Targeted Next Generation Sequencing Identifies Novel Mutations in RP1 as a Relatively Common Cause of Autosomal Recessive Rod-Cone Dystrophy - Inserm - Institut national de la santé et de la recherche médicale Accéder directement au contenu
Article Dans Une Revue BioMed Research International Année : 2015

Targeted Next Generation Sequencing Identifies Novel Mutations in RP1 as a Relatively Common Cause of Autosomal Recessive Rod-Cone Dystrophy

Said El Shamieh
Institut de la Vision
Elise Boulanger-Scemama
  • Fonction : Auteur
Institut de la Vision
Marie-Elise Lancelot
  • Fonction : Auteur
Institut de la Vision
Aline Antonio
  • Fonction : Auteur
Institut de la Vision
Vanessa Démontant
  • Fonction : Auteur
Institut de la Vision
Christel Condroyer
  • Fonction : Auteur
  • PersonId : 938769
Institut de la Vision
Mélanie Letexier
  • Fonction : Auteur
  • PersonId : 925185
IntegraGen SA
Jean-Paul Saraiva
  • Fonction : Auteur
IntegraGen SA
Saddek Mohand-Saïd
  • Fonction : Auteur
Institut de la Vision
José-Alain Sahel
Académie des sciences [Paris, France]
Institute of Ophthalmology
Institut de la Vision
Isabelle Audo
Connectez-vous pour contacter l'auteur
Institut de la Vision
Institute of Ophthalmology
Christina Zeitz
Connectez-vous pour contacter l'auteur
Institut de la Vision

Résumé

We report ophthalmic and genetic findings in families with autosomal recessive rod-cone dystrophy (arRCD) and RP1 mutations. Detailed ophthalmic examination was performed in 242 sporadic and arRCD subjects. Genomic DNA was investigated using our customized next generation sequencing panel targeting up to 123 genes implicated in inherited retinal disorders. Stringent filtering coupled with Sanger sequencing and followed by cosegregation analysis was performed to confirm biallelism and the implication of the most likely disease causing variants. Sequencing identified 9 RP1 mutations in 7 index cases. Eight of the mutations were novel, and all cosegregated with severe arRCD phenotype, found associated with additional macular changes. Among the identified mutations, 4 belong to a region, previously associated with arRCD, and 5 others in a region previously associated with adRCD. Our prevalence studies showed that RP1 mutations account for up to 2.5% of arRCD. These results point out for the necessity of sequencing RP1 when genetically investigating sporadic and arRCD. It further highlights the interest of unbiased sequencing technique, which allows investigating the implication of the same gene in different modes of inheritance. Finally, it reports that different regions of RP1 can also lead to arRCD.

Domaines

Organes des sens
Fichier principal
Vignette du fichier
485624.pdf (1.77 Mo) Télécharger le fichier
Origine : Publication financée par une institution

Gestionnaire HAL-UPMC  : Connectez-vous pour contacter le contributeur

https://hal.sorbonne-universite.fr/hal-01211446

Soumis le : lundi 5 octobre 2015-10:39:03

Dernière modification le : mardi 9 avril 2024-10:43:10

Archivage à long terme le : mercredi 6 janvier 2016-10:25:47

Télécharger pour visualiser

Dates et versions

hal-01211446 , version 1 (05-10-2015)

Licence

Paternité

Identifiants

Citer

Said El Shamieh, Elise Boulanger-Scemama, Marie-Elise Lancelot, Aline Antonio, Vanessa Démontant, et al.. Targeted Next Generation Sequencing Identifies Novel Mutations in RP1 as a Relatively Common Cause of Autosomal Recessive Rod-Cone Dystrophy. BioMed Research International , 2015, 2015, pp.485624. ⟨10.1155/2015/485624⟩. ⟨hal-01211446⟩

Exporter

BibTeX XML-TEI Dublin Core DC Terms EndNote DataCite

Collections

INSERM UPMC CNRS U968 SORBONNE-UNIVERSITE SU-MEDECINE
219 Consultations
150 Téléchargements

Altmetric

Partager

Gmail Facebook X LinkedIn More