Abstract

The primary aim of this proposal is to create a Research Group focused on the pharmacogenetics of anticancer agents (PAAR Group). The PAAR Group includes investigators from the University of Chicago (UC), St. Jude Children's Research Hospital (SJCRH), Tulane University, and the University of Pittsburgh. The PAAR Group will be chaired by Mark Ratain, Chairman, Committee on Clinical Pharmacology at UC, and a medical oncologist. The Vice-Chair will be Mary Relling, a molecular and clinical pharmacologist at SJCRH. The Group will be governed by an Executive Committee of six senior investigators. The scope of the Group's activities will include both pharmacokinetic and pharmacodynamic polymorphisms affecting response to anticancer agents.
The aims of the proposal are: 1) To create a mulitdisciplinary, collaborative, and comprehensive Pharmacogenetics of Anticancer Agents Research Group (PAAR Group) with the capabilities to identify and evaluate polymorphisms in drug metabolizing enzymes, transporters, or targets relevant to anticancer agents. 2) To identify new polymorphisms in drug metabolizing enzymes, transporters, or targets relevant to anticancer agents. 3) To determine the association between new and previously identified polymorphisms (genotype) and variability in toxicity and/or response to anticancer agents (phenotype). 4) To define the population diversity of polymorphisms of clinical interest. 5) To create shared resources of value to other Research Groups in the Pharmacogenetic Research Network. The initial focus of the Group's activities will be on a class of drugs called topoisomerase inhibitors, widely used in both hematologic malignancies and solid tumors. The Group will utilize a consistent general research scheme, including four decision levels. Projects will require approval by the Executive Committee to progress to the next decision level. These levels are: DL1, evaluation of phenotypic variability; DL2, evaluation of genotypic variability and collection of preliminary data to support genotypic-phenotypic concordance; DL3, demonstration in preclinical model of genotypic-phenotypic concordance; DL4, prospective clinical studies of genotypic-phenotypic concordance and population diversity studies. The Group proposes four projects for the first year, involving UGT (DL4), CYP3A4 (DL4), carboxylesterases (DL1), and MLL (a gene involved in topoisomerase inhibitor-induced leukemogenesis) (DL2). A fifth project evaluating cellular susceptibility to topoisomerase inhibitors (DL1) will begin in year 2. Three core facilities are proposed: Molecular Genetics (includes sub-Core focused on gene array technology at Tulane), Liver Bank (includes sub-Core to acquire livers at Pittsburgh), and Lymphoblastoid Cell Line. The Group investigators will interact extensively in most of the proposed projects and core facilities. The PAAR Group will participate in the NIGMS Pharmacogenetic Research Network, and agrees to abide by the recommendations of the Network Steering Committee. The PAAR Group will maintain a pharmacogenetic database, and release its data to the Network Database Group on request.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01GM061393-04
Application #
6636468
Study Section
Special Emphasis Panel (ZRG1-MGN (01))
Program Officer
Long, Rochelle M
Project Start
2000-04-01
Project End
2005-03-31
Budget Start
2003-04-01
Budget End
2004-03-31
Support Year
4
Fiscal Year
2003
Total Cost
$3,043,577
Indirect Cost

  Institution

Name
University of Chicago
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
005421136
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Zhou, Shuqin; Skaar, Debra J; Jacobson, Pamala A et al. (2018) Pharmacogenomics of Medications Commonly Used in the Intensive Care Unit. Front Pharmacol 9:1436
House, Larry; Seminerio, Michael J; Mirkov, Snezana et al. (2018) Metabolism of megestrol acetate in vitro and the role of oxidative metabolites. Xenobiotica 48:973-983
Gamazon, Eric R; Trendowski, Matthew R; Wen, Yujia et al. (2018) Gene and MicroRNA Perturbations of Cellular Response to Pemetrexed Implicate Biological Networks and Enable Imputation of Response in Lung Adenocarcinoma. Sci Rep 8:733
Li, M; Seiser, E L; Baldwin, R M et al. (2018) ABC transporter polymorphisms are associated with irinotecan pharmacokinetics and neutropenia. Pharmacogenomics J 18:35-42
Geeleher, Paul; Nath, Aritro; Wang, Fan et al. (2018) Cancer expression quantitative trait loci (eQTLs) can be determined from heterogeneous tumor gene expression data by modeling variation in tumor purity. Genome Biol 19:130
Wing, Claudia; Komatsu, Masaaki; Delaney, Shannon M et al. (2017) Application of stem cell derived neuronal cells to evaluate neurotoxic chemotherapy. Stem Cell Res 22:79-88
Rudin, Shoshana; Marable, Marcus; Huang, R Stephanie (2017) The Promise of Pharmacogenomics in Reducing Toxicity During Acute Lymphoblastic Leukemia Maintenance Treatment. Genomics Proteomics Bioinformatics 15:82-93
Geeleher, Paul; Huang, R Stephanie (2017) Exploring the Link between the Germline and Somatic Genome in Cancer. Cancer Discov 7:354-355
Geeleher, Paul; Zhang, Zhenyu; Wang, Fan et al. (2017) Discovering novel pharmacogenomic biomarkers by imputing drug response in cancer patients from large genomics studies. Genome Res 27:1743-1751
Eadon, Michael T; Hause, Ronald J; Stark, Amy L et al. (2017) Genetic Variants Contributing to Colistin Cytotoxicity: Identification of TGIF1 and HOXD10 Using a Population Genomics Approach. Int J Mol Sci 18:

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