Abstract

Biomarkers in cancer research are considered a central component of the expected improvements in prevention, detection, treatment and monitoring. There are potentially useful in many different types of studies and for many different purposes. Critical questions are whether they are valid to use, how can they be utilized in a valid and efficient way, and then if they are used how confident is one in the conclusions that are obtained. The use of biomarkers to advance understanding in cancer science has great potential, but also has some risks. Biomarkers are subject to uncertainty in their measurement, they may not be measuring exactly the quantity of interest, and since they are not explicitly measures of symptoms their use to aid in decision making or evaluation of therapies in a clinical setting is subject to uncertainty. Thus careful analysis of data from studies that involve biomarkers is crucial. There are many statistical challenges that arise in such studies. This application is concerned with developing, evaluating and applying statistical methods for data that involves biomarkers.
The first aim i s concerned with adding biomarkers to prediction models that may be used to stratify or classify patients. In this aim we develop approaches for integrating data from other sources to improve the prediction models. This research will have broad applicability. Innovative aspects involve the use of targeted ridge regression, multi-kernel machine modeling, and importance sampling to incorporate information from the literature.
The second aim i s concerned with clinical trials where the biomarker is to be used to evaluate a therapy as a surrogate endpoint. Because of the nature of the scientific question causal modeling is very natural in this context. We propose to develop both potential outcomes and structural causal models. We will investigate both single trial and multi trial settings with different endpoint types.
The third aim i s concerned with therapies that may be effective only for a subgroup of patients, and to be useful this subgroup is determined by a small number of predictive biomarkers. For data from randomized clinical trials we suggest a unified modeling approach, and will investigate the use of single index models with variable selection and multivariate partial least squares to aid in the subgroup identification. Inference following subgroup identification is challenging, we suggest an innovative scheme to simulate data under an appropriate null distribution. All 3 aims in this proposal address fundamental and significant problems in translational oncology research. Successful completion of the aims will have an impact both in understanding and utilizing biomarkers and also in developing statistical methodology that can be more broadly applicable to other fields.

Public Health Relevance

Biomarkers are considered a central component of the expected improvements in prevention, detection, treatment and monitoring in cancer. Critical questions about biomarkers are when and whether they are valid to use, how can they be utilized in a valid and efficient way, and then if they are used how confident is one in the conclusions that are obtained. This proposal is concerned with developing proper and efficient statistical methods for evaluation of biomarker data.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA129102-06
Application #
8603224
Study Section
Cancer Biomarkers Study Section (CBSS)
Program Officer
Feuer, Eric J
Project Start
2007-07-01
Project End
2015-12-31
Budget Start
2014-01-01
Budget End
2014-12-31
Support Year
6
Fiscal Year
2014
Total Cost
$224,677
Indirect Cost
$63,964

  Institution

Name
University of Michigan Ann Arbor
Department
Biostatistics & Other Math Sci
Type
Schools of Public Health
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Shen, Jincheng; Wang, Lu; Daignault, Stephanie et al. (2018) Estimating the Optimal Personalized Treatment Strategy Based on Selected Variables to Prolong Survival via Random Survival Forest with Weighted Bootstrap. J Biopharm Stat 28:362-381
Schmitd, Ligia B; Beesley, Lauren J; Russo, Nickole et al. (2018) Redefining Perineural Invasion: Integration of Biology With Clinical Outcome. Neoplasia 20:657-667
Cho, Youngjoo; Hu, Chen; Ghosh, Debashis (2018) Covariate adjustment using propensity scores for dependent censoring problems in the accelerated failure time model. Stat Med 37:390-404
Manohar, Poorni M; Beesley, Lauren J; Bellile, Emily L et al. (2018) Prognostic Value of FDG-PET/CT Metabolic Parameters in Metastatic Radioiodine-Refractory Differentiated Thyroid Cancer. Clin Nucl Med 43:641-647
Cheng, Wenting; Taylor, Jeremy M G; Vokonas, Pantel S et al. (2018) Improving estimation and prediction in linear regression incorporating external information from an established reduced model. Stat Med 37:1515-1530
Boonstra, Philip S; Barbaro, Ryan P (2018) Incorporating historical models with adaptive Bayesian updates. Biostatistics :
Shen, Jincheng; Wang, Lu; Taylor, Jeremy M G (2017) Estimation of the optimal regime in treatment of prostate cancer recurrence from observational data using flexible weighting models. Biometrics 73:635-645
Suresh, Krithika; Taylor, Jeremy M G; Spratt, Daniel E et al. (2017) Comparison of joint modeling and landmarking for dynamic prediction under an illness-death model. Biom J 59:1277-1300
Conlon, Asc; Taylor, Jmg; Elliott, M R (2017) Surrogacy assessment using principal stratification and a Gaussian copula model. Stat Methods Med Res 26:88-107
Conlon, Anna; Taylor, Jeremy; Li, Yun et al. (2017) Links between causal effects and causal association for surrogacy evaluation in a gaussian setting. Stat Med 36:4243-4265

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