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- Exploring the Benefits of Adaptive Sequential Designs in Time-to-Event Endpoint Settings
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- Abstract:
- Sequential analysis is frequently employed to address ethical and financial issues in clinical trials.
Sequential analysis may be performed using standard group sequential designs, or, more recently, with
adaptive designs that use estimates of treatment effect to modify the maximal statistical information to
be collected. In the general setting in which statistical information and clinical trial costs are functions of
the number of subjects used, it has yet to be established whether there is any major efficiency advantage
to adaptive designs over traditional group sequential designs. In survival analysis, however, statistical
information (and hence efficiency) is most closely related to the observed number of events, while trial
costs still depend on the number of patients accrued. As the number of subjects may dominate the cost
of a trial, an adaptive design that specifies a reduced maximal possible sample size when an extreme
treatment effect has been observed may allow early termination of accrual and therefore a more costefficient
trial. We investigate and compare the tradeoffs between efficiency (as measured by average
number of observed events required), power, and cost (a function of the number of subjects accrued
and length of observation) for standard group sequential methods and an adaptive design that allows
for early termination of accrual. We find that when certain trial design parameters are constrained,
an adaptive approach to terminating subject accrual may improve upon the cost efficiency of a group
sequential clinical trial investigating time-to-event endpoints. However, when the spectrum of group
sequential designs considered is broadened, the advantage of the adaptive designs is less clear.
- Subject Area:
- Clinical Trials
- Suggested Citation:
- Sarah C. Emerson, Kyle Rudser, and Scott S. Emerson,
"Exploring the Benefits of Adaptive Sequential Designs in Time-to-Event Endpoint Settings"
(January 13, 2010).
UW Biostatistics Working Paper Series.
Working Paper 356.
http://www.bepress.com/uwbiostat/paper356