A practical comparison of  group-sequential and adaptive designs

Kelly, P; Sooriyarachchi, M.R.; Stallard, N.; Todd, S.

dc.contributor.author	Kelly, P
dc.contributor.author	Sooriyarachchi, M.R.
dc.contributor.author	Stallard, N.
dc.contributor.author	Todd, S.
dc.date.accessioned	2021-07-07T03:29:22Z
dc.date.available	2021-07-07T03:29:22Z
dc.date.issued	2005
dc.identifier.citation	Kelly, P. Sooriyarachchi, M.R., Stallard, N. and Todd, S. A practical comparison of group-sequential and adaptive designs Journal of Biopharmaceutical Statistics 15: 719 – 738, 2005	en_US
dc.identifier.uri	http://archive.cmb.ac.lk:8080/xmlui/handle/70130/5489
dc.description.abstract	Sequential methods provide a formal framework by which clinical trial data can be monitored as they accumulate. The results from interim analyses can be used either to modify the design of the remainder of the trial or to stop the trial as soon as sufficient evidence of either the presence or absence of a treatment effect is available. The circumstances under which the trial will be stopped with a claim of superiority for the experimental treatment, must, however, be determined in advance so as to control the overall type I error rate. One approach to calculating the stopping rule is the group-sequential method. A relatively recent alternative to group-sequential approaches is the adaptive design method. This latter approach provides considerable flexibility in changes to the design of a clinical trial at an interim point. However, a criticism is that the method by which evidence from different parts of the trial is combined means that a final comparison of treatments is not based on a sufficient statistic for the treatment difference, suggesting that the method may lack power. The aim of this paper is to compare two adaptive design approaches with the groupsequential approach. We first compare the form of the stopping boundaries obtained using the different methods. We then focus on a comparison of the power of the different trials when they are designed so as to be as similar as possible. We conclude that all methods acceptably control type I error rate and power when the sample size is modified based on a variance estimate, provided no interim analysis is so small that the asymptotic properties of the test statistic no longer hold. In the latter case, the group-sequential approach is to be preferred. Provided that asymptotic assumptions hold, the adaptive design approaches control the type I error rate even if the sample size is adjusted on the basis of an estimate of the treatment effect, showing that the adaptive designs allow more modifications than the group-sequential method.	en_US
dc.language.iso	en	en_US
dc.subject	Fisher’s combination test; Fisher’s product; Power; Sequential clinical trials; Sequential design.	en_US
dc.title	A practical comparison of group-sequential and adaptive designs	en_US
dc.type	Article	en_US