TY - JOUR
T1 - Characterization of a multiple epigenetic marker panel for lung cancer detection and risk assessment in plasma
AU - Hsu, Han Shui
AU - Chen, Tsz Pei
AU - Hung, Chein Hui
AU - Wen, Chiao Kai
AU - Lin, Rou Kai
AU - Lee, Hui Chen
AU - Wang, Yi Ching
PY - 2007/11/1
Y1 - 2007/11/1
N2 - BACKGROUND. Methylation patterns may be useful biomarkers of cancer detection and risk assessment. METHODS. The methylation status of 6 genes, including a candidate tumor suppressor gene (BLU), the Cadherin 13 gene (CDH13), the fragile histidine triad gene (FHIT), the cell cycle control gene p16, the retinoic acid receptor β gene (RARβ), and the Ras association domain family 1 gene (RASSF1A), was examined in plasma samples, corresponding tumor tissues, and normal lung tissues from a group of 63 patients with lung cancer and in plasma samples from 36 cancer-free individuals. The detection rate of the p16 gene was validated in a test group of 20 patients with lung cancer. RESULTS. The concordance of methylation in tumor tissues and plasma samples was 86%, 87%, 80%, 75%, 76%, and 84% for the BLU, CDH13, FHIT, p16, RARβ, and RASSF1A genes, respectively. The test group showed a similar concordance for p16 methylation detection. Multiple logistic regression analysis showed that the odds ratio for having lung cancer was 10.204 for individuals with p16 methylation (P = .013) and 9.952 for individuals with RASSFIA methylation (P = .019). After several trial tests, the authors established that methylation for ≥2 of the 6 markers met the criterion for an elevated risk of cancer. Comparisons yielded a sensitivity of 73%, a specificity of 82%, and a concordance of 75% between the methylation patterns in tumor tissues and in corresponding plasma samples. The detection rate was relatively high in cigarette smokers with advanced squamous cell lung cancer. CONCLUSIONS. The current results indicated that multiple epigenetic markers in the plasma, especially the p16 and RASSF1A genes, can be used for lung cancer detection. This methylation marker panel should improve the detection of cancer or the risk assessment for lung cancer in combination with conventional diagnostic tools.
AB - BACKGROUND. Methylation patterns may be useful biomarkers of cancer detection and risk assessment. METHODS. The methylation status of 6 genes, including a candidate tumor suppressor gene (BLU), the Cadherin 13 gene (CDH13), the fragile histidine triad gene (FHIT), the cell cycle control gene p16, the retinoic acid receptor β gene (RARβ), and the Ras association domain family 1 gene (RASSF1A), was examined in plasma samples, corresponding tumor tissues, and normal lung tissues from a group of 63 patients with lung cancer and in plasma samples from 36 cancer-free individuals. The detection rate of the p16 gene was validated in a test group of 20 patients with lung cancer. RESULTS. The concordance of methylation in tumor tissues and plasma samples was 86%, 87%, 80%, 75%, 76%, and 84% for the BLU, CDH13, FHIT, p16, RARβ, and RASSF1A genes, respectively. The test group showed a similar concordance for p16 methylation detection. Multiple logistic regression analysis showed that the odds ratio for having lung cancer was 10.204 for individuals with p16 methylation (P = .013) and 9.952 for individuals with RASSFIA methylation (P = .019). After several trial tests, the authors established that methylation for ≥2 of the 6 markers met the criterion for an elevated risk of cancer. Comparisons yielded a sensitivity of 73%, a specificity of 82%, and a concordance of 75% between the methylation patterns in tumor tissues and in corresponding plasma samples. The detection rate was relatively high in cigarette smokers with advanced squamous cell lung cancer. CONCLUSIONS. The current results indicated that multiple epigenetic markers in the plasma, especially the p16 and RASSF1A genes, can be used for lung cancer detection. This methylation marker panel should improve the detection of cancer or the risk assessment for lung cancer in combination with conventional diagnostic tools.
KW - Case-control study
KW - Methylation-specific polymerase chain reaction
KW - Nonsmall cell lung cancer
KW - Plasma
KW - Tumor suppressor gene
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U2 - 10.1002/cncr.23001
DO - 10.1002/cncr.23001
M3 - Article
C2 - 17876837
AN - SCOPUS:35648953334
SN - 0008-543X
VL - 110
SP - 2019
EP - 2026
JO - Cancer
JF - Cancer
IS - 9
ER -