for a period of time • Important to evaluate safety and tolerability of multiple
dosing at steady state • Design is similar in structure to SAD design
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Multiple Ascending Dose (MAD) design
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increasing dose
e.g., one dose taken daily for 10 days 6:2 (active:placebo) randomization
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An Overview of Drug Development Phase IIa trials
Safety Proof of concept Efficacy / PK / Dose finding
~ 11-15 years
Research Development
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• Phase IIa – Proof of concept • Phase IIb – Dose finding
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Proof of Concept (PoC) A key milestone in drug development
• Definition given by PhRMA (Pharmaceutical Research and Manufactures of America):
PoC is the earliest point in the drug development process at which the weight of evidence suggests that it is reasonably likely that the key attributes for success are present and the key causes of failure are absent
• PoC is the translational step from “Research” to “Clinical Development”
Cartwright, et al. (2010)
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Cartwright, M. E., et al. (2010). Proof of Concept: a PhRMA position paper with recommendations for best practice, Clinical Pharmacology and Therapeutics, vol. 87, p. 278–285.
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Example PoC study Fisch, R., et al. (2014)
• Cystic Fibrosis (CF):
– a “genetic disorder ... that affects mostly the lungs... Long-term issues include difficulty breathing .. as a result of frequent lung infections.” [Wikipedia]
• Study design: randomized, double-blind, placebo-controlled parallel groups trial
• Primary endpoint: change from baseline in percentage of predicted Forced Expired Volume over 1 second (FEV1) at day 28
• Fisch, R., Jones, I., Jones, J., et al. (2014) Bayesian Design of Proof-of-Concept Trials. Therapeutic and Regulatory Science. Published online 14 May 2014.
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PoC criteria What is “weight of evidence”?
• Not only interested in statistical significance (p-value) of effect of drug vs placebo
• But whether the improvement over placebo is clinically relevant.
• Need both to declare a successful PoC study result
• Also need to consider probability of making correct PoC decision
• Bayesian methodology most suited to planning and analysing a PoC study
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Bayesian Methodology very short introduction
• Gives a formal way of integrating prior knowledge of the treatment effect in the form of a prior distribution with the distribution of the data from the trial in the form of the likelihood to give an updated estimate of the treatment effect in the form of a posterior distribution
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PoC criteria clinical relevance
• Define a threshold separating marginal from competitive efficacy. Given various names: – target difference; minimum clinically important
difference ; walk-away-point, ... • Generally smaller than both treatment effect of
best compounds on market and “alternative” treatment effect used in traditional power calculations.
• But can be higher in a more aggressive PoC study
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Example PoC study, cont’d Fisch, R., et al. (2014)
• Historical data from a competitor shows mean improvements over placebo of around 10% in the primary endpoint in a similar population
• Clinical considerations lead to the decision that if the true improvement of the drug over placebo was greater than 5% then it would be good enough to take further into development
• Hence the walk-away-point was set at 5%
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Example PoC study, cont’d Fisch, R., et al. (2014)
• Recall, that in addition to this clinical requirement, we also require statistical significance when drug is compared to placebo, i.e., strong evidence that improvement is greater than zero
• This was expressed as a 10% one-sided significance level
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PoC criteria What has to be achieved to declare a positive PoC
• Let θ = true difference between means of the primary endpoint when drug is compared to placebo
• PoC criteria (Bayesian in nature):
– Significance: Prob(θ >0 | data from trial) >= 0.90
– Relevance: Prob(θ > 5% | data from trial) >= 0.50
• In the former we require high level of confidence and in the latter a moderate level of confidence
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PoC: Possible decisions Go, Stop, Indeterminate
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relevance
significance
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PoC: Possible decisions Go, Stop, Indeterminate
• A well-designed PoC study will aim to minimize the chance of a false decision ...
• and achieve an acceptable balance between the probabilities of GO or STOP decisions and the probability of an INDETERMINATE decision
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Optimizing the design of a PoC study Using operating characteristics
• How do we decide if the design of the PoC study (sample size, choice of decision thresholds) is good enough?
• The answer is to calculate the operating characteristics of the design, e.g., the posterior probabilities of making correct decisions under different choices for the true value of the treatment effect
• This is done either using technical calculations in simple situations or by simulation in more complicated situations (interim analysis, sample size re-estimation,...)
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PoC Example cont’d operating characteristics for CF design
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Plot shows posterior probability (vertical axis) of each decision (GO: green curve, STOP: red curve, IND: orange curve), as the size of the drug vs placebo effect changes from 0 to 8 (horizontal axis)
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PoC Example cont’d operating characteristics for CF design
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Plot shows posterior probability (vertical axis) of each decision (GO: green curve, STOP: red curve, IND: orange curve), as the size of the drug vs placebo effect changes from 0 to 8 (horizontal axis)
three probabilities add to 1 for each treatment difference
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PoC Operating Characteristics sample size 78 (52:26)
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90% chance to stop when difference=0
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PoC Operating Characteristics sample size 78 (52:26)
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50% chance of GO when difference=5%
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PoC Operating Characteristics sample size 78 (52:26)
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Maximum chance (30% approx) of indeterminate occurs when difference is about 4%
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PoC Operating Characteristics sample size 78 (52:26)
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Chance of a GO decision is 68% approx when difference is 6%
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PoC Operating Characteristics use these to look at design modifications • Modifications such as – Changing sample size – Adding an interim analysis
• stop or go decision at interim • re-estimate sample size at interim
– Changing decision thresholds • Can be investigated by simulating the trial many
(1000s) times within a computer • Final choice of design can then be made based
on operating characteristics
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An Overview of Drug Development Phase IIb trials
Safety Proof of concept Efficacy / PK / Dose finding
~ 11-15 years
Research Development
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• Phase IIa – Proof of concept • Phase IIb – Dose finding
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Phase II Dose Finding Phase IIb trials
• A well-known quote to begin with:
All things are poison and nothing is without poison, only the dose permits something not to be poison. - Paracelsus (1493-1541)
Source: Wikipedia
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What needs to be learned in Phase IIb?
• Determine the dose-response relationship. • What is the effect size the drug can achieve? • Identify increasing part of dose-response (what is the
largest dose with placebo-like effect, what is the smallest dose with (close-to) maximum effect)?
• Which doses lead to an unacceptable efficacy tolerability/safety trade-off (i.e., what is the therapeutic window)?
• Ultimately to choose dose(s) for Phase III trial
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What are the important features of a dose-response relationship?
• In the following we consider a basic shape for the dose-response and identify some important metrics
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Standard (increasing) dose response shape
Placebo response
Maximum response
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Standard (increasing) dose response shape
Placebo response
Maximum response
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Standard (increasing) dose response shape
Placebo response
Maximum response
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Standard (increasing) dose response shape
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Often can specify a clinically relevant effect Δ above Placebo
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Standard (increasing) dose response shape Effective dose range
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Standard (increasing) dose response shape Alternative target responses: 50% and 90% of maximum response
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Standard (increasing) dose response shape ED50 and ED90
EDxx : dose that gives xx percent of the maximum improvement over Placebo
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Standard (increasing) dose response shape Dose range of interest: steep part of the curve
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Emax model One very useful parameterization of the dose response model (D=dose)
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Sigmoid Emax Model A generalization of the Emax model (additional parameter h)
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Number of Active Doses
• If dose-response curve was known: – 3-4 doses enough, placed to cover interesting range
and maximim effect • Larger number of doses become necessary due to
uncertainty • Adequate trade-off often in the range of 4-6 active doses
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NVA case-study
Example
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Publication available
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NVA237: a treatment for COPD • Chronic Obstructive Pulmonary Disease (COPD) is a
disease of the lungs characterized by airflow limitation which is not fully reversible
• The investigational drug NVA237 is a dry powder formulation of the muscarinic receptor antagonist glycopyrronium bromide
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A placebo-controlled study with 6 treatment groups
• The primary purpose of the study was to provide data about the efficacy of four doses of NVA237 (12.5, 25, 50 and 100μg o.d.) and open-label tiotropium (18μg) and to identify a dose of NVA237 that could be investigated in Phase III studies
• The primary endpoint was the evaluation of the bronchodilatory efficacy of NVA237 in patients with stable COPD in terms of trough forced expiratory volume over 1 second (FEV1) following 7 days of treatment 62
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Plot of means with confidence intervals using data from completed trial
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Clinically meaningful effect 1.2L over placebo
Plot of observed means plus 95% confidence intervals
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Plot of means with confidence intervals using data from completed trial
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Clinically meaningful effect 1.2L over placebo
What shape, i.e., model, describes these data best? Is an Emax model the best fit?
Plot of observed means plus 95% confidence intervals
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Is Emax the only realistic shape for the NVA dose response?
• Although we might prefer to fit an Emax model, this may not be the only possible dose-response shape
• In fact at the planning stage of the NVA trial, there was some uncertainty regarding the shape of the dose-response
• Five different shapes were considered
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Candidate models specified before trial start
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Candidate models specified before trial start
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How to decide which one fits the trial data best?
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MCP-Mod Methodology
Developed by Statistical Methodologists
at Novartis Pharma
Choosing models under uncertainty
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What is MCP-Mod? Multiple Comparison Procedures – Modelling: Overview (1/2)
• A method for model-based dose-response testing and estimation • MCP-step
- Establish a dose-response signal (i.e., that the dose-response curve is not flat) using multiple comparison procedures
• Mod-step - Estimate the dose-response curve and target doses
of interest (ED50, ED90, MED, etc.) using modelling techniques
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CHMP Qualification Opinion
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NVA Example: Final Model Choice Output from R DoseFinding package (Bornkamp, et al., 2015)
# Estimated Dose Response Models: # emax model # e0 eMax ed50 # 1.244 0.169 18.004 # ... #
# Selected model (AIC): emax # # Estimated TD, Delta=0.12 # emax sigEmax quadratic # 44.0640 45.1114 46.2157
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THE END (of the lecture)
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But not the journey!