Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients

INTRODUCTION: 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 activ...

Descripción completa

Detalles Bibliográficos
Autores principales: Borsatto, Taciane, Sperb-Ludwig, Fernanda, Lima, Samyra E., S. Carvalho, Maria R., S. Fonseca, Pablo A., S. Camelo, José, M. Ribeiro, Erlane, F. V. de Medeiros, Paula, M. Lourenço, Charles, F. M. de Souza, Carolina, Boy, Raquel, Félix, Têmis M., M. Bittar, Camila, L. C. Pinto, Louise, C. Neto, Eurico, J. Blom, Henk, D. Schwartz, Ida V.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5428951/
https://www.ncbi.nlm.nih.gov/pubmed/28498829
http://dx.doi.org/10.1371/journal.pone.0177503
_version_ 1783235937591885824
author Borsatto, Taciane
Sperb-Ludwig, Fernanda
Lima, Samyra E.
S. Carvalho, Maria R.
S. Fonseca, Pablo A.
S. Camelo, José
M. Ribeiro, Erlane
F. V. de Medeiros, Paula
M. Lourenço, Charles
F. M. de Souza, Carolina
Boy, Raquel
Félix, Têmis M.
M. Bittar, Camila
L. C. Pinto, Louise
C. Neto, Eurico
J. Blom, Henk
D. Schwartz, Ida V.
author_facet Borsatto, Taciane
Sperb-Ludwig, Fernanda
Lima, Samyra E.
S. Carvalho, Maria R.
S. Fonseca, Pablo A.
S. Camelo, José
M. Ribeiro, Erlane
F. V. de Medeiros, Paula
M. Lourenço, Charles
F. M. de Souza, Carolina
Boy, Raquel
Félix, Têmis M.
M. Bittar, Camila
L. C. Pinto, Louise
C. Neto, Eurico
J. Blom, Henk
D. Schwartz, Ida V.
author_sort Borsatto, Taciane
collection PubMed
description INTRODUCTION: 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. RESULTS: 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. CONCLUSIONS: 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.
format Online
Article
Text
id pubmed-5428951
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-54289512017-05-26 Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients Borsatto, Taciane Sperb-Ludwig, Fernanda Lima, Samyra E. S. Carvalho, Maria R. S. Fonseca, Pablo A. S. Camelo, José M. Ribeiro, Erlane F. V. de Medeiros, Paula M. Lourenço, Charles F. M. de Souza, Carolina Boy, Raquel Félix, Têmis M. M. Bittar, Camila L. C. Pinto, Louise C. Neto, Eurico J. Blom, Henk D. Schwartz, Ida V. PLoS One Research Article INTRODUCTION: 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. RESULTS: 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. CONCLUSIONS: 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. Public Library of Science 2017-05-12 /pmc/articles/PMC5428951/ /pubmed/28498829 http://dx.doi.org/10.1371/journal.pone.0177503 Text en © 2017 Borsatto et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Borsatto, Taciane
Sperb-Ludwig, Fernanda
Lima, Samyra E.
S. Carvalho, Maria R.
S. Fonseca, Pablo A.
S. Camelo, José
M. Ribeiro, Erlane
F. V. de Medeiros, Paula
M. Lourenço, Charles
F. M. de Souza, Carolina
Boy, Raquel
Félix, Têmis M.
M. Bittar, Camila
L. C. Pinto, Louise
C. Neto, Eurico
J. Blom, Henk
D. Schwartz, Ida V.
Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients
title Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients
title_full Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients
title_fullStr Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients
title_full_unstemmed Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients
title_short Biotinidase deficiency: Genotype-biochemical phenotype association in Brazilian patients
title_sort biotinidase deficiency: genotype-biochemical phenotype association in brazilian patients
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5428951/
https://www.ncbi.nlm.nih.gov/pubmed/28498829
http://dx.doi.org/10.1371/journal.pone.0177503
work_keys_str_mv AT borsattotaciane biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT sperbludwigfernanda biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT limasamyrae biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT scarvalhomariar biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT sfonsecapabloa biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT scamelojose biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT mribeiroerlane biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT fvdemedeirospaula biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT mlourencocharles biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT fmdesouzacarolina biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT boyraquel biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT felixtemism biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT mbittarcamila biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT lcpintolouise biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT cnetoeurico biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT jblomhenk biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients
AT dschwartzidav biotinidasedeficiencygenotypebiochemicalphenotypeassociationinbrazilianpatients

Ejemplares similares