Abstract

Randomized clinical trials are and will continue to be the key vehicle for evaluation of new and existing cancer therapies. This revolutionary era of advances in the biological sciences is leading to the discovery of novel biomarkers and complex genetic and genomic information that may be highly associated with various clinical outcomes, offering the tantalizing opportunity to exploit this information to both improve the precision of the analyses of trials and to develop models of longitudinal disease progression that may reveal important insights. A recurrent challenge is that missing data and subject drop-out are commonplace, presenting complications for analyses of these trials. Through a series of aims addressing these issues, this project proposes research that will have a significant impact on the quality and strength of inferences possible from current cancer clinical trials. That it is possible to improve efficiency of primary analyses of clinical trials by exploiting prognostic baseline auxiliary information is well known;however, such analyses are controversial because of the temptation to choose the analysis that leads to the most dramatic treatment effect. In the first aim, new methods for such """"""""covariate adjustment"""""""" will be studied that circumvent this issue and can improve over existing approaches. In the second aim, these methods will be extended so that they may be used in the common case where outcomes are missing due to drop-out. Efficient methods for longitudinal analysis of measures such as quality of life and biomarkers in the presence of drop-out will also be developed. Understanding the relationship between such longitudinal measures and clinical outcomes such as time to recurrence or survival time is of key importance.
The third aim focuses on development of methods for assessing the correctness of so-called joint statistical models used for this purpose and for assessing the influence of particular observations on the fit ofthe model, where the data used to develop the model may be missing. Finally, taking appropriate account of missing data sometimes requires unverifiable assumptions about why the data are missing, which are incorporated in models that thus cannot be checked based on the data.
The fourth aim i s devoted to development of a new statistical framework for assessing how sensitive conclusions are to the modeling assumptions made.

Public Health Relevance

Randomized clinical trials in cancer research are the most important mechanism for the evaluation of new and existing therapies. Statistical methods will be developed that will improve the precision of the analyses of these trials and provide tools for drawing valid conclusions when some of the data intended to be collected are missing, e.g., if some subjects drop out ofthe trial, offering cancer researchers an expanded set of tools that will greatly improve the quality and strength of analyses of current cancer clinical trials.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA142538-03
Application #
8375169
Study Section
Special Emphasis Panel (ZCA1-RPRB-7)
Project Start
Project End
Budget Start
2012-04-25
Budget End
2013-03-31
Support Year
3
Fiscal Year
2012
Total Cost
$269,750
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Type
DUNS #
608195277
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Yang, Shu; Tsiatis, Anastasios A; Blazing, Michael (2018) Modeling survival distribution as a function of time to treatment discontinuation: A dynamic treatment regime approach. Biometrics 74:900-909
Chen, Jingxiang; Zhang, Chong; Kosorok, Michael R et al. (2018) Double Sparsity Kernel Learning with Automatic Variable Selection and Data Extraction. Stat Interface 11:401-420
Kang, Suhyun; Lu, Wenbin; Zhang, Jiajia (2018) ON ESTIMATION OF THE OPTIMAL TREATMENT REGIME WITH THE ADDITIVE HAZARDS MODEL. Stat Sin 28:1539-1560
Maity, Arnab; Zhao, Jing; Sullivan, Patrick F et al. (2018) Inference on phenotype-specific effects of genes using multivariate kernel machine regression. Genet Epidemiol 42:64-79
Sibley, Alexander; Li, Zhiguo; Jiang, Yu et al. (2018) Facilitating the Calculation of the Efficient Score Using Symbolic Computing. Am Stat 72:199-205
Liu, Ying; Wang, Yuanjia; Kosorok, Michael R et al. (2018) Augmented outcome-weighted learning for estimating optimal dynamic treatment regimens. Stat Med 37:3776-3788
Wong, Kin Yau; Zeng, Donglin; Lin, D Y (2018) Efficient Estimation for Semiparametric Structural Equation Models With Censored Data. J Am Stat Assoc 113:893-905
Zhou, Jie; Zhang, Jiajia; Lu, Wenbin (2018) Computationally Efficient Estimation for the Generalized Odds Rate Mixture Cure Model with Interval-Censored Data. J Comput Graph Stat 27:48-58
Butler, Emily L; Laber, Eric B; Davis, Sonia M et al. (2018) Incorporating Patient Preferences into Estimation of Optimal Individualized Treatment Rules. Biometrics 74:18-26
Li, Zhiguo; Wang, Xiaofei; Wu, Yuan et al. (2018) Sample size calculation for studies with grouped survival data. Stat Med 37:3904-3917

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