A multicenter, double-blinded validation study of methylation biomarkers for progression prediction in Barrett's esophagus

Zhe Jin; Yulan Cheng; Wen Gu; Yingye Zheng; Fumiaki Sato; Yuriko Mori; Alexandru V. Olaru; Bogdan C. Paun; Jian Yang; Takatsugu Kan; Tetsuo Ito; James P. Hamilton; Florin M. Selaru; Rachana Agarwal; Stefan David; John M. Abraham; Herbert C. Wolfsen; Michael B. Wallace; Nicholas J. Shaheen; Kay Washington; Jean Wang; Marcia Irene Canto; Achyut Bhattacharyya; Mark A. Nelson; Paul D. Wagner; Yvonne Romero; Kenneth K. Wang; Ziding Feng; Richard E. Sampliner; Stephen J. Meltzer

doi:10.1158/0008-5472.CAN-09-0028

A multicenter, double-blinded validation study of methylation biomarkers for progression prediction in Barrett's esophagus

Zhe Jin, Yulan Cheng, Wen Gu, Yingye Zheng, Fumiaki Sato, Yuriko Mori, Alexandru V. Olaru, Bogdan C. Paun, Jian Yang, Takatsugu Kan, Tetsuo Ito, James P. Hamilton, Florin M. Selaru, Rachana Agarwal, Stefan David, John M. Abraham, Herbert C. Wolfsen, Michael B. Wallace, Nicholas J. Shaheen, Kay WashingtonJean Wang, Marcia Irene Canto, Achyut Bhattacharyya, Mark A. Nelson, Paul D. Wagner, Yvonne Romero, Kenneth K. Wang, Ziding Feng, Richard E. Sampliner, Stephen J. Meltzer

School of Medicine

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156 Scopus citations

Abstract

Esophageal adenocarcinoma risk in Barrett's esophagus (BE) is increased 30- to 125-fold versus the general population. Among all BE patients, however, neoplastic progression occurs only once per 200 patient-years. Molecular biomarkers are therefore needed to risk-stratify patients for more efficient surveillance endoscopy and to improve the early detection of progression. We therefore performed a retrospective, multicenter, double-blinded validation study of eight BE progression prediction methylation biomarkers. Progression or nonprogression were determined at 2 years (tier 1) and 4 years (tier 2). Methylation was assayed in 145 nonprogressors and 50 progressors using real-time quantitative methylationspecific PCR. Progressors were significantly older than nonprogressors (70.6 versus 62.5 years; P < 0.001). We evaluated a linear combination of the eight markers, using coefficients from a multivariate logistic regression analysis. Areas under the ROC curve (AUC) were high in the 2-year, 4-year, and combined data models (0.843, 0.829, and 0.840; P < 0.001, <0.001, and <0.001, respectively). In addition, even after rigorous overfitting correction, the incremental AUCs contributed by panels based on the 8 markers plus age versus age alone were substantial (Δ-AUC = 0.152, 0.114, and 0.118, respectively) in all 3 models. A methylation biomarker-based panel to predict neoplastic progression in BE has potential clinical value in improving both the efficiency of surveillance endoscopy and the early detection of neoplasia.

Original language	English (US)
Pages (from-to)	4112-4115
Number of pages	4
Journal	Cancer Research
Volume	69
Issue number	10
DOIs	https://doi.org/10.1158/0008-5472.CAN-09-0028
State	Published - May 15 2009

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/0008-5472.CAN-09-0028

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Jin, Z., Cheng, Y., Gu, W., Zheng, Y., Sato, F., Mori, Y., Olaru, A. V., Paun, B. C., Yang, J., Kan, T., Ito, T., Hamilton, J. P., Selaru, F. M., Agarwal, R., David, S., Abraham, J. M., Wolfsen, H. C., Wallace, M. B., Shaheen, N. J., ... Meltzer, S. J. (2009). A multicenter, double-blinded validation study of methylation biomarkers for progression prediction in Barrett's esophagus. Cancer Research, 69(10), 4112-4115. https://doi.org/10.1158/0008-5472.CAN-09-0028

Jin, Z, Cheng, Y, Gu, W, Zheng, Y, Sato, F, Mori, Y, Olaru, AV, Paun, BC, Yang, J, Kan, T, Ito, T, Hamilton, JP , Selaru, FM, Agarwal, R, David, S, Abraham, JM, Wolfsen, HC, Wallace, MB, Shaheen, NJ, Washington, K, Wang, J, Canto, MI, Bhattacharyya, A, Nelson, MA, Wagner, PD, Romero, Y, Wang, KK, Feng, Z, Sampliner, RE & Meltzer, SJ 2009, 'A multicenter, double-blinded validation study of methylation biomarkers for progression prediction in Barrett's esophagus', Cancer Research, vol. 69, no. 10, pp. 4112-4115. https://doi.org/10.1158/0008-5472.CAN-09-0028

@article{372300f766e8436eacbee9d9fb9ef334,

title = "A multicenter, double-blinded validation study of methylation biomarkers for progression prediction in Barrett's esophagus",

abstract = "Esophageal adenocarcinoma risk in Barrett's esophagus (BE) is increased 30- to 125-fold versus the general population. Among all BE patients, however, neoplastic progression occurs only once per 200 patient-years. Molecular biomarkers are therefore needed to risk-stratify patients for more efficient surveillance endoscopy and to improve the early detection of progression. We therefore performed a retrospective, multicenter, double-blinded validation study of eight BE progression prediction methylation biomarkers. Progression or nonprogression were determined at 2 years (tier 1) and 4 years (tier 2). Methylation was assayed in 145 nonprogressors and 50 progressors using real-time quantitative methylationspecific PCR. Progressors were significantly older than nonprogressors (70.6 versus 62.5 years; P < 0.001). We evaluated a linear combination of the eight markers, using coefficients from a multivariate logistic regression analysis. Areas under the ROC curve (AUC) were high in the 2-year, 4-year, and combined data models (0.843, 0.829, and 0.840; P < 0.001, <0.001, and <0.001, respectively). In addition, even after rigorous overfitting correction, the incremental AUCs contributed by panels based on the 8 markers plus age versus age alone were substantial (Δ-AUC = 0.152, 0.114, and 0.118, respectively) in all 3 models. A methylation biomarker-based panel to predict neoplastic progression in BE has potential clinical value in improving both the efficiency of surveillance endoscopy and the early detection of neoplasia.",

author = "Zhe Jin and Yulan Cheng and Wen Gu and Yingye Zheng and Fumiaki Sato and Yuriko Mori and Olaru, {Alexandru V.} and Paun, {Bogdan C.} and Jian Yang and Takatsugu Kan and Tetsuo Ito and Hamilton, {James P.} and Selaru, {Florin M.} and Rachana Agarwal and Stefan David and Abraham, {John M.} and Wolfsen, {Herbert C.} and Wallace, {Michael B.} and Shaheen, {Nicholas J.} and Kay Washington and Jean Wang and Canto, {Marcia Irene} and Achyut Bhattacharyya and Nelson, {Mark A.} and Wagner, {Paul D.} and Yvonne Romero and Wang, {Kenneth K.} and Ziding Feng and Sampliner, {Richard E.} and Meltzer, {Stephen J.}",

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T1 - A multicenter, double-blinded validation study of methylation biomarkers for progression prediction in Barrett's esophagus

AU - Jin, Zhe

AU - Cheng, Yulan

AU - Gu, Wen

AU - Zheng, Yingye

AU - Sato, Fumiaki

AU - Mori, Yuriko

AU - Olaru, Alexandru V.

AU - Paun, Bogdan C.

AU - Yang, Jian

AU - Kan, Takatsugu

AU - Ito, Tetsuo

AU - Hamilton, James P.

AU - Selaru, Florin M.

AU - Agarwal, Rachana

AU - David, Stefan

AU - Abraham, John M.

AU - Wolfsen, Herbert C.

AU - Wallace, Michael B.

AU - Shaheen, Nicholas J.

AU - Washington, Kay

AU - Wang, Jean

AU - Canto, Marcia Irene

AU - Bhattacharyya, Achyut

AU - Nelson, Mark A.

AU - Wagner, Paul D.

AU - Romero, Yvonne

AU - Wang, Kenneth K.

AU - Feng, Ziding

AU - Sampliner, Richard E.

AU - Meltzer, Stephen J.

PY - 2009/5/15

Y1 - 2009/5/15

N2 - Esophageal adenocarcinoma risk in Barrett's esophagus (BE) is increased 30- to 125-fold versus the general population. Among all BE patients, however, neoplastic progression occurs only once per 200 patient-years. Molecular biomarkers are therefore needed to risk-stratify patients for more efficient surveillance endoscopy and to improve the early detection of progression. We therefore performed a retrospective, multicenter, double-blinded validation study of eight BE progression prediction methylation biomarkers. Progression or nonprogression were determined at 2 years (tier 1) and 4 years (tier 2). Methylation was assayed in 145 nonprogressors and 50 progressors using real-time quantitative methylationspecific PCR. Progressors were significantly older than nonprogressors (70.6 versus 62.5 years; P < 0.001). We evaluated a linear combination of the eight markers, using coefficients from a multivariate logistic regression analysis. Areas under the ROC curve (AUC) were high in the 2-year, 4-year, and combined data models (0.843, 0.829, and 0.840; P < 0.001, <0.001, and <0.001, respectively). In addition, even after rigorous overfitting correction, the incremental AUCs contributed by panels based on the 8 markers plus age versus age alone were substantial (Δ-AUC = 0.152, 0.114, and 0.118, respectively) in all 3 models. A methylation biomarker-based panel to predict neoplastic progression in BE has potential clinical value in improving both the efficiency of surveillance endoscopy and the early detection of neoplasia.

AB - Esophageal adenocarcinoma risk in Barrett's esophagus (BE) is increased 30- to 125-fold versus the general population. Among all BE patients, however, neoplastic progression occurs only once per 200 patient-years. Molecular biomarkers are therefore needed to risk-stratify patients for more efficient surveillance endoscopy and to improve the early detection of progression. We therefore performed a retrospective, multicenter, double-blinded validation study of eight BE progression prediction methylation biomarkers. Progression or nonprogression were determined at 2 years (tier 1) and 4 years (tier 2). Methylation was assayed in 145 nonprogressors and 50 progressors using real-time quantitative methylationspecific PCR. Progressors were significantly older than nonprogressors (70.6 versus 62.5 years; P < 0.001). We evaluated a linear combination of the eight markers, using coefficients from a multivariate logistic regression analysis. Areas under the ROC curve (AUC) were high in the 2-year, 4-year, and combined data models (0.843, 0.829, and 0.840; P < 0.001, <0.001, and <0.001, respectively). In addition, even after rigorous overfitting correction, the incremental AUCs contributed by panels based on the 8 markers plus age versus age alone were substantial (Δ-AUC = 0.152, 0.114, and 0.118, respectively) in all 3 models. A methylation biomarker-based panel to predict neoplastic progression in BE has potential clinical value in improving both the efficiency of surveillance endoscopy and the early detection of neoplasia.

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JO - Cancer Research

JF - Cancer Research

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ER -

A multicenter, double-blinded validation study of methylation biomarkers for progression prediction in Barrett's esophagus

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