1. Expanding the phenotypic spectrum in RDH12-associated retinal disease
- Author
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Shizuo Mukai, Kevin Ferenchak, Rachel M. Huckfeldt, Erin Zampaglione, Naomi E Wagner, Hilary A Scott, Emily Place, Kinga M. Bujakowska, Katherine R. Chao, Stephanie DiTroia, Eric A. Pierce, and Daniel Navarro-Gomez
- Subjects
Retinal degeneration ,Research Report ,Male ,genetic structures ,chemistry.chemical_compound ,0302 clinical medicine ,cone-rod dystrophy ,Child ,Genetics ,0303 health sciences ,macular dystrophy ,medicine.diagnostic_test ,Optical Imaging ,severe visual impairment ,General Medicine ,Macular dystrophy ,Pedigree ,Phenotype ,Child, Preschool ,Female ,Tomography, Optical Coherence ,Adult ,Retinal Disorder ,Adolescent ,Biology ,pigmentary retinal degeneration ,03 medical and health sciences ,Young Adult ,Retinal Diseases ,Retinitis pigmentosa ,Exome Sequencing ,medicine ,Humans ,Genetic Predisposition to Disease ,Allele ,Alleles ,Genetic Association Studies ,030304 developmental biology ,Genetic testing ,progressive visual field defects ,Dystrophy ,Retinal ,medicine.disease ,central scotoma ,Alcohol Oxidoreductases ,progressive central visual loss ,chemistry ,Amino Acid Substitution ,peripheral visual field loss ,Genetic Loci ,Mutation ,030221 ophthalmology & optometry - Abstract
Retinol dehydrogenase 12, RDH12, plays a pivotal role in the visual cycle to ensure the maintenance of normal vision. Alterations in activity of this protein result in photoreceptor death and decreased vision beginning at an early age and progressing to substantial vision loss later in life. Here we describe 11 patients with retinal degeneration that underwent next-generation sequencing (NGS) with a targeted panel of all currently known inherited retinal degeneration (IRD) genes and whole-exome sequencing to identify the genetic causality of their retinal disease. These patients display a range of phenotypic severity prompting clinical diagnoses of macular dystrophy, cone-rod dystrophy, retinitis pigmentosa, and early-onset severe retinal dystrophy all attributed to biallelic recessive mutations in RDH12. We report 15 causal alleles and expand the repertoire of known RDH12 mutations with four novel variants: c.215A > G (p.Asp72Gly); c.362T > C (p.Ile121Thr); c.440A > C (p.Asn147Thr); and c.697G > A (p.Val233Ille). The broad phenotypic spectrum observed with biallelic RDH12 mutations has been observed in other genetic forms of IRDs, but the diversity is particularly notable here given the prior association of RDH12 primarily with severe early-onset disease. This breadth emphasizes the importance of broad genetic testing for inherited retinal disorders and extends the pool of individuals who may benefit from imminent gene-targeted therapies.
- Published
- 2020