Sample size planning for phase II trials based on success probabilities for phase III

We present an approach for planning a phase II trial in a time‐to‐event setting that considers the whole phase II/III clinical development programme. We derive stopping boundaries after phase II that minimise the number of events under side conditions for the conditional probabilities of correct go/no‐go decision after phase II as well as the conditional success probabilities for phase III. In addition, we give general recommendations for the choice of phase II sample size. Our simulations show that unconditional probabilities of go/no‐go decision as well as the unconditional success probabilities for phase III are influenced by the number of events observed in phase II. However, choosing more than 150 events in phase II seems not necessary as the impact on these probabilities then becomes quite small. We recommend considering aspects like the number of compounds in phase II and the resources available when determining the sample size. The lower the number of compounds and the lower the resources are for phase III, the higher the investment for phase II should be. Copyright © 2015 John Wiley & Sons, Ltd.

http://onlinelibrary.wiley.com/resolve/doi?DOI=10.1002%2Fpst.1717

Source: Pharmaceutical Statistics - September 1, 2015 Category: Statistics Authors: Heiko Götte, Armin Schüler, Marietta Kirchner, Meinhard Kieser Tags: Main Paper Source Type: research

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