Abstract

The goal of the research project is to carry out an extensive investigation of several areas of statistical methodology for the design and analysis of biomedical studies, applicable to various areas of health research, especially cancer clinical trials and epidemiology. The research falls into four main categories: (a). Evaluation of adaptive group sequential clinical trials. This methodology permits design modifications in mid-course, while preserving the Type I error. The changes may be caused by information either internal or external to the trial. We will emphasize procedures based on the sufficiency principle so that efficiency (power) is maximized. We will develop a theory of optimal adaptive tests and produce a """"""""catalog"""""""" of conventional non-adaptive designs that are easy to implement yet are almost as efficient. We investigate the related topic of strategies of accelerating the process of staged development of new therapies. (b). Statistical design and analysis of studies that involve clustered data. These arise, for example, in familial aggregation, teratology and cluster randomized trials. We concentrate on binary, continuous, survival and multivariate mixed type endpoints from clusters of unequal sizes. Responses are exchangeable, possibly after inclusion of covariates, which may act at cluster- or individual-level. We develop both likelihood based and Bayesian inferences procedures, the latter utilizing MCMC techniques. Inclusion of higher order interaction terms permit examination of the complexity of the correlation structure. (c). Design and evaluation of dynamic diagnostic indices that may be used as tools for monitoring pros pectively for onset and stages of disease using accumulating serial biomarker measurements. We propose the use of hidden continuous time Markov chain models for longitudinal biomarker data and apply reversible jump MCMC methods. A particular application is to PSA as a marker for stages of prostate cancer. (d). Various other topics that arise in analyses and meta-analyses of clinical trial data.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA066218-25
Application #
6866927
Study Section
Biostatistical Methods and Research Design Study Section (BMRD)
Program Officer
Feuer, Eric J
Project Start
1995-03-01
Project End
2008-12-31
Budget Start
2005-01-17
Budget End
2005-12-31
Support Year
25
Fiscal Year
2005
Total Cost
$169,320
Indirect Cost

  Institution

Name
Cornell University
Department
Miscellaneous
Type
Schools of Engineering
DUNS #
872612445
City
Ithaca
State
NY
Country
United States
Zip Code
14850

  Publications

Wang, C; Turnbull, B W; Nielsen, S S et al. (2011) Bayesian analysis of longitudinal Johne's disease diagnostic data without a gold standard test. J Dairy Sci 94:2320-8
Jennison, Christopher; Turnbull, Bruce W (2006) Efficient group sequential designs when there are several effect sizes under consideration. Stat Med 25:917-32
Wang, C; Turnbull, B W; Grohn, Y T et al. (2006) Estimating receiver operating characteristic curves with covariates when there is no perfect reference test for diagnosis of Johne's disease. J Dairy Sci 89:3038-46
Jennison, Christopher; Turnbull, Bruce W (2005) Meta-analyses and adaptive group sequential designs in the clinical development process. J Biopharm Stat 15:537-58
Stefanescu, Catalina; Turnbull, Bruce W (2005) On the multivariate probit model for exchangeable binary data with covariates. Biom J 47:206-18
Jennison, Christopher; Turnbull, Bruce W (2003) Mid-course sample size modification in clinical trials based on the observed treatment effect. Stat Med 22:971-93
Stefanescu, Catalina; Turnbull, Bruce W (2003) Likelihood inference for exchangeable binary data with varying cluster sizes. Biometrics 59:18-24
McCulloch, C E; Lin, H; Slate, E H et al. (2002) Discovering subpopulation structure with latent class mixed models. Stat Med 21:417-29
Slate, E H; Turnbull, B W (2000) Statistical models for longitudinal biomarkers of disease onset. Stat Med 19:617-37