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The clinical and mutational spectrum of B3GAT3 linkeropathy: two case reports and literature review

Authors :
Brecht Guillemyn
Fransiska Malfait
Sofie Symoens
Delfien Syx
Elisabeth Steichen-Gersdorf
Sheela Nampoothiri
Franco Laccone
Marlies Colman
Tim Van Damme
Source :
Orphanet Journal of Rare Diseases, ORPHANET JOURNAL OF RARE DISEASES, Orphanet Journal of Rare Diseases, Vol 14, Iss 1, Pp 1-10 (2019)
Publication Year :
2019
Publisher :
BioMed Central, 2019.

Abstract

Background Proteoglycans are large and structurally complex macromolecules which can be found in abundancy in the extracellular matrix and on the surface of all animal cells. Mutations in the genes encoding the enzymes responsible for the formation of the tetrasaccharide linker region between the proteoglycan core protein and the glycosaminoglycan side chains lead to a spectrum of severe and overlapping autosomal recessive connective tissue disorders, collectively coined the ‘glycosaminoglycan linkeropathies’. Results We report the clinical findings of two novel patients with a complex linkeropathy due to biallelic mutations in B3GAT3, the gene that encodes glucuronosyltransferase I, which catalyzes the addition of the ultimate saccharide to the linker region. We identified a previously reported c.667G > A missense mutation and an unreported homozygous c.416C > T missense mutation. We also performed a genotype and phenotype-oriented literature overview of all hitherto reported patients harbouring B3GAT3 mutations. A total of 23 patients from 10 families harbouring bi-allelic mutations and one patient with a heterozygeous splice-site mutation in B3GAT3 have been reported. They all display a complex phenotype characterized by consistent presence of skeletal dysplasia (including short stature, kyphosis, scoliosis and deformity of the long bones), facial dysmorphology, and spatulate distal phalanges. More variably present are cardiac defects, joint hypermobility, joint dislocations/contractures and fractures. Seven different B3GAT3 mutations have been reported, and although the number of patients is still limited, some phenotype-genotype correlations start to emerge. The more severe phenotypes seem to have mutations located in the substrate acceptor subdomain of the catalytic domain of the glucuronosyltransferase I protein while more mildly affected phenotypes seem to have mutations in the NTP-sugar donor substrate binding subdomain. Conclusions Loss-of-function mutations in B3GAT3 are associated with a complex connective tissue phenotype characterized by disproportionate short stature, skeletal dysplasia, facial dysmorphism, spatulate distal phalanges and -to a lesser extent- joint contractures, joint hypermobility with dislocations, cardiac defects and bone fragility. Based on the limited number of reported patients, some genotype-phenotype correlations start to emerge.

Details

Language :
English
ISSN :
17501172
Volume :
14
Database :
OpenAIRE
Journal :
Orphanet Journal of Rare Diseases
Accession number :
edsair.doi.dedup.....b4e0200b4f42aac1e9c39b28fe1ca22b