Novel splice site IDUA gene mutation in Tunisian pedigrees with hurler syndrome.

Chkioua, Latifa; Boudabous, Hela; Jaballi, Ibtissem; Grissa, Oussama; Turkia, Hadhami Ben; Tebib, Neji; Laradi, Sandrine

Chkioua, Latifa; Boudabous, Hela; Jaballi, Ibtissem; Grissa, Oussama; Turkia, Hadhami Ben; Tebib, Neji; Laradi, Sandrine.

Afiliação

Chkioua L; Faculty of pharmacy, University of Monastir, 5000, Monastir, Tunisia. chkioualatifa2002@yahoo.fr.
Boudabous H; Faculty of pharmacy of Monastir, University of Monastir, Avenue Avicenne, 5019, Monastir, Tunisia. chkioualatifa2002@yahoo.fr.
Jaballi I; La Rabta Hospital, 1007, Tunis, Tunisia.
Grissa O; Faculty of pharmacy, University of Monastir, 5000, Monastir, Tunisia.
Turkia HB; Faculty of pharmacy, University of Monastir, 5000, Monastir, Tunisia.
Tebib N; La Rabta Hospital, 1007, Tunis, Tunisia.
Laradi S; La Rabta Hospital, 1007, Tunis, Tunisia.

Diagn Pathol ; 13(1): 35, 2018 May 29.

Article em En | MEDLINE | ID: mdl-29843745

ABSTRACT

ABSTRACT

BACKGROUND:

The mucopolysaccharidosis type I (MPS I) is a lysosomal storage disease resulting from the defective activity of the enzyme α-L-iduronidase (IDUA). The disease has three major clinical subtypes (severe Hurler syndrome, intermediate Hurler-Scheie syndrome and attenuated Scheie syndrome). We aim to identify the genetic variants in MPS I patients and to investigate the effect of the novel splice site mutation on splicing of IDUA- mRNA variability using bioinformatics tools.

METHODS:

The IDUA mutations were determined in four MPS I patients from four families from Northern Tunisia, by amplifying and sequencing each of the IDUA exons and intron-exon junctions.

RESULTS:

One novel splice site IDUA mutation, c.1650 + 1G > T in intron 11 and two previously reported mutations, p.A75T and p.R555H, were detected. The patients in families 1 and 2 who have the Hurler phenotype were homozygotes for the novel splice site mutation c.1650 + 1G > T. The patient in family 3, who also had the Hurler phenotype, was a compound heterozygote for the novel splice site mutation c.1650 + 1G > T and for the previously reported missense mutation p.A75T. The patient in family 4 who had the Hurler-Scheie phenotype was a compound heterozygote for the novel splice site mutation c.1650 + 1G > T and for the previously reported missense mutation p.R555H. In addition, four known IDUA polymorphisms were identified. Bioinformatics tools allowed us to associate the variant c.1650 + 1G > T with the severe clinical phenotype of MPS I. This variant affects the essential nucleotide + 1 (G to T) of the donor splice site of IDUA intron 11. The G > T in intron 11 leads to wild type donor site broken with minus 19.97% value compared to normal value with 0%, hence the new splice site acceptor has plus 5.59%.

CONCLUSIONS:

The present findings indicate that the identified mutations facilitate the accurate carrier detection (genetic counseling of at-risk relatives) and the molecular prenatal diagnosis in Tunisia.

Assuntos

Iduronidase/genética; Mucopolissacaridose I/genética; Criança; Pré-Escolar; Feminino; Humanos; Masculino; Mutação; Linhagem; Tunísia

Palavras-chave

Compound heterozygote; Homozygous; Mucopolysaccharidosis type I; Splice site mutation; α-L-iduronidase

Texto completo

Imprimir

XML

PubMed Links

Buscar no Google

Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Mucopolissacaridose I / Iduronidase Tipo de estudo: Prognostic_studies Limite: Child / Child, preschool / Female / Humans / Male País/Região como assunto: Africa Idioma: En Ano de publicação: 2018 Tipo de documento: Article

Texto completo

Imprimir

XML

PubMed Links

Buscar no Google