Identification of New Differentially Methylated Genes That Have Potential Functional Consequences in Prostate Cancer

Many differentially methylated genes have been identified in prostate cancer (PCa), primarily using candidate gene-based assays. Recently, several global DNA methylation profiles have been reported in PCa, however, each of these has weaknesses in terms of ability to observe global DNA methylation al...

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Autores principales: Kim, Jin W., Kim, Seong-Tae, Turner, Aubrey R., Young, Tracey, Smith, Shelly, Liu, Wennuan, Lindberg, Johan, Egevad, Lars, Gronberg, Henrik, Isaacs, William B., Xu, Jianfeng
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3485209/
https://www.ncbi.nlm.nih.gov/pubmed/23119026
http://dx.doi.org/10.1371/journal.pone.0048455
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author Kim, Jin W.
Kim, Seong-Tae
Turner, Aubrey R.
Young, Tracey
Smith, Shelly
Liu, Wennuan
Lindberg, Johan
Egevad, Lars
Gronberg, Henrik
Isaacs, William B.
Xu, Jianfeng
author_facet Kim, Jin W.
Kim, Seong-Tae
Turner, Aubrey R.
Young, Tracey
Smith, Shelly
Liu, Wennuan
Lindberg, Johan
Egevad, Lars
Gronberg, Henrik
Isaacs, William B.
Xu, Jianfeng
author_sort Kim, Jin W.
collection PubMed
description Many differentially methylated genes have been identified in prostate cancer (PCa), primarily using candidate gene-based assays. Recently, several global DNA methylation profiles have been reported in PCa, however, each of these has weaknesses in terms of ability to observe global DNA methylation alterations in PCa. We hypothesize that there remains unidentified aberrant DNA methylation in PCa, which may be identified using higher resolution assay methods. We used the newly developed Illumina HumanMethylation450 BeadChip in PCa (n = 19) and adjacent normal tissues (n = 4) and combined these with gene expression data for identifying new DNA methylation that may have functional consequences in PCa development and progression. We also confirmed our methylation results in an independent data set. Two aberrant DNA methylation genes were validated among an additional 56 PCa samples and 55 adjacent normal tissues. A total 28,735 CpG sites showed significant differences in DNA methylation (FDR adjusted P<0.05), defined as a mean methylation difference of at least 20% between PCa and normal samples. Furthermore, a total of 122 genes had more than one differentially methylated CpG site in their promoter region and a gene expression pattern that was inverse to the direction of change in DNA methylation (e.g. decreased expression with increased methylation, and vice-versa). Aberrant DNA methylation of two genes, AOX1 and SPON2, were confirmed via bisulfate sequencing, with most of the respective CpG sites showing significant differences between tumor samples and normal tissues. The AOX1 promoter region showed hypermethylation in 92.6% of 54 tested PCa samples in contrast to only three out of 53 tested normal tissues. This study used a new BeadChip combined with gene expression data in PCa to identify novel differentially methylated CpG sites located within genes. The newly identified differentially methylated genes may be used as biomarkers for PCa diagnosis.
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spelling pubmed-34852092012-11-01 Identification of New Differentially Methylated Genes That Have Potential Functional Consequences in Prostate Cancer Kim, Jin W. Kim, Seong-Tae Turner, Aubrey R. Young, Tracey Smith, Shelly Liu, Wennuan Lindberg, Johan Egevad, Lars Gronberg, Henrik Isaacs, William B. Xu, Jianfeng PLoS One Research Article Many differentially methylated genes have been identified in prostate cancer (PCa), primarily using candidate gene-based assays. Recently, several global DNA methylation profiles have been reported in PCa, however, each of these has weaknesses in terms of ability to observe global DNA methylation alterations in PCa. We hypothesize that there remains unidentified aberrant DNA methylation in PCa, which may be identified using higher resolution assay methods. We used the newly developed Illumina HumanMethylation450 BeadChip in PCa (n = 19) and adjacent normal tissues (n = 4) and combined these with gene expression data for identifying new DNA methylation that may have functional consequences in PCa development and progression. We also confirmed our methylation results in an independent data set. Two aberrant DNA methylation genes were validated among an additional 56 PCa samples and 55 adjacent normal tissues. A total 28,735 CpG sites showed significant differences in DNA methylation (FDR adjusted P<0.05), defined as a mean methylation difference of at least 20% between PCa and normal samples. Furthermore, a total of 122 genes had more than one differentially methylated CpG site in their promoter region and a gene expression pattern that was inverse to the direction of change in DNA methylation (e.g. decreased expression with increased methylation, and vice-versa). Aberrant DNA methylation of two genes, AOX1 and SPON2, were confirmed via bisulfate sequencing, with most of the respective CpG sites showing significant differences between tumor samples and normal tissues. The AOX1 promoter region showed hypermethylation in 92.6% of 54 tested PCa samples in contrast to only three out of 53 tested normal tissues. This study used a new BeadChip combined with gene expression data in PCa to identify novel differentially methylated CpG sites located within genes. The newly identified differentially methylated genes may be used as biomarkers for PCa diagnosis. Public Library of Science 2012-10-31 /pmc/articles/PMC3485209/ /pubmed/23119026 http://dx.doi.org/10.1371/journal.pone.0048455 Text en © 2012 Kim et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Kim, Jin W.
Kim, Seong-Tae
Turner, Aubrey R.
Young, Tracey
Smith, Shelly
Liu, Wennuan
Lindberg, Johan
Egevad, Lars
Gronberg, Henrik
Isaacs, William B.
Xu, Jianfeng
Identification of New Differentially Methylated Genes That Have Potential Functional Consequences in Prostate Cancer
title Identification of New Differentially Methylated Genes That Have Potential Functional Consequences in Prostate Cancer
title_full Identification of New Differentially Methylated Genes That Have Potential Functional Consequences in Prostate Cancer
title_fullStr Identification of New Differentially Methylated Genes That Have Potential Functional Consequences in Prostate Cancer
title_full_unstemmed Identification of New Differentially Methylated Genes That Have Potential Functional Consequences in Prostate Cancer
title_short Identification of New Differentially Methylated Genes That Have Potential Functional Consequences in Prostate Cancer
title_sort identification of new differentially methylated genes that have potential functional consequences in prostate cancer
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3485209/
https://www.ncbi.nlm.nih.gov/pubmed/23119026
http://dx.doi.org/10.1371/journal.pone.0048455
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