Publication

Global Assessment of Genetic Variation Influencing Response to Retinoid Chemoprevention in Head and Neck Cancer Patients

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Last modified
  • 05/20/2025
Type of Material
Authors
    J. Jack Lee, University of Texas MD Anderson Cancer CenterXifeng Wu, University of Texas MD Anderson Cancer CenterMichelle A. T. Hildebrandt, University of Texas MD Anderson Cancer CenterrHushan Yang, University of Texas MD Anderson Cancer CenterFadlo Khuri, Emory UniversityEdward Kim, University of Texas MD Anderson Cancer CenterJian Gu, University of Texas MD Anderson Cancer CenterYuanqing Ye, University of Texas MD Anderson Cancer CenterReuben Lotan, University of Texas MD Anderson Cancer CenterMargaret R. Spitz, University of Texas MD Anderson Cancer CenterWaun Ki Hong, University of Texas MD Anderson Cancer Center
Language
  • English
Date
  • 2011-02-01
Publisher
  • American Association for Cancer Research
Publication Version
Copyright Statement
  • ©2011 AACR.
Final Published Version (URL)
Title of Journal or Parent Work
ISSN
  • 1940-6207
Volume
  • 4
Issue
  • 2
Start Page
  • 185
End Page
  • 193
Grant/Funding Information
  • Grant Support: NIH grants CA52051 (WKH); CA97007 (WKH); CA106541 (XW); and CA86390 (MRS).
Supplemental Material (URL)
Abstract
  • Head and neck squamous cell carcinoma (HNSCC) patients are at an increased risk of developing a second primary tumor (SPT) or recurrence following curative treatment. 13-cis-retinoic acid (13-cRA) has been tested in chemoprevention clinical trials, but the results have been inconclusive. We genotyped 9,465 single nucleotide polymorphisms (SNP) in 450 patients fromthe Retinoid Head and Neck Second Primary Trial. SNPs were analyzed for associations with SPT/recurrence in patients receiving placebo to identify prognosis markers and further analyzed for effects of 13-cRA in patients with these prognostic loci. Thirteen loci identified a majority subgroup of patients at a high risk of SPT/recurrence and in whom 13-cRA was protective. Patients carrying the common genotype of rs3118570 in the retinoid X receptor (RXRA) were at a 3.33-fold increased risk (95% CI, 1.67-6.67) and represented more than 70% of the study population. This locus also identified individuals who received benefit from chemoprevention with a 38% reduced risk (95% CI, 0.43-0.90). Analyses of cumulative effect and potential gene-gene interactions also implicated CDC25C:rs6596428 and JAK2:rs1887427 as 2 other genetic loci with major roles in prognosis and 13-cRA response. Patients with all 3 common genotypes had a 76% reduction in SPT/recurrence (95% CI, 0.093-0.64) following 13-cRA chemoprevention. Carriers of these common genotypes constituted a substantial percentage of the study population, indicating that a pharmacogenetic approach could help select patients for 13-cRA chemoprevention. The lack of any alternatives for reducing risk in these patients highlights the need for future clinical trials to prospectively validate our findings.
Author Notes
  • Waun Ki Hong, Department of Thoracic/Head and Neck Medical Oncology, The University of Texas MD Anderson Cancer Center, Houston, TX 77030, Phone: 713-792-7770, FAX: 713-404-9696, whong@mdanderson.org.
Keywords
Research Categories
  • Biology, Genetics
  • Health Sciences, Oncology
  • Health Sciences, Epidemiology

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