The role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.

The role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.

Pituitary adenomas (PAs) are commonly occurring neoplasms with diverse endocrine and neurological effects. Although somatic gene mutations are uncommon in sporadic PAs, recent studies lend support to epigenetic modification as a potential cause of tumorigenesis and tumor progression.A systematic lit...

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Main Authors: Matthew Pease, Chao Ling, William J Mack, Kai Wang, Gabriel Zada
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3867353?pdf=render
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spelling doaj-25d8960af4bd458dad23e1bef8b631ed2020-11-25T01:52:50ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-01812e8261910.1371/journal.pone.0082619The role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.Matthew PeaseChao LingWilliam J MackKai WangGabriel ZadaPituitary adenomas (PAs) are commonly occurring neoplasms with diverse endocrine and neurological effects. Although somatic gene mutations are uncommon in sporadic PAs, recent studies lend support to epigenetic modification as a potential cause of tumorigenesis and tumor progression.A systematic literature review of the PubMed and Google Scholar databases was conducted to identify abstracts (n=1,082) pertaining to key targets and mechanisms implicated in epigenetic dysregulation of PAs published between 1993-2013. Data regarding histopathological subtype, target genes, mode of epigenetic modification, and clinical correlation were recorded and analyzed.Of the 47 that studies met inclusion criteria and focused on epigenomic assessment of PAs, only 2 were genome-scale analyses. Current evidence supports epigenetic alteration in at least 24 PA genes, which were categorized into four groups based on function and epigenetic alteration: 1) Sixteen tumor suppressor genes silenced via DNA methylation; 2) Two oncogenes overexpressed via histone acetylation and hypomethylation; 3) Three imprinted genes with selective allelic silencing; and 4) One epigenome writer inducing abnormal genome-scale activity and 5) Two transcription regulators indirectly modifying the genome. Of these, 5 genes (CDKN2A, GADD45y, FGFR2, caspase-8, and PTAG) showed particular susceptibility to epigenetic modification, with abnormal DNA methylation in >50% of PA samples. Several genes displayed correlations between epigenetic modification and clinically relevant parameters, including invasiveness (CDKN2A; DAPK; Rb1), sex (MAGE-A3), tumor size (GNAS1), and histopathological subtype (CDKN2A; MEG3; p27; RASSF1A; Rb1).Epigenetic modification of selected PA genes may play a key role in tumorigenesis and progression, which may translate into important diagnostic and therapeutic applications.http://europepmc.org/articles/PMC3867353?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Matthew Pease
Chao Ling
William J Mack
Kai Wang
Gabriel Zada
spellingShingle Matthew Pease
Chao Ling
William J Mack
Kai Wang
Gabriel Zada
The role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.
PLoS ONE
author_facet Matthew Pease
Chao Ling
William J Mack
Kai Wang
Gabriel Zada
author_sort Matthew Pease
title The role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.
title_short The role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.
title_full The role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.
title_fullStr The role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.
title_full_unstemmed The role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.
title_sort role of epigenetic modification in tumorigenesis and progression of pituitary adenomas: a systematic review of the literature.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Pituitary adenomas (PAs) are commonly occurring neoplasms with diverse endocrine and neurological effects. Although somatic gene mutations are uncommon in sporadic PAs, recent studies lend support to epigenetic modification as a potential cause of tumorigenesis and tumor progression.A systematic literature review of the PubMed and Google Scholar databases was conducted to identify abstracts (n=1,082) pertaining to key targets and mechanisms implicated in epigenetic dysregulation of PAs published between 1993-2013. Data regarding histopathological subtype, target genes, mode of epigenetic modification, and clinical correlation were recorded and analyzed.Of the 47 that studies met inclusion criteria and focused on epigenomic assessment of PAs, only 2 were genome-scale analyses. Current evidence supports epigenetic alteration in at least 24 PA genes, which were categorized into four groups based on function and epigenetic alteration: 1) Sixteen tumor suppressor genes silenced via DNA methylation; 2) Two oncogenes overexpressed via histone acetylation and hypomethylation; 3) Three imprinted genes with selective allelic silencing; and 4) One epigenome writer inducing abnormal genome-scale activity and 5) Two transcription regulators indirectly modifying the genome. Of these, 5 genes (CDKN2A, GADD45y, FGFR2, caspase-8, and PTAG) showed particular susceptibility to epigenetic modification, with abnormal DNA methylation in >50% of PA samples. Several genes displayed correlations between epigenetic modification and clinically relevant parameters, including invasiveness (CDKN2A; DAPK; Rb1), sex (MAGE-A3), tumor size (GNAS1), and histopathological subtype (CDKN2A; MEG3; p27; RASSF1A; Rb1).Epigenetic modification of selected PA genes may play a key role in tumorigenesis and progression, which may translate into important diagnostic and therapeutic applications.
url http://europepmc.org/articles/PMC3867353?pdf=render
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