Abstract

The successful application of pharmacogenetics requires a full understanding of the expression of genotype as phenotype. A large number of genes code for proteins that mediate response to medicines, and while it is clear that variations in one gene can alter the clinical response to a medicine significantly, this is rare. We propose to study multiple genetic influences on the clinical pharmacology of an important drug: tamoxifen. Our goal is to define multiple genetic influences on the action of this drug as a model for many other drugs, where multiple genetic variations are likely to alter pharmacologic responses. An interdisciplinary group of investigators will use a pharmacogenetic and analytical core laboratory and the resources of the Lombardi Cancer Center to study genetic influences on the metabolism, pharmacokinetics, efficacy and toxicity of tamoxifen. While tamoxifen has been shown to be metabolized by genetically polymorphic cytochrome P450 enzymes in human liver microsomes in vitro, the hypothesis that mutations in the genes coding for these enzymes might alter the drug's metabolism, effects or toxicity has never been tested in vivo, either in normal volunteers or in women with breast cancer. We have the following specific goals: 1) Determine the variability in the contributions of three genetically polymorphic enzymes (CYP2C9, CYP2D6 and CYP3A) to tamoxifen metabolism in human liver microsomes and in isolated human hepatocytes; 2) Test the hypothesis that CYP2D6, CYP3A or CYP2C9 genetics alter the pharmacokinetics of tamoxifen and its metabolites in a clinical trial in patients being prescribed tamoxifen as an adjuvant; 3) Test the hypothesis that metabolic pharmacogenetics influence the efficacy of tamoxifen through analysis of tamoxifen concentrations and metabolic genotypes in patients enrolled in the NSABP-P1 trial: a comparison of the preventive efficacy of tamoxifen and placebo; and 4) Test the hypothesis that genetics alter the toxicity of tamoxifen by A) testing the hypothesis that genetic polymorphisms that influence the metabolism of tamoxifen change the incidence of hot flashes that occur after administration of the drug., and B) testing whether the adverse effects of tamoxifen on cardiac QT interval are influenced by genetic polymorphisms in metabolism and/or ion channels. The multiple pharmacogenetic influences on these measures of tamoxifen effect will be analyzed to determine the pharmacogenetic profile of subjects most likely to experience efficacy, or to experience adverse effects from tamoxifen.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project--Cooperative Agreements (U01)
Project #
1U01GM061373-01
Application #
6132621
Study Section
Special Emphasis Panel (ZRG1-MGN (01))
Program Officer
Long, Rochelle M
Project Start
2000-05-01
Project End
2001-07-31
Budget Start
2000-05-01
Budget End
2001-07-31
Support Year
1
Fiscal Year
2000
Total Cost
$1,249,122
Indirect Cost

  Institution

Name
Georgetown University
Department
Pharmacology
Type
Schools of Medicine
DUNS #
049515844
City
Washington
State
DC
Country
United States
Zip Code
20057

  Publications

Robarge, Jason D; Desta, Zereunesay; Nguyen, Anne T et al. (2017) Effects of exemestane and letrozole therapy on plasma concentrations of estrogens in a randomized trial of postmenopausal women with breast cancer. Breast Cancer Res Treat 161:453-461
Hertz, Daniel L; Speth, Kelly A; Kidwell, Kelley M et al. (2017) Variable aromatase inhibitor plasma concentrations do not correlate with circulating estrogen concentrations in post-menopausal breast cancer patients. Breast Cancer Res Treat 165:659-668
Hertz, D L; Kidwell, K M; Seewald, N J et al. (2017) Polymorphisms in drug-metabolizing enzymes and steady-state exemestane concentration in postmenopausal patients with breast cancer. Pharmacogenomics J 17:521-527
Kadakia, Kunal C; Kidwell, Kelley M; Seewald, Nicholas J et al. (2017) Prospective assessment of patient-reported outcomes and estradiol and drug concentrations in patients experiencing toxicity from adjuvant aromatase inhibitors. Breast Cancer Res Treat 164:411-419
Marcath, Lauren A; Deal, Allison M; Van Wieren, Emily et al. (2017) Comprehensive assessment of cytochromes P450 and transporter genetics with endoxifen concentration during tamoxifen treatment. Pharmacogenet Genomics 27:402-409
Hertz, Daniel L; Deal, Allison; Ibrahim, Joseph G et al. (2016) Tamoxifen Dose Escalation in Patients With Diminished CYP2D6 Activity Normalizes Endoxifen Concentrations Without Increasing Toxicity. Oncologist 21:795-803
Santa-Maria, Cesar A; Blackford, Amanda; Nguyen, Anne T et al. (2016) Association of Variants in Candidate Genes with Lipid Profiles in Women with Early Breast Cancer on Adjuvant Aromatase Inhibitor Therapy. Clin Cancer Res 22:1395-402
Kadakia, Kunal C; Snyder, Claire F; Kidwell, Kelley M et al. (2016) Patient-Reported Outcomes and Early Discontinuation in Aromatase Inhibitor-Treated Postmenopausal Women With Early Stage Breast Cancer. Oncologist 21:539-46
Oesterreich, Steffi; Henry, N Lynn; Kidwell, Kelley M et al. (2015) Associations between genetic variants and the effect of letrozole and exemestane on bone mass and bone turnover. Breast Cancer Res Treat 154:263-73
Ingle, James N; Kalari, Krishna R; Buzdar, Aman U et al. (2015) Estrogens and their precursors in postmenopausal women with early breast cancer receiving anastrozole. Steroids 99:32-8

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