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Journal of Biopharmaceutical Statistics Volume 23, 2013 - Issue 5
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Original Articles

A Review of Statistical Issues with Progression-Free Survival as an Interval-Censored Time-to-Event Endpoint

Xing Sun Merck & Co., Merck Research Labs, North Wales, Pennsylvania, USACorrespondence[email protected]
,
Xiaoyun Li Merck & Co., Merck Research Labs, North Wales, Pennsylvania, USA
,
Cong Chen Merck & Co., Merck Research Labs, North Wales, Pennsylvania, USA
&
Yang Song Merck & Co., Merck Research Labs, North Wales, Pennsylvania, USA
Pages 986-1003 | Received 22 Feb 2011, Accepted 08 Jun 2012, Published online: 19 Aug 2013
 
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Abstract

Frequent rise of interval-censored time-to-event data in randomized clinical trials (e.g., progression-free survival [PFS] in oncology) challenges statistical researchers in the pharmaceutical industry in various ways. These challenges exist in both trial design and data analysis. Conventional statistical methods treating intervals as fixed points, which are generally practiced by pharmaceutical industry, sometimes yield inferior or even flawed analysis results in extreme cases for interval-censored data. In this article, we examine the limitation of these standard methods under typical clinical trial settings and further review and compare several existing nonparametric likelihood-based methods for interval-censored data, methods that are more sophisticated but robust. Trial design issues involved with interval-censored data comprise another topic to be explored in this article. Unlike right-censored survival data, expected sample size or power for a trial with interval-censored data relies heavily on the parametric distribution of the baseline survival function as well as the frequency of assessments. There can be substantial power loss in trials with interval-censored data if the assessments are very infrequent. Such an additional dependency controverts many fundamental assumptions and principles in conventional survival trial designs, especially the group sequential design (e.g., the concept of information fraction). In this article, we discuss these fundamental changes and available tools to work around their impacts. Although progression-free survival is often used as a discussion point in the article, the general conclusions are equally applicable to other interval-censored time-to-event endpoints.

ACKNOWLEDGMENT

We thank the anonymous referee and the associate editor for their thoughtful comments, which have helped improve the presentation of this article.

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