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Título
Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients
dc.contributorFacultad de Veterinariaes_ES
dc.contributor.authorBorsatto, Taciane
dc.contributor.authorSperb-Ludwig, Fernanda
dc.contributor.authorLima, Samyra E.
dc.contributor.authorCarvalho, María R.S.
dc.contributor.authorDe Souza Fonseca, Pablo Augusto
dc.contributor.authorCamelo, José S.
dc.contributor.authorRibeiro, Erlane M.
dc.contributor.authorDe Medeiros, Paula F. V.
dc.contributor.authorLourenço, Charles M.
dc.contributor.authorDe Souza, Carolina F. M.
dc.contributor.authorBoy, Raquel
dc.contributor.authorFélix, Têmis M.
dc.contributor.authorBittar, Camila M.
dc.contributor.authorPinto, Louise L. C.
dc.contributor.authorNeto, Eurico C.
dc.contributor.authorBlom, Henk J.
dc.contributor.authorSchwartz, Ida V. D.
dc.contributor.otherProducción Animales_ES
dc.date2017
dc.date.accessioned2024-01-31T08:11:55Z
dc.date.available2024-01-31T08:11:55Z
dc.identifier.citationBorsatto, T., Sperb-Ludwig, F., Lima, S. E., Carvalho, M. R. S., Fonseca, P. A. S., Camelo, J. S., Ribeiro, E. M., De Medeiros, P. F. V., Lourenço, C. M., De Souza, C. F. M., Boy, R., Félix, T. M., Bittar, C. M., Pinto, L. L. C., Neto, E. C., Blom, H. J., & Schwartz, I. V. D. (2017). Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients. PLoS ONE, 12(5). https://doi.org/10.1371/JOURNAL.PONE.0177503es_ES
dc.identifier.otherhttps://journals.plos.org/plosone/article?id=10.1371/journal.pone.0177503es_ES
dc.identifier.urihttps://hdl.handle.net/10612/17935
dc.description.abstract[EN] The association between the BTD genotype and biochemical phenotype [profound biotinidase deficiency (BD), partial BD or heterozygous activity] is not always consistent. This study aimed to investigate the genotype-biochemical phenotype association in patients with low biotinidase activity. Methods All exons, the 5'UTR and the promoter of the BTD gene were sequenced in 72 Brazilian individuals who exhibited low biotinidase activity. For each patient, the expected biochemical phenotype based on the known genotype was compared with the observed biochemical phenotype. Additional non-genetic factors that could affect the biotinidase activity were also analysed. Most individuals were identified by neonatal screening (n = 66/72). When consecutive results for the same patient were compared, age, prematurity and neonatal jaundice appeared to affect the level of biotinidase activity. The biochemical phenotype at the time of the second blood collection changed in 11/22 patients compared to results from the first sample. Three novel variants were found: c.1337T>C (p.L446P), c.1466A>G (p.N489S) and c.962G>A (p.W321*). Some patients with the same genotype presented different biochemical phenotypes. The expected and observed biochemical phenotypes agreed in 68.5% of cases (concordant patients). The non-coding variants c.-183G>A, c.-315A>G and c.-514C>T were present in heterozygosis in 5/17 discordant patients. In addition, c.- 183G>A and c.-514C>T were also present in 10/37 concordant patients. The variants found in the promoter region do not appear to have a strong impact on biotinidase activity. Since there is a disparity between the BTD genotype and biochemical phenotype, and biotinidase activity may be affected by both genetic and non-genetic factors, we suggest that the diagnosis of BD should be based on more than one measurement of plasma biotinidase activity. DNA analysis can be of additional relevance to differentiate between partial BD and heterozygosity.es_ES
dc.languageenges_ES
dc.publisherPloses_ES
dc.rightsAttribution-NonCommercial-NoDerivatives 4.0 Internacional*
dc.rights.urihttp://creativecommons.org/licenses/by-nc-nd/4.0/*
dc.subjectGenéticaes_ES
dc.subject.otherBiotinidasees_ES
dc.subject.otherGenotypinges_ES
dc.subject.otherMutationses_ES
dc.subject.otherHumanes_ES
dc.titleBiotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patientses_ES
dc.typeinfo:eu-repo/semantics/articlees_ES
dc.identifier.doi10.1371/journal.pone.0177503
dc.description.peerreviewedSIes_ES
dc.rights.accessRightsinfo:eu-repo/semantics/openAccesses_ES
dc.identifier.essn1932-6203
dc.journal.titlePLOS ONEes_ES
dc.volume.number12es_ES
dc.issue.number5es_ES
dc.page.initiale0177503es_ES
dc.type.hasVersioninfo:eu-repo/semantics/publishedVersiones_ES
dc.subject.unesco32 Ciencias Médicases_ES
dc.subject.unesco2409 Genéticaes_ES
dc.description.projectThis study received financial support from Fundo de Incentivo à Pesquisa e Eventos/Hospital de Clínicas de Porto Alegre (FIPE-HCPA) for research materials and publication fee. Post Graduate Program in Genetics and Molecular Biology (Universidade Federal do Rio Grande do Sul) funded the translation. ECN has a commercial affiliation (CTN Diagnósticos) which did not have any role or financial contribution to this research. TB have fellowship from the Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (Capes). FS had fellowship from the Fundação de Amparo à Pesquisa do Estado do Rio Grande do Sul (FAPERGS). IVDS, MRSC and PASF have fellowships from the Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq). HB receives a research grant of Orphan Europe. The funders did no provide support in the form of salaries for any author, and did not have any additional role in the study design, data collection and analysis, decision to publish, or preparation of the manuscript. The specific roles of these authors are articulated in the ‘author contributions’ section.es_ES


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