Afficher la couverture 'Alpha-mannosidosis in Tunisian consanguineous families: Potential involvement of variants in GHR and SLC19A3 genes in the variable expressivity of cognitive impairment | Mkaouar, Rahma' en grand format
/5

0 avis

Alpha-mannosidosis in Tunisian consanguineous families: Potential involvement of variants in GHR and SLC19A3 genes in the variable expressivity of cognitive impairment

Archive ouverte

Mkaouar, Rahma | Riahi, Zied | Charfeddine, Cherine | Chelly, Imen | Boudabbous, Hela | Dallali, Hamza | Bonnet, Crystel | Hechmi, Meriem | Bekri, Soumeya | Zitouna, Nadia | Zekri, Lotfi | Tounsi, Amel | Kefi, Rym | Marrakchi, Jihene | Messaoud, Olfa | Kraoua, Ichraf | Maalej, Sonia | Turki Ben Youssef, Ilhem | Ben Hmid, Ahlem | Giraudet, Fabrice | Bouchoucha, Sami | Tebib, Neji | Besbes, Ghazi | Petit, Christine | Mrad, Ridha | Abdelhak, Sonia | Trabelsi, Mediha

Edité par CCSD ; Public Library of Science -

International audience. Alpha-Mannosidosis (AM) is an ultra-rare storage disorder caused by a deficiency of lysosomal alpha-mannosidase encoded by the MAN2B1 gene. Clinical presentation of AM includes mental retardation, recurrent infections, hearing loss, dysmorphic features, and motor dysfunctions. AM has never been reported in Tunisia. We report here the clinical and genetic study of six patients from two Tunisian families with AM. The AM diagnosis was confirmed by an enzymatic activity assay. Genetic investigation was conducted by Sanger sequencing of the mutational hotspots for the first family and by ES analysis for the second one. In the first family, a frameshift duplication p.(Ser802GlnfsTer129) was identified in the MAN2B1 gene. For the second family, ES analysis led to the identification of a missense mutation p.(Arg229Trp) in the MAN2B1 gene in four affected family members. The p.(Ser802GlnfsTer129) mutation induces a premature termination codon which may trigger RNA degradation by the NMD system. The decrease in the levels of MAN2B1 synthesis could explain the severe phenotype observed in the index case. According to the literature, the p.(Arg229Trp) missense variant does not have an impact on MAN2B1 maturation and transportation, which correlates with a moderate clinical sub-type. To explain the intra-familial variability of cognitive impairment, exome analysis allowed the identification of two likely pathogenic variants in GHR and SLC19A3 genes potentially associated to cognitive decline. The present study raises awareness about underdiagnosis of AM in the region that deprives patients from accessing adequate care. Indeed, early diagnosis is critical in order to prevent disease progression and to propose enzyme replacement therapy.

Suggestions

Du même auteur

Current phenotypic and genetic spectrum of syndromic deafness in Tunisia: paving the way for precision auditory health

Archive ouverte | Mkaouar, Rahma | CCSD

International audience. Hearing impairment (HI) is a prevalent neurosensory condition globally, impacting 5% of the population, with over 50% of congenital cases attributed to genetic etiologies. In Tunisia, HI unde...

Corrigendum: Current phenotypic and genetic spectrum of syndromic deafness in Tunisia: paving the way for precision auditory health

Archive ouverte | Mkaouar, Rahma | CCSD

International audience. [This corrects the article DOI: 10.3389/fgene.2024.1384094.].

A Tunisian family with a novel mutation in the gene CYP 4F22 for lamellar ichthyosis and co‐occurrence of hearing loss in a child due to mutation in the SLC 26A4 gene

Archive ouverte | Sayeb, Marwa | CCSD

International audience. Background: Co-occurrence of two genetic diseases is challenging for accurate diagnosis and genetic counseling. The recent availability of whole exome sequencing (WES) has dramatically improv...

Chargement des enrichissements...