Literature DB >> 21497773

Germline polymorphisms discovered via a cell-based, genome-wide approach predict platinum response in head and neck cancers.

Dana Ziliak1, Peter H O'Donnell, Hae Kyung Im, Eric R Gamazon, Peixian Chen, Shannon Delaney, Sunita Shukla, Soma Das, Nancy J Cox, Everett E Vokes, Ezra E W Cohen, M Eileen Dolan, R Stephanie Huang.   

Abstract

Identifying patients prior to treatment who are more likely to benefit from chemotherapeutic agents or more likely to experience adverse events is an aim of personalized medicine. Pharmacogenomics offers a potential means of achieving this goal through the discovery of predictive germline genetic biomarkers. When applied particularly to the treatment of head and neck cancers, such information could offer significant benefit to patients as a means of potentially reducing morbidity associated with platinum-based chemotherapy. We developed a genome-wide, cell-based approach to identify single nucleotide polymorphisms (SNPs) associated with platinum susceptibility and then evaluated these SNPs as predictors for response and toxicity in head and neck cancer patients treated with platinum-based therapy as part of a phase II clinical trial. Sixty head and neck cancer patients were evaluated. Of 45 genome-wide SNPs examined, we found that 2 SNPs, rs6870861 (P=0.004; false discovery rate [FDR] <0.05) and rs2551038 (P=0.005; FDR <0.05), were associated significantly with overall response to carboplatin-based induction chemotherapy when incorporated into a model along with total carboplatin exposure. Interestingly, these 2 SNPs are associated strongly with the baseline expression of >20 genes (all P ≤10(-4)), and that 2 genes (SLC22A5 and SLCO4C1) are important organic cation/anion transporters known to affect platinum uptake and clearance. Several other SNPs were associated nominally with carboplatin-related hematologic toxicities. These findings demonstrate importantly that a genome-wide, cell-based model can identify novel germline genetic biomarkers of platinum susceptibility, which are replicable in a clinical setting with treated cancer patients and seem clinically meaningful for potentially enabling future personalization of care in such patients.
Copyright © 2011 Mosby, Inc. All rights reserved.

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Year:  2011        PMID: 21497773      PMCID: PMC3079878          DOI: 10.1016/j.trsl.2011.01.005

Source DB:  PubMed          Journal:  Transl Res        ISSN: 1878-1810            Impact factor:   7.012


  31 in total

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Authors:  David I Rosenthal; Angel I Blanco
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Review 4.  Use of CEPH and non-CEPH lymphoblast cell lines in pharmacogenetic studies.

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  32 in total

1.  Genome-wide association and pharmacological profiling of 29 anticancer agents using lymphoblastoid cell lines.

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3.  Clinical Evaluation of Cisplatin Sensitivity of Germline Polymorphisms in Neoadjuvant Chemotherapy for Urothelial Cancer.

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4.  SCAN: a systems biology approach to pharmacogenomic discovery.

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Review 5.  Relating human genetic variation to variation in drug responses.

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7.  Lymphoblastoid cell lines in pharmacogenomics: how applicable are they to clinical outcomes?

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8.  Identification of novel germline polymorphisms governing capecitabine sensitivity.

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9.  Genetic and epigenetic variants contributing to clofarabine cytotoxicity.

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Review 10.  Using germline genomics to individualize pediatric cancer treatments.

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