Literature DB >> 28943681

Robust treatment comparison based on utilities of semi-competing risks in non-small-cell lung cancer.

Thomas A Murray1, Peter F Thall1, Ying Yuan1, Sarah McAvoy2, Daniel R Gomez2.   

Abstract

A design is presented for a randomized clinical trial comparing two second-line treatments, chemotherapy versus chemotherapy plus reirradiation, for treatment of recurrent non-small-cell lung cancer. The central research question is whether the potential efficacy benefit that adding reirradiation to chemotherapy may provide justifies its potential for increasing the risk of toxicity. The design uses two co-primary outcomes: time to disease progression or death, and time to severe toxicity. Because patients may be given an active third-line treatment at disease progression that confounds second-line treatment effects on toxicity and survival following disease progression, for the purpose of this comparative study follow-up ends at disease progression or death. In contrast, follow-up for disease progression or death continues after severe toxicity, so these are semi-competing risks. A conditionally conjugate Bayesian model that is robust to misspecification is formulated using piecewise exponential distributions. A numerical utility function is elicited from the physicians that characterizes desirabilities of the possible co-primary outcome realizations. A comparative test based on posterior mean utilities is proposed. A simulation study is presented to evaluate test performance for a variety of treatment differences, and a sensitivity assessment to the elicited utility function is performed. General guidelines are given for constructing a design in similar settings, and a computer program for simulation and trial conduct is provided.

Entities:  

Keywords:  Bayesian Analysis; Group Sequential; Piecewise Exponential Model; Radiation Oncology; Randomized Comparative Trial; Utility Elicitation

Year:  2017        PMID: 28943681      PMCID: PMC5607962          DOI: 10.1080/01621459.2016.1176926

Source DB:  PubMed          Journal:  J Am Stat Assoc        ISSN: 0162-1459            Impact factor:   5.033


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