MicroRNA expression profile in head and neck cancer

dc.contributor.authorSEVERINO, PATRICIA
dc.contributor.authorBRUGGEMANN, HOLGER
dc.contributor.authorANDREGHETTO, FLAVIA M.
dc.contributor.authorCAMPS, CARME
dc.contributor.authorKLINGBEIL, MARIA de F.G.
dc.contributor.authorPEREIRA, WELBERT O. de
dc.contributor.authorSOARES, RENATA M.
dc.contributor.authorMOYSES, RAQUEL
dc.contributor.authorWUNSCH FILHO, VICTOR
dc.contributor.authorMATHOR, MONICA B.
dc.contributor.authorNUNES, FABIO D.
dc.contributor.authorRAGOUSSIS, JIANNIS
dc.contributor.authorTAJARA, ELOIZA H.
dc.coverageInternacionalpt_BR
dc.date.accessioned2014-08-13T13:11:20Z
dc.date.available2014-08-13T13:11:20Z
dc.date.issued2013pt_BR
dc.description.abstractAbstract Background: Current evidence implicates aberrant microRNA expression patterns in human malignancies; measurement of microRNA expression may have diagnostic and prognostic applications. Roles for microRNAs in head and neck squamous cell carcinomas (HNSCC) are largely unknown. HNSCC, a smoking-related cancer, is one of the most common malignancies worldwide but reliable diagnostic and prognostic markers have not been discovered so far. Some studies have evaluated the potential use of microRNA as biomarkers with clinical application in HNSCC. Methods: MicroRNA expression profile of oral squamous cell carcinoma samples was determined by means of DNA microarrays. We also performed gain-of-function assays for two differentially expressed microRNA using two squamous cell carcinoma cell lines and normal oral keratinocytes. The effect of the over-expression of these molecules was evaluated by means of global gene expression profiling and cell proliferation assessment. Results: Altered microRNA expression was detected for a total of 72 microRNAs. Among these we found well studied molecules, such as the miR-17-92 cluster, comprising potent oncogenic microRNA, and miR-34, recently found to interact with p53. HOX-cluster embedded miR-196a/b and miR-10b were up- and down-regulated, respectively, in tumor samples. Since validated HOX gene targets for these microRNAs are not consistently deregulated in HNSCC, we performed gain-of-function experiments, in an attempt to outline their possible role. Our results suggest that both molecules interfere in cell proliferation through distinct processes, possibly targeting a small set of genes involved in cell cycle progression. Conclusions: Functional data on miRNAs in HNSCC is still scarce. Our data corroborate current literature and brings new insights into the role of microRNAs in HNSCC. We also show that miR-196a and miR-10b, not previously associated with HNSCC, may play an oncogenic role in this disease through the deregulation of cell proliferation. The study of microRNA alterations in HNSCC is an essential step to the mechanistic understanding of tumor formation and could lead to the discovery of clinically relevant biomarkers.
dc.identifier.citationSEVERINO, PATRICIA; BRUGGEMANN, HOLGER; ANDREGHETTO, FLAVIA M.; CAMPS, CARME; KLINGBEIL, MARIA de F.G.; PEREIRA, WELBERT O. de; SOARES, RENATA M.; MOYSES, RAQUEL; WUNSCH FILHO, VICTOR; MATHOR, MONICA B.; NUNES, FABIO D.; RAGOUSSIS, JIANNIS; TAJARA, ELOIZA H. MicroRNA expression profile in head and neck cancer: HOX-cluster embedded microRNA-196a and microRNA-10b dysregulation implicated in cell proliferation. <b>BMC Cancer</b>, v. artigo 533, 2013. DOI: <a href="https://dx.doi.org/10.1186/1471-2407-13-533">10.1186/1471-2407-13-533</a>. Disponível em: http://repositorio.ipen.br/handle/123456789/8925.
dc.identifier.doi10.1186/1471-2407-13-533
dc.identifier.issn1471-2407pt_BR
dc.identifier.orcidhttp://orcid.org/0000-0002-7294-9106
dc.identifier.urihttp://repositorio.ipen.br/handle/123456789/8925
dc.identifier.volartigo 533
dc.relation.ispartofBMC Cancerpt_BR
dc.rightsopenAccess
dc.subjectcarcinomas
dc.subjecthead
dc.subjectneck
dc.subjectmessenger-rna
dc.subjectcell proliferation
dc.subjectsample preparation
dc.subjectdna
dc.subjecttumor cells
dc.subjectkeratin
dc.subjectbiological markers
dc.titleMicroRNA expression profile in head and neck cancerpt_BR
dc.typeArtigo de periódicopt_BR
dspace.entity.typePublication
ipen.autorPATRÍCIA SEVERINO
ipen.autorRENATA MACHADO SOARES
ipen.autorRAQUEL MOYSES
ipen.autorVICTOR WUNSCH-FILHO
ipen.autorFÁBIO DAUMAS NUNES
ipen.autorMONICA BEATRIZ MATHOR
ipen.autorMARIA FATIMA GUARIZO KLINGBEIL
ipen.autorFLAVIA MAZIERO ANDREGHETTO
ipen.codigoautor10638
ipen.codigoautor10634
ipen.codigoautor11917
ipen.codigoautor11918
ipen.codigoautor10636
ipen.codigoautor209
ipen.codigoautor3309
ipen.codigoautor10633
ipen.contributor.ipenauthorPATRÍCIA SEVERINO
ipen.contributor.ipenauthorRENATA MACHADO SOARES
ipen.contributor.ipenauthorRAQUEL MOYSES
ipen.contributor.ipenauthorVICTOR WUNSCH-FILHO
ipen.contributor.ipenauthorFÁBIO DAUMAS NUNES
ipen.contributor.ipenauthorMONICA BEATRIZ MATHOR
ipen.contributor.ipenauthorMARIA FATIMA GUARIZO KLINGBEIL
ipen.contributor.ipenauthorFLAVIA MAZIERO ANDREGHETTO
ipen.date.recebimento14-08pt_BR
ipen.identifier.fi3.319pt_BR
ipen.identifier.ipendoc20013pt_BR
ipen.identifier.iwosWoSpt_BR
ipen.identifier.ods3
ipen.range.fi3.000 - 4.499
ipen.subtituloHOX-cluster embedded microRNA-196a and microRNA-10b dysregulation implicated in cell proliferation
ipen.type.genreArtigo
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relation.isAuthorOfPublication.latestForDiscovery00494ed4-d07a-4fae-8c2a-462aaf800bec
sigepi.autor.atividadeSEVERINO, PATRICIA:10638:-1:S
sigepi.autor.atividadeANDREGHETTO, FLAVIA M.:10633:-1:N
sigepi.autor.atividadeKLINGBEIL, MARIA DE F.G.:3309:230:N
sigepi.autor.atividadeSOARES, RENATA M.:10634:-1:N
sigepi.autor.atividadeMOYSES, RAQUEL:11917:-1:N
sigepi.autor.atividadeWUNSCH FILHO, VICTOR:11918:-1:N
sigepi.autor.atividadeMATHOR, MONICA B.:209:220:N
sigepi.autor.atividadeNUNES, FABIO D.:10636:-1:N

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