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Abstract

Following phase I dose-finding oncology trials completed in Western countries, Asian investigators often conduct further phase I trials to determine the maximum tolerated dose for Asian patients. This may be due to concerns about possible differences in treatment tolerability between Caucasian and Asian patient groups. Our proposed approach aims to appropriately borrow strength from a previous Caucasian trial to improve the maximum tolerated dose determination in an Asian population of patients. We design an Asian phase I trial using the Bayesian continual reassessment method. First we analyze toxicity data from a Caucasian trial to derive the prior distributions for a subsequent Asian trial. Then, we calibrate the informativeness of the prior distributions according to prior effective sample size defined by Morita et al. Extensive simulation studies demonstrate favourable operating characteristics of the proposed method, compared with two methods based on power and noninformative priors, respectively.

Keywords

dose finding phase I study design historical data prior effective sample size continual reassessment method

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References

Morita

. Application of the continual reassessment method to a phase I dose-finding trial in Japanese patients: East meets West. Stat Med. 2011;30:2090–2097.

Ogura

Morita

Yonemori

. Exploring ethnic differences in toxicity in early-phase clinical trials for oncology drugs [published online March 3, 2014]. Therapeutic Innovation & Regulatory Science.

Budman

Meropol

Reigner

. Preliminary studies of a novel oral fluoropyrimidine carbamate: capecitabine. J Clin Oncol. 1998;16:1795–1802.

Mackean

Planting

Twelves

. Phase I and pharmacologic study of intermittent twice-daily oral therapy with capecitabine in patients with advanced and/or metastatic cancer. J Clin Oncol. 1998;16:2977–2985.

Pharmaceuticals Medical Devices Agency. Review reports (capecitabine) [in Japanese]. http://www.info.pmda.go.jp/shinyaku/P200700068/45004500_21500AMZ00400_A100_1.pdf. Accessed March 25, 2014.

O’Quigley

Pepe

Fisher

. Continual reassessment method: a practical design for phase I clinical trials in cancer. Biometrics 1990;46:33–48.

Thall

Lee

S-J

. Practical model-based dose-finding in phase I clinical trials: method based on toxicity. Int J Gynecol Cancer. 2003;13:251–261.

Carter

. Study design principles for the clinical evaluation of new drugs as developed by the chemotherapy program of the National Cancer Institute. In: Staquet

, ed. The Design of Clinical Trials in Cancer Therapy. Brussels, Belgium: Editions Scientifiques Europrennes; 1973:242–289.

Morita

Thall

Mueller

. Determining the effective sample size of a parametric prior. Biometrics. 2008;64:595–602.

10.

Morita

Thall

Mueller

. Evaluating the impact of prior assumptions in Bayesian biostatistics. Stat Biosci. 2010;2:1–17.

11.

Ibrahim

Chen

. Power prior distributions for regression models. Stat Sci. 2000;15:46–60.

12.

Gilks

Richardson

Spiegelhalter

. Markov Chain Monte Carlo in Practice. London, England: Chapman & Hall; 1996.

13.

Neuenschwander

Branson

Spiegelhalter

. A note on the power prior. Stat Med. 2009;28:3562–3566.

14.

Viele

Berry

Neuenschwander

. Use of historical control data for assessing treatment effects in clinical trials. Pharm Stat. 2014;13:41–54.

15.

Morita

Thall

Mueller

. Prior effective sample size in conditionally independent hierarchical models. Bayesian Anal. 2012;7:591–614.

16.

Liu

Hsiao

Hsueh

. Bayesian approach to evaluation of bridging studies. J Biopharm Stat. 2002;12:401–408.

17.

Goodman

Sladky

. A Bayesian approaches to randomized controlled trials in children utilizing information from adults: the case of Guillain-Barre syndrome. Clin Trials. 2005;2:305–310.

18.

Schoenfeld

. Bayesian design using adult data to augment pediatric trials. Clin Trials. 2009;6:297–304.

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Incorporating Historical Data in Bayesian Phase I Trial Design

Abstract

Keywords

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