Leukocyte DNA methylation signature differentiates pancreatic cancer patients from healthy controls.

Leukocyte DNA methylation signature differentiates pancreatic cancer patients from healthy controls.

Pancreatic adenocarcinoma (PaC) is one of most difficult tumors to treat. Much of this is attributed to the late diagnosis. To identify biomarkers for early detection, we examined DNA methylation differences in leukocyte DNA between PaC cases and controls in a two-phase study. In phase I, we measure...

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Main Authors: Katrina S Pedersen, William R Bamlet, Ann L Oberg, Mariza de Andrade, Martha E Matsumoto, Hui Tang, Stephen N Thibodeau, Gloria M Petersen, Liang Wang
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2011-03-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3063802?pdf=render
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spelling doaj-1a82d48ff64649d6bca7a525be7200232020-11-25T02:32:13ZengPublic Library of Science (PLoS)PLoS ONE1932-62032011-03-0163e1822310.1371/journal.pone.0018223Leukocyte DNA methylation signature differentiates pancreatic cancer patients from healthy controls.Katrina S PedersenWilliam R BamletAnn L ObergMariza de AndradeMartha E MatsumotoHui TangStephen N ThibodeauGloria M PetersenLiang WangPancreatic adenocarcinoma (PaC) is one of most difficult tumors to treat. Much of this is attributed to the late diagnosis. To identify biomarkers for early detection, we examined DNA methylation differences in leukocyte DNA between PaC cases and controls in a two-phase study. In phase I, we measured methylation levels at 1,505 CpG sites in treatment-naïve leukocyte DNA from 132 never-smoker PaC patients and 60 never-smoker healthy controls. We found significant differences in 110 CpG sites (false discovery rate <0.05). In phase II, we tested and validated 88 of 96 phase I selected CpG sites in 240 PaC cases and 240 matched controls (p≤0.05). Using penalized logistic regression, we built a prediction model consisting of five CpG sites (IL10_P348, LCN2_P86, ZAP70_P220, AIM2_P624, TAL1_P817) that discriminated PaC patients from controls (C-statistic = 0.85 in phase I; 0.76 in phase II). Interestingly, one CpG site (LCN2_P86) alone could discriminate resectable patients from controls (C-statistic= 0.78 in phase I; 0.74 in phase II). We also performed methylation quantitative trait loci (methQTL) analysis and identified three CpG sites (AGXT_P180_F, ALOX12_E85_R, JAK3_P1075_R) where the methylation levels were significantly associated with single nucleotide polymorphisms (SNPs) (false discovery rate <0.05). Our results demonstrate that epigenetic variation in easily obtainable leukocyte DNA, manifested by reproducible methylation differences, may be used to detect PaC patients. The methylation differences at certain CpG sites are partially attributable to genetic variation. This study strongly supports future epigenome-wide association study using leukocyte DNA for biomarker discovery in human diseases.http://europepmc.org/articles/PMC3063802?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Katrina S Pedersen
William R Bamlet
Ann L Oberg
Mariza de Andrade
Martha E Matsumoto
Hui Tang
Stephen N Thibodeau
Gloria M Petersen
Liang Wang
spellingShingle Katrina S Pedersen
William R Bamlet
Ann L Oberg
Mariza de Andrade
Martha E Matsumoto
Hui Tang
Stephen N Thibodeau
Gloria M Petersen
Liang Wang
Leukocyte DNA methylation signature differentiates pancreatic cancer patients from healthy controls.
PLoS ONE
author_facet Katrina S Pedersen
William R Bamlet
Ann L Oberg
Mariza de Andrade
Martha E Matsumoto
Hui Tang
Stephen N Thibodeau
Gloria M Petersen
Liang Wang
author_sort Katrina S Pedersen
title Leukocyte DNA methylation signature differentiates pancreatic cancer patients from healthy controls.
title_short Leukocyte DNA methylation signature differentiates pancreatic cancer patients from healthy controls.
title_full Leukocyte DNA methylation signature differentiates pancreatic cancer patients from healthy controls.
title_fullStr Leukocyte DNA methylation signature differentiates pancreatic cancer patients from healthy controls.
title_full_unstemmed Leukocyte DNA methylation signature differentiates pancreatic cancer patients from healthy controls.
title_sort leukocyte dna methylation signature differentiates pancreatic cancer patients from healthy controls.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2011-03-01
description Pancreatic adenocarcinoma (PaC) is one of most difficult tumors to treat. Much of this is attributed to the late diagnosis. To identify biomarkers for early detection, we examined DNA methylation differences in leukocyte DNA between PaC cases and controls in a two-phase study. In phase I, we measured methylation levels at 1,505 CpG sites in treatment-naïve leukocyte DNA from 132 never-smoker PaC patients and 60 never-smoker healthy controls. We found significant differences in 110 CpG sites (false discovery rate <0.05). In phase II, we tested and validated 88 of 96 phase I selected CpG sites in 240 PaC cases and 240 matched controls (p≤0.05). Using penalized logistic regression, we built a prediction model consisting of five CpG sites (IL10_P348, LCN2_P86, ZAP70_P220, AIM2_P624, TAL1_P817) that discriminated PaC patients from controls (C-statistic = 0.85 in phase I; 0.76 in phase II). Interestingly, one CpG site (LCN2_P86) alone could discriminate resectable patients from controls (C-statistic= 0.78 in phase I; 0.74 in phase II). We also performed methylation quantitative trait loci (methQTL) analysis and identified three CpG sites (AGXT_P180_F, ALOX12_E85_R, JAK3_P1075_R) where the methylation levels were significantly associated with single nucleotide polymorphisms (SNPs) (false discovery rate <0.05). Our results demonstrate that epigenetic variation in easily obtainable leukocyte DNA, manifested by reproducible methylation differences, may be used to detect PaC patients. The methylation differences at certain CpG sites are partially attributable to genetic variation. This study strongly supports future epigenome-wide association study using leukocyte DNA for biomarker discovery in human diseases.
url http://europepmc.org/articles/PMC3063802?pdf=render
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AT stephennthibodeau leukocytednamethylationsignaturedifferentiatespancreaticcancerpatientsfromhealthycontrols
AT gloriampetersen leukocytednamethylationsignaturedifferentiatespancreaticcancerpatientsfromhealthycontrols
AT liangwang leukocytednamethylationsignaturedifferentiatespancreaticcancerpatientsfromhealthycontrols
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