Abstract

Mortality from lung cancer could be reduced through implementation of chemopreventive strategies to reverse or impede progression of premalignant disease. Ingestion of L-selenomethionine has been associated with a 50% decrease in expected rates of lung cancer. ECOG 5597, """"""""A Phase III Chemoprevention Trial of Selenium Supplementation in Persons with Resected Stage I Non-Small Cell Lung Cancer (NSCLC),"""""""" will test the hypothesis that selenium can decrease the rate of second primary tumors in patients who have undergone surgery for stage I NSCLC. Selenium may prevent lung cancer by protecting tissue from oxidative damage, inducing apoptosis of premalignant cells, and/or by acting as a demethylating agent through inhibition of cytosine DNA- methyltransferase. The identification of biomarkers that predict the efficacy of selenium would aid in the validation of this agent as a chemopreventive. We have targeted genes inactivated by CpG island methylation as candidate biomarkers and demonstrated that aberrant methylation of the p16 and O6-methylguanine-DNA methyltransferase (MGMT) promoters can be detected in DNA from sputum in 100% of patients with squamous cell carcinoma up to 3 y before clinical diagnosis. Moreover, the prevalence of these markers in sputum from cancer-free, high-risk subjects approximates lifetime risk for lung cancer. Additional studies indicate that adenocarcinoma can also be detected through analysis of these and other genes in sputum and/or plasma. We have now extended these studies to begin developing a panel of methylation markers for predicting the development of lung cancer. In this study of sputum samples from 25 incident lung cancer cases and 25 matched controls, the presence of any of the four methylation markers examined was associated with a 6.3-fold increase in the risk for lung cancer. Thus, the use of aberrant gene methylation as a molecular marker system represents a powerful approach to evaluate the efficacy of selenium intervention. Using longitudinal collected sputum and plasma from subjects enrolled on ECOG 5597, we will first determine the prevalence for methylation of p16, MGMT, and death associated protein kinase after tumor resection. People positive for the methylation markers will be followed to determine how the methylation profile changes during intake of selenium versus placebo. Second, a nested, case-control study will determine whether changes in promoter hypermethylation predict development of a second primary lung cancer. These laboratory studies will specifically address mechanisms by which selenium is proposed to exert its chemopreventive effect. Our findings could identify molecular markers to monitor the [efficacy of selenium supplementation in future prevention trials in cancer-free subiects with a history of smoking.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA095568-05
Application #
7168840
Study Section
Clinical Oncology Study Section (CONC)
Program Officer
Kagan, Jacob
Project Start
2003-02-05
Project End
2008-02-25
Budget Start
2007-02-01
Budget End
2008-02-25
Support Year
5
Fiscal Year
2007
Total Cost
$655,631
Indirect Cost

  Institution

Name
Lovelace Biomedical & Environmental Research
Department
Type
DUNS #
045911138
City
Albuquerque
State
NM
Country
United States
Zip Code
87108

  Publications

Belinsky, Steven A; Leng, Shuguang; Wu, Guodong et al. (2017) Gene Methylation Biomarkers in Sputum and Plasma as Predictors for Lung Cancer Recurrence. Cancer Prev Res (Phila) 10:635-640
Leng, Shuguang; Wu, Guodong; Klinge, Donna M et al. (2017) Gene methylation biomarkers in sputum as a classifier for lung cancer risk. Oncotarget 8:63978-63985
Belinsky, Steven A (2015) Unmasking the lung cancer epigenome. Annu Rev Physiol 77:453-74
Tessema, Mathewos; Yingling, Christin M; Liu, Yushi et al. (2014) Genome-wide unmasking of epigenetically silenced genes in lung adenocarcinoma from smokers and never smokers. Carcinogenesis 35:1248-57
Tessema, Mathewos; Yingling, Christin M; Snider, Amanda M et al. (2014) GATA2 is epigenetically repressed in human and mouse lung tumors and is not requisite for survival of KRAS mutant lung cancer. J Thorac Oncol 9:784-93
Belinsky, Steven A; Grimes, Marcie J; Picchi, Maria A et al. (2011) Combination therapy with vidaza and entinostat suppresses tumor growth and reprograms the epigenome in an orthotopic lung cancer model. Cancer Res 71:454-62
Lyon, Christopher M; Klinge, Donna M; Do, Kieu C et al. (2009) Rosiglitazone prevents the progression of preinvasive lung cancer in a murine model. Carcinogenesis 30:2095-9
Belinsky, Steven A; Schiller, Joan H; Stidley, Christine A (2008) DNA methylation biomarkers to assess therapy and chemoprevention for non-small cell lung cancer. Nutr Rev 66 Suppl 1:S24-6
Ju, Wei; Wang, Xia; Shi, Honglian et al. (2007) A critical role of luteolin-induced reactive oxygen species in blockage of tumor necrosis factor-activated nuclear factor-kappaB pathway and sensitization of apoptosis in lung cancer cells. Mol Pharmacol 71:1381-8
Vuillemenot, Brian R; Hutt, Julie A; Belinsky, Steven A (2006) Gene promoter hypermethylation in mouse lung tumors. Mol Cancer Res 4:267-73

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