A pharmacogenetic study of docetaxel and thalidomide in patients with androgen-independent prostate cancer (AIPC) using targeted human DMET genotyping platform.

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Abstracts

2007 ASCO Annual Meeting

A pharmacogenetic study of docetaxel and thalidomide in patients with androgen-independent prostate cancer (AIPC) using targeted human DMET genotyping platform.

Sub-category:

Pharmacogenomics

Category:

Developmental Therapeutics: Molecular Therapeutics

Meeting:

2007 ASCO Annual Meeting

Session Type and Session Title:

General Poster Session, Developmental Therapeutics: Molecular Therapeutics

Abstract No:

3580

Citation:

Journal of Clinical Oncology, 2007 ASCO Annual Meeting Proceedings Part I. Vol 25, No. 18S (June 20 Supplement), 2007: 3580

Author(s):

J. F. Deeken, T. Cormier, D. K. Price, S. Steinberg, K. Tran, D. J. Liewehr, S. B. Ockers, P. Hardenbol, W. Dahut, X. Miao, W. D. Figg

Abstract:

Background: Pharmacogenetic research holds the promise of individualizing cancer therapy by reducing inter-individual variability in drug response, thus enhancing efficacy and reducing toxicity. Past research has been limited due to the lack of a robust genotyping platform that can screen for single nucleotide polymorphisms (SNPs) in the dozens of genes known to be involved in drug disposition. We pilot tested the new Affymetrix Targeted Human Drug Metabolizing Enzymes and Transporter (DMET) 1.0 panel in an exploratory study of docetaxel and thalidomide. The DMET 1.0 panel tests for 1,229 genetic variations in 169 drug disposition genes, including 49 CYP450 genes, 73 non-CYP genes, and 47 transporters. Methods: DNA samples from 47 patients with AIPC enrolled in a randomized phase II trial using docetaxel and thalidomide vs. docetaxel alone were genotyped using the DMET 1.0 panel. Patients' response was determined using RECIST criteria. Toxicities were graded using the NCI-CTC, and patients were identified if they experienced grade 3 or 4 toxicity. Given the distinct side effect profiles of these two drugs, specific toxicities were assigned as being due to either docetaxel or thalidomide. An association between the SNP parameters and clinical response or toxicity was tested using Mehta's modification to Fisher's exact test. Reported results were limited to those where p<0.01. Results: Six SNPs in three genes were associated with response to therapy: PPAR-delta (p=0.0011), SULT1C2 (p=0.0083), and CHST3 (4 SNPs, p=0.0001 to 0.0034). For toxicities associated with docetaxel, five SNPs in three genes were identified: UGT1A1 (2 SNPs, p=0.0009 to 0.0094), UGT1A9 (2 SNPs, p=0.0016 to 0.0096), and CYP2A7 (p=0.0027). SNPs in CYP2B6 (p=0.0033), ABCC1 (p=0.0036), and ABCC6 (p=0.0075) were associated with toxicities from thalidomide. Conclusion: We identified nine genes in which SNPs were potentially significantly associated with clinical response and toxicity to treatment. These results highlight the important role that non-CYP450 and phase II drug metabolizing enzymes may play in the efficacy and disposition of docetaxel and thalidomide. Confirmatory studies are warranted.

Abstract Disclosures

Abstracts that were granted an exception in accordance with ASCO's Conflict of Interest Policy and are designated with a caret symbol (^) here and in the print version.

Associated Presentation(s):

1. A pharmacogenetic study of docetaxel and thalidomide in patients with androgen-independent prostate cancer (AIPC) using targeted human DMET genotyping platform.

Meeting: 2007 ASCO Annual Meeting
Presenter: John F Deeken, MD
Session: Developmental Therapeutics: Molecular Therapeutics (General Poster Session)

Other Abstracts in this Sub-Category:

		1. Identification of sensitivity markers for BMS-536924, an inhibitor for insulin-like growth factor-1 receptor. Meeting: 2007 ASCO Annual Meeting Abstract No: 3506 First Author: F. Huang Category: Developmental Therapeutics: Molecular Therapeutics - Pharmacogenomics
		2. Identification of predictive and surrogate molecular markers for dasatinib in prostate cancer: Rationale for patient selection and efficacy monitoring. Meeting: 2007 ASCO Annual Meeting Abstract No: 3579 First Author: X. Wang Category: Developmental Therapeutics: Molecular Therapeutics - Pharmacogenomics
		3. Pharmacogenetic prediction for tumor response, toxicity, and survival of NSCLC patients treated with irinotecan and cisplatin chemotherapy. Meeting: 2007 ASCO Annual Meeting Abstract No: 3581 First Author: J. Han Category: Developmental Therapeutics: Molecular Therapeutics - Pharmacogenomics
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Abstracts by J. F. Deeken:

		1. Efficacy of combining targeted therapies cetuximab and dasatinib for resistant salivary gland carcinomas in vitro. Meeting: 2010 ASCO Annual Meeting Abstract No: 5557 First Author: A. Brohl Category: Head and Neck Cancer
		2. Final reporting of a phase I clinical trial of the oral PPAR-gamma agonist, CS-7017, in patients with advanced malignancies. Meeting: 2010 ASCO Annual Meeting Abstract No: 2526 First Author: M. J. Pishvaian Category: Developmental Therapeutics - Clinical Pharmacology and Immunotherapy - Phase I Studies
		3. Improved outcomes in HPV+ versus HPV- locally advanced head and neck squamous cell carcinoma (LAH&NSCC) when treated with cetuximab and concurrent radiation. Meeting: 2010 ASCO Annual Meeting Abstract No: e16023 First Author: M. Howard Category: Head and Neck Cancer
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Presentations by J. F. Deeken:

		1. Treating HIV+ patients for non-AIDS-defining cancers (NADCs) in the era of targeted chemotherapy: An AIDS malignancy consortium study of sunitinib in patients on ART. Meeting: 2010 ASCO Annual Meeting Presenter: John F. Deeken Session: Trials in Progress Poster Session (Trials in Progress Poster Session)
		2. A pharmacogenetic study of docetaxel and thalidomide in patients with androgen-independent prostate cancer (AIPC) using targeted human DMET genotyping platform. Meeting: 2007 ASCO Annual Meeting Presenter: John F Deeken, MD Session: Developmental Therapeutics: Molecular Therapeutics (General Poster Session)
		3. Identification of novel single nucleotide polymorphisms (SNPs) associated with risk and prognosis in patients with androgen independent prostate cancer (AIPC) using a new genotyping platform, the affymetrix DME-T panel. Meeting: 2007 Prostate Cancer Symposium Presenter: John F Deeken, MD Session: General Poster Session A (General Poster Session)
		More...

Educational Book Manuscripts by J. F. Deeken:

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