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AuthorCardoso, Leila C. A.
AuthorCastaño, Jair A. Tenorio
AuthorPereira, Hanna S.
AuthorLima, Maria Angélica de F. D.
AuthorSantos, Anna Cláudia E. dos
AuthorFaria, Paulo S. de
AuthorFerman, Sima
AuthorSeuánez, Héctor N.
AuthorNevado, Julián B.
AuthorAlmeida, José Carlos Cabral de
AuthorLapunzina, Pablo
AuthorVargas, Fernando R.
Access date2013-08-21T12:57:27Z
Available date2013-08-21T12:57:27Z
Document date2011
URIhttps://www.arca.fiocruz.br/handle/icict/6809
Languageengpt_BR
Rightsopen access
TitleConstitutional and somatic methylation status of DMRH19 and KvDMR in Wilms tumor patientspt_BR
TypeArticlept_BR
DOI10.1590/S1415-47572012005000073
AbstractThe most frequent epigenetic alterations in Wilms tumor (WT) occur at WT2, assigned to 11p15. WT2 consists of two domains: telomeric domain 1 (DMRH19) that contains the IGF2 gene and an imprinted maternally expressed transcript (H19) and centromeric domain 2 (KvDMR) that contains the genes KCNQ1, KCNQ1OT1 and CDKN1C. In this work, we used pyrosequencing and MS-MLPA to compare the methylation patterns of DMRH19/KvDMR in blood and tumor samples from 40 WT patients. Normal constitutional KvDMR methylation indicated that most of the epigenetic alterations in WT occur at DMRH19. Constitutional DMRH19 hypermethylation (HM DMRH19) was observed in two patients with Beckwith-Wiedemann syndrome. Pyrosequencing and MS-MLPA showed HM DMRH19 in 28/34 tumor samples: 16/34 with isolated HM DMRH19 and 12/34 with concomitant HM DMRH19 and KvDMR hypomethylation, indicating paternal uniparental disomy. With the exception of one blood sample, the MS-MLPA and pyrosequencing findings were concordant. Diffuse or focal anaplasia was present in five tumor samples and was associated with isolated somatic HM DMRH19 in four of them. Constitutional 11p15 methylation abnormalities were present in 5% of the samples and somatic abnormalities in the majority of tumors. Combined analysis of DMRH19/KvDMR by pyrosequencing and MS-MLPA is beneficial for characterizing epigenetic anomalies in WT, and MS-MLPA is useful and reliable for estimation of DNA methylation in a clinical setting.pt_BR
AffilliationUniversidade Federal do Rio de Janeiro. Departamento de Genética. Rio de Janeiro, RJ, Brasil / Instituto Nacional de Câncer. Programa de Genética. Rio de Janeiro, RJ, Brasilpt_BR
AffilliationHospital Universitario La Paz. Instituto de Genética Médica y Molecular. La Paz, Bolíviapt_BR
AffilliationInstituto Nacional de Câncer. Programa de Genética. Rio de Janeiro, RJ, Brasilpt_BR
AffilliationInstituto Nacional de Câncer. Programa de Genética. Rio de Janeiro, RJ, Brasil / Universidade Federal do Estado do Rio de Janeiro. Departamento de Genética e Biologia Molecular. Rio de Janeiro, RJ, Brasilpt_BR
AffilliationUniversidade Federal do Rio de Janeiro. Departamento de Genética. Rio de Janeiro, RJ, Brasilpt_BR
AffilliationInstituto Nacional de Câncer. Divisão de Patologia. Rio de Janeiro, RJ, Brasilpt_BR
AffilliationInstituto Nacional de Câncer. Serviço de Oncologia Pediátrica. Rio de Janeiro, RJ, Brasilpt_BR
AffilliationUniversidade Federal do Rio de Janeiro. Departamento de Genética. Rio de Janeiro, RJ, Brasil / Instituto Nacional de Câncer. Programa de Genética. Rio de Janeiro, RJ, Brasilpt_BR
AffilliationHospital Universitario La Paz. Instituto de Genética Médica y Molecular. La Paz, Bolíviapt_BR
AffilliationFundação Oswaldo Cruz. Instituto Nacional de Saúde da Mulher. da Criança e da Saúde. Departamento de Genética. Rio de Janeiro, RJ, Brasilpt_BR
AffilliationHospital Universitario La Paz. Instituto de Genética Médica y Molecular. La Paz, Bolíviapt_BR
AffilliationUniversidade Federal do Rio de Janeiro. Departamento de Genética. Rio de Janeiro, RJ, Brasil / Instituto Nacional de Câncer. Programa de Genética. Rio de Janeiro, RJ, Brasil / Universidade Federal do Estado do Rio de Janeiro. Departamento de Genética e Biologia Molecular. Rio de Janeiro, RJ, Brasilpt_BR
SubjectEpigeneticpt_BR
SubjectHistopathologypt_BR
SubjectMethylationpt_BR
SubjectMS-MLPApt_BR
SubjectPyrosequencingpt_BR
DeCSEpigênese Genéticapt_BR
DeCSPatologiapt_BR
DeCSMetilaçãopt_BR


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