| Literature DB >> 29659094 |
Isabelle Audo1,2,3, Saddek Mohand-Said1,2, Elise Boulanger-Scemama1,4, Xavier Zanlonghi5, Christel Condroyer1, Vanessa Démontant1, Fiona Boyard1, Aline Antonio1, Cécile Méjécase1, Said El Shamieh1,6, José-Alain Sahel1,2,3,4,7,8, Christina Zeitz1.
Abstract
MER tyrosine kinase (MERTK) encodes a surface receptor localized at the apical membrane of the retinal pigment epithelium. It plays a critical role in photoreceptor outer segment internalization prior to phagocytosis. Mutations in MERTK have been associated with severe autosomal recessive retinal dystrophies in the RCS rat and in humans. We present here a comprehensive review of all reported MERTK disease causing variants with the associated phenotype. In addition, we provide further data and insights of a large cohort of 1,195 inherited retinal dystrophies (IRD) index cases applying state-of-the-art genotyping techniques and summarize current knowledge. A total of 79 variants have now been identified underlying rod-cone dystrophy and cone-rod dystrophy including 11 novel variants reported here. The mutation spectrum in MERTK includes 33 missense, 12 nonsense, 12 splice defects, 12 small deletions, two small insertion-deletions, three small duplications, and two exonic and three gross deletions. Altogether, mutations in MERTK account for ∼2% of IRD cases with a severe retinal phenotype. These data are important for current and future therapeutic trials including gene replacement therapy or cell-based therapy.Entities:
Keywords: MERTK; inherited retinal dystrophy; mutation prevalence; mutation spectrum
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Year: 2018 PMID: 29659094 DOI: 10.1002/humu.23431
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878