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dc.creatorTopalović, Vladanka
dc.creatorSchwirtlich, Marija
dc.creatorStevanović, Milena
dc.creatorMojsin, Marija
dc.date.accessioned2022-11-15T14:53:39Z
dc.date.available2022-11-15T14:53:39Z
dc.date.issued2017
dc.identifier.issn0006-2979
dc.identifier.urihttps://imagine.imgge.bg.ac.rs/handle/123456789/1077
dc.description.abstractTranscription factors OCT4 and NANOG are main constituents of a functional network that controls proliferation and pluripotency maintenance of stem cells as well as early lineage decisions. We investigated expression profiles of OCT4 and NANOG during the early phases of neural differentiation using NT2/D1 cells induced by retinoic acid as an in vitro model system of human neurogenesis. We demonstrated decrease in OCT4 and NANOG mRNA and protein levels following exposure to retinoic acid. Next, by employing chromatin immunoprecipitation, we investigated profiles of selected H3 and H2B histone marks deposited on the promoters of the OCT4 and NANOG genes. We found decline in H3K4me3, H2BK5ac, and H2BK120ac on both promoters, which paralleled the decrease in OCT4 and NANOG expression. Moreover, we found that the H2BK16ac mark is differentially enriched on these two promoters, pointing to differences in epigenetic regulation of OCT4 and NANOG gene expression. Finally, based on our data, we suggest that the early response of pluripotency genes OCT4 and NANOG to the differentiation-inducing stimuli is mediated by dynamic changes in chromatin marks, while DNA methylation is acquired in the later stages of neurogenesis.en
dc.publisherMaik Nauka/Interperiodica/Springer, New York
dc.relationinfo:eu-repo/grantAgreement/MESTD/Basic Research (BR or ON)/173051/RS//
dc.rightsrestrictedAccess
dc.sourceBiochemistry-Moscow
dc.subjectOCT4en
dc.subjectNT2/D1 cell lineen
dc.subjectNANOGen
dc.subjecthistone modificationsen
dc.titleHistone modifications on the promoters of human OCT4 and NANOG genes at the onset of neural differentiation of NT2/D1 cellsen
dc.typearticle
dc.rights.licenseARR
dc.citation.epage722
dc.citation.issue6
dc.citation.other82(6): 715-722
dc.citation.rankM23
dc.citation.spage715
dc.citation.volume82
dc.identifier.doi10.1134/S0006297917060086
dc.identifier.pmid28601081
dc.identifier.scopus2-s2.0-85020708521
dc.identifier.wos000403456200008
dc.type.versionpublishedVersion


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