Splice site variants in the canonical donor site of <i>MED13L</i> exon 7 lead to intron retention in patients with <i>MED13L</i> syndrome. - Université de Lille
Article Dans Une Revue Journal of Medical Genetics Année : 2024

Splice site variants in the canonical donor site of MED13L exon 7 lead to intron retention in patients with MED13L syndrome.

Résumé

Pathogenic variants in the MED13L gene are associated with the autosomal dominant MED13L syndrome, which is characterised by global developmental delay and cardiac malformations. We investigated two heterozygous MED13L variants located at the canonical donor splice site motif of exon 7: c.1009+1G>C and c.1009+5G>C. We report that in silico predictions suggested two possible outcomes: exon 7 skipping, resulting in loss of the phosphodegron motif essential for MED13L regulation, or activation of a cryptic donor site in intron 7, leading to intron retention. RNA analysis confirmed that both variants affected the exon 7 splice donor site, resulting in the retention of 73 bp of intron 7. This retention caused a frameshift and premature translation termination, consistent with haploinsufficiency. Our results highlight the importance of combining predictive and experimental approaches to understand the functional impact of splice site variants. These insights into the molecular consequences of MED13L variants provide a deeper understanding of the genetic basis of MED13L syndrome.
Fichier non déposé

Dates et versions

hal-04717914 , version 1 (02-10-2024)

Identifiants

Citer

Jade Fauqueux, Simon Boussion, Caroline Thuillier, Evine Meurisse, Didier Lacombe, et al.. Splice site variants in the canonical donor site of MED13L exon 7 lead to intron retention in patients with MED13L syndrome.. Journal of Medical Genetics, 2024, J Med Genet, ⟨10.1136/jmg-2024-110154⟩. ⟨hal-04717914⟩

Collections

UNIV-LILLE
17 Consultations
0 Téléchargements

Altmetric

Partager

More