Inflammation-induced DNA methylation of DNA polymerase gamma alters the metabolic profile of colon tumors

dc.contributor.authorMaiuri, Ashley R.
dc.contributor.authorLi, Hongde
dc.contributor.authorStein, Barry D.
dc.contributor.authorTennessen, Jason M.
dc.contributor.authorO’Hagan, Heather M.
dc.contributor.departmentMedicine, School of Medicineen_US
dc.date.accessioned2019-05-20T20:23:39Z
dc.date.available2019-05-20T20:23:39Z
dc.date.issued2018-07-10
dc.description.abstractBackground: Inflammation, metabolism, and epigenetic modulation are highly interconnected processes that can be altered during tumorigenesis. However, because of the complexity of these interactions, direct cause and effect during tumorigenesis have been difficult to prove. Previously, using a murine model of inflammation-induced colon tumorigenesis, we determined that the promoter of the catalytic subunit of DNA polymerase gamma (Polg) is DNA hypermethylated and silenced in inflammation-induced tumors, but not in non-inflammation-induced (mock) tumors, suggesting that inflammation can induce silencing of Polg through promoting DNA methylation during tumorigenesis. Polg is the only mitochondrial DNA polymerase and mutations in Polg cause mitochondrial diseases in humans. Because of the role of mitochondria in metabolism, we hypothesized that silencing of Polg in inflammation-induced tumors would result in these tumors having altered metabolism in comparison to mock tumors. Methods: Inflammation-induced and mock colon tumors and colon epithelium from a mouse model of inflammation-induced colon tumorigenesis were assayed for alterations in Polg expression, mitochondria, and metabolism. Organoids derived from these tissues were used to study the direct effect of loss of Polg on mitochondria and metabolism. Results: We demonstrate that inflammation-induced tumors with reduced Polg expression have decreased mitochondrial DNA content and numbers of mitochondria compared to normal epithelium or mock tumors. Tumoroids derived from mock and inflammation-induced tumors retained key characteristics of the original tumors. Inflammation-induced tumoroids had increased glucose uptake and lactate secretion relative to mock tumoroids. shRNA-mediated knockdown of Polg in mock tumoroids reduced mtDNA content, increased glucose uptake and lactate secretion, and made the tumoroids more resistant to oxidative stress. Conclusions: These results suggest that inflammation-induced DNA methylation and silencing of Polg plays an important role in the tumorigenesis process by resulting in reduced mitochondria levels and altered metabolism. An enhanced understanding of how metabolism is altered in and drives inflammation-induced tumorigenesis will provide potential therapeutic targets.en_US
dc.eprint.versionFinal published versionen_US
dc.identifier.citationMaiuri, A. R., Li, H., Stein, B. D., Tennessen, J. M., & O'Hagan, H. M. (2018). Inflammation-induced DNA methylation of DNA polymerase gamma alters the metabolic profile of colon tumors. Cancer & metabolism, 6, 9. doi:10.1186/s40170-018-0182-7en_US
dc.identifier.urihttps://hdl.handle.net/1805/19401
dc.language.isoen_USen_US
dc.publisherBMCen_US
dc.relation.isversionof10.1186/s40170-018-0182-7en_US
dc.relation.journalCancer & Metabolismen_US
dc.rightsAttribution 3.0 United States*
dc.rights.urihttp://creativecommons.org/licenses/by/3.0/us/*
dc.sourcePMCen_US
dc.subjectDNA methylationen_US
dc.subjectDNA polymerase gammaen_US
dc.subjectGlucose uptakeen_US
dc.subjectGlycolysisen_US
dc.subjectInflammationen_US
dc.subjectMitochondriaen_US
dc.titleInflammation-induced DNA methylation of DNA polymerase gamma alters the metabolic profile of colon tumorsen_US
dc.typeArticleen_US
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