Modulation of mitochondrial DNA copy number in a model of glioblastoma induces changes to DNA methylation and gene expression of the nuclear genome in tumours

Modulation of mitochondrial DNA copy number in a model of glioblastoma induces changes to DNA methylation and gene expression of the nuclear genome in tumours

Abstract Background There are multiple copies of mitochondrial DNA (mtDNA) present in each cell type, and they are strictly regulated in a cell-specific manner by a group of nuclear-encoded mtDNA-specific replication factors. This strict regulation of mtDNA copy number is mediated by cell-specific D...

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Main Authors: Xin Sun, Justin C. St John
Format: Article
Language:English
Published: BMC 2018-09-01
Series:Epigenetics & Chromatin
Subjects:
Mitochondrial DNA
DNA methylation
Gene expression
Tumorigenesis
POLG
Online Access:http://link.springer.com/article/10.1186/s13072-018-0223-z
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spelling doaj-01301ea5146b4c6994807eff102557882020-11-25T02:08:39ZengBMCEpigenetics & Chromatin1756-89352018-09-0111111810.1186/s13072-018-0223-zModulation of mitochondrial DNA copy number in a model of glioblastoma induces changes to DNA methylation and gene expression of the nuclear genome in tumoursXin Sun0Justin C. St John1Mitochondrial Genetics Group, Hudson Institute of Medical ResearchMitochondrial Genetics Group, Hudson Institute of Medical ResearchAbstract Background There are multiple copies of mitochondrial DNA (mtDNA) present in each cell type, and they are strictly regulated in a cell-specific manner by a group of nuclear-encoded mtDNA-specific replication factors. This strict regulation of mtDNA copy number is mediated by cell-specific DNA methylation of these replication factors. Glioblastoma multiforme, HSR-GBM1, cells are hyper-methylated and maintain low mtDNA copy number to support their tumorigenic status. We have previously shown that when HSR-GBM1 cells with 50% of their original mtDNA content were inoculated into mice, tumours grew more aggressively than non-depleted cells. However, when the cells possessed only 3% and 0.2% of their original mtDNA content, tumour formation was less frequent and the initiation of tumorigenesis was significantly delayed. Importantly, the process of tumorigenesis was dependent on mtDNA copy number being restored to pre-depletion levels. Results By performing whole genome MeDIP-Seq and RNA-Seq on tumours generated from cells possessing 100%, 50%, 0.3% and 0.2% of their original mtDNA content, we determined that restoration of mtDNA copy number caused significant changes to both the nuclear methylome and its transcriptome for each tumour type. The affected genes were specifically associated with gene networks and pathways involving behaviour, nervous system development, cell differentiation and regulation of transcription and cellular processes. The mtDNA-specific replication factors were also modulated. Conclusions Our results highlight the bidirectional control of the nuclear and mitochondrial genomes through modulation of DNA methylation to control mtDNA copy number, which, in turn, modulates nuclear gene expression during tumorigenesis.http://link.springer.com/article/10.1186/s13072-018-0223-zMitochondrial DNADNA methylationGene expressionTumorigenesisPOLG
collection DOAJ
language English
format Article
sources DOAJ
author Xin Sun
Justin C. St John
spellingShingle Xin Sun
Justin C. St John
Modulation of mitochondrial DNA copy number in a model of glioblastoma induces changes to DNA methylation and gene expression of the nuclear genome in tumours
Epigenetics & Chromatin
Mitochondrial DNA
DNA methylation
Gene expression
Tumorigenesis
POLG
author_facet Xin Sun
Justin C. St John
author_sort Xin Sun
title Modulation of mitochondrial DNA copy number in a model of glioblastoma induces changes to DNA methylation and gene expression of the nuclear genome in tumours
title_short Modulation of mitochondrial DNA copy number in a model of glioblastoma induces changes to DNA methylation and gene expression of the nuclear genome in tumours
title_full Modulation of mitochondrial DNA copy number in a model of glioblastoma induces changes to DNA methylation and gene expression of the nuclear genome in tumours
title_fullStr Modulation of mitochondrial DNA copy number in a model of glioblastoma induces changes to DNA methylation and gene expression of the nuclear genome in tumours
title_full_unstemmed Modulation of mitochondrial DNA copy number in a model of glioblastoma induces changes to DNA methylation and gene expression of the nuclear genome in tumours
title_sort modulation of mitochondrial dna copy number in a model of glioblastoma induces changes to dna methylation and gene expression of the nuclear genome in tumours
publisher BMC
series Epigenetics & Chromatin
issn 1756-8935
publishDate 2018-09-01
description Abstract Background There are multiple copies of mitochondrial DNA (mtDNA) present in each cell type, and they are strictly regulated in a cell-specific manner by a group of nuclear-encoded mtDNA-specific replication factors. This strict regulation of mtDNA copy number is mediated by cell-specific DNA methylation of these replication factors. Glioblastoma multiforme, HSR-GBM1, cells are hyper-methylated and maintain low mtDNA copy number to support their tumorigenic status. We have previously shown that when HSR-GBM1 cells with 50% of their original mtDNA content were inoculated into mice, tumours grew more aggressively than non-depleted cells. However, when the cells possessed only 3% and 0.2% of their original mtDNA content, tumour formation was less frequent and the initiation of tumorigenesis was significantly delayed. Importantly, the process of tumorigenesis was dependent on mtDNA copy number being restored to pre-depletion levels. Results By performing whole genome MeDIP-Seq and RNA-Seq on tumours generated from cells possessing 100%, 50%, 0.3% and 0.2% of their original mtDNA content, we determined that restoration of mtDNA copy number caused significant changes to both the nuclear methylome and its transcriptome for each tumour type. The affected genes were specifically associated with gene networks and pathways involving behaviour, nervous system development, cell differentiation and regulation of transcription and cellular processes. The mtDNA-specific replication factors were also modulated. Conclusions Our results highlight the bidirectional control of the nuclear and mitochondrial genomes through modulation of DNA methylation to control mtDNA copy number, which, in turn, modulates nuclear gene expression during tumorigenesis.
topic Mitochondrial DNA
DNA methylation
Gene expression
Tumorigenesis
POLG
url http://link.springer.com/article/10.1186/s13072-018-0223-z
work_keys_str_mv AT xinsun modulationofmitochondrialdnacopynumberinamodelofglioblastomainduceschangestodnamethylationandgeneexpressionofthenucleargenomeintumours
AT justincstjohn modulationofmitochondrialdnacopynumberinamodelofglioblastomainduceschangestodnamethylationandgeneexpressionofthenucleargenomeintumours
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