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dc.contributor.authorRodriguez, David Enrique Aguilarpt_BR
dc.contributor.authorLima, Carmen Silvia Passospt_BR
dc.contributor.authorLourenço, Gustavo Jacobpt_BR
dc.contributor.authorFigueiredo, Maria Estelapt_BR
dc.contributor.authorCarneiro, Jorge David Aivazoglupt_BR
dc.contributor.authorTone, Luiz Gonzagapt_BR
dc.contributor.authorLlerena Jr., Juan Clintonpt_BR
dc.contributor.authorToscano, Raquel Alvespt_BR
dc.contributor.authorBrandalise, Silviapt_BR
dc.contributor.authorPinto Júnior, Walterpt_BR
dc.contributor.authorCosta, Fernando Ferreirapt_BR
dc.contributor.authorBertuzzo, Carmen Sílviapt_BR
dc.date.accessioned2017-12-07T04:43:37Z-
dc.date.available2017-12-07T04:43:37Z-
dc.date.issued2005pt_BR
dc.identifier.citationGenet. Mol. Biol.,v.28,n.2,p.205-209,2005pt_BR
dc.identifier.urihttp://repositorio.unb.br/handle/10482/26521-
dc.description.abstractFanconi anaemia (FA) is a recessive autosomal disease determined by mutations in genes of at least eleven complementation groups, with distinct distributions in different populations. As far as we know, there are no reports regarding the molecular characterisation of the disease in unselected FA patients in Brazil. OBECTIVE: This study aimed to investigate the most prevalent mutations of FANCA and FANCC genes in Brazilian patients with FA. METHODS: Genomic DNA obtained from 22 racially and ethnically diverse unrelated FA patients (mean age ± SD: 14.0 ± 7.8 years; 10 male, 12 female; 14 white, 8 black) was analysed by polymerase chain reaction and restriction site assays for identification of FANCA (delta3788-3790) and FANCC (delta322G, IVS4+4A -> T, W22X, L496R, R548X, Q13X, R185X, and L554P) gene mutations. RESULTS: Mutations in FANCA and FANCC genes were identified in 6 (27.3%) and 14 (63.6%) out of 22 patients, respectively. The disease could not be attributed to the tested mutations in the two remaining patients enrolled in the study (9.1%). The registry of the two most prevalent gene abnormalities (delta3788-3790 and IVS4 + 4 -> T) revealed that they were present in 18.2% and 15.9% of the FA alleles, respectively. Additional FANCC gene mutations were found in the study, with the following prevalence: delta322G (11.4%), W22X (9.1%), Q13X (2.3%), L554P (2.3%), and R548X (2.3%) of total FA alleles. CONCLUSION: These results suggest that mutations of FANCA and FANCC genes are the most prevalent mutations among FA patients in Brazil.pt_BR
dc.language.isoenpt_BR
dc.publisherSociedade Brasileira de Genéticapt_BR
dc.rightsAcesso Abertopt_BR
dc.titleMolecular analysis of the most prevalent mutations of the FANCA and FANCC genes in Brazilian patients with Fanconi anaemiapt_BR
dc.typeArtigopt_BR
dc.subject.keywordAnemia de Fanconipt_BR
dc.subject.keywordTeste debpt_BR
dc.subject.keywordDiagnóstico molecularpt_BR
dc.identifier.doihttps://dx.doi.org/10.1590/S1415-47572005000200004pt_BR
dc.description.unidadeEm processamento-
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