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dc.contributor.authorThomas, R.
dc.contributor.authorTrapani, D.
dc.contributor.authorGoodyer-Sait, L.
dc.contributor.authorTomkova, M.
dc.contributor.authorFernández Rozadilla, Ceres
dc.contributor.authorSahnane, N.
dc.contributor.authorWoolley, C.
dc.contributor.authorDavis, H.
dc.contributor.authorChegwidden, L.
dc.contributor.authorKriaucionis, S.
dc.contributor.authorMaughan, T.
dc.contributor.authorLeedham, S.
dc.contributor.authorPalles, C.
dc.contributor.authorFurlan, D.
dc.contributor.authorTomlinson, I.
dc.contributor.authorLewis, A.
dc.date.accessioned2021-10-14T12:58:49Z
dc.date.available2021-10-14T12:58:49Z
dc.date.issued2019
dc.identifier.issn2045-2322
dc.identifier.otherhttps://www.ncbi.nlm.nih.gov/pubmed/31530880
dc.identifier.otherhttps://www.ncbi.nlm.nih.gov/pmc/articles/PMC6748923/pdf/41598_2019_Article_49952.pdf
dc.identifier.urihttp://hdl.handle.net/20.500.11940/15553
dc.description.abstractExpression of the mismatch repair gene MutL homolog 1 (MLH1) is silenced in a clinically important subgroup of sporadic colorectal cancers. These cancers exhibit hypermutability with microsatellite instability (MSI) and differ from microsatellite-stable (MSS) colorectal cancers in both prognosis and response to therapies. Loss of MLH1 is usually due to epigenetic silencing with associated promoter methylation; coding somatic mutations rarely occur. Here we use the presence of a colorectal cancer (CRC) risk variant (rs1800734) within the MLH1 promoter to investigate the poorly understood mechanisms of MLH1 promoter methylation and loss of expression. We confirm the association of rs1800734 with MSI+ but not MSS cancer risk in our own data and by meta-analysis. Using sensitive allele-specific detection methods, we demonstrate that MLH1 is the target gene for rs1800734 mediated cancer risk. In normal colon tissue, small allele-specific differences exist only in MLH1 promoter methylation, but not gene expression. In contrast, allele-specific differences in both MLH1 methylation and expression are present in MSI+ cancers. We show that MLH1 transcriptional repression is dependent on DNA methylation and can be reversed by a methylation inhibitor. The rs1800734 allele influences the rate of methylation loss and amount of re-expression. The transcription factor TFAP4 binds to the rs1800734 region but with much weaker binding to the risk than the protective allele. TFAP4 binding is absent on both alleles when promoter methylation is present. Thus we propose that TFAP4 binding shields the protective rs1800734 allele of the MLH1 promoter from BRAF induced DNA methylation more effectively than the risk allele.
dc.rightsAtribución 4.0 Internacional
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.titleThe polymorphic variant rs1800734 influences methylation acquisition and allele-specific TFAP4 binding in the MLH1 promoter leading to differential mRNA expression
dc.typeArtigoes
dc.authorsophosFernández Rozadilla, Ceres
dc.identifier.doi10.1038/s41598-019-49952-x
dc.identifier.pmid31530880
dc.identifier.sophos31008
dc.issue.number1
dc.journal.titleScientific Reports
dc.organizationServizo Galego de Saúde::Dirección Xeral de Asistencia Sanitaria::Fundación Pública Galega de Medicina Xenómica
dc.organizationServizo Galego de Saúde::Estrutura de Xestión Integrada (EOXI)::Instituto de Investigación Sanitaria de Santiago de Compostela (IDIS)
dc.page.initial13463es
dc.rights.accessRightsopenAccess
dc.subject.keywordFPGMX
dc.subject.keywordIDIS
dc.typefidesArtículo Científico (incluye Original, Original breve, Revisión Sistemática y Meta-análisis)
dc.typesophosArtículo Original
dc.volume.number9


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