Genotype–phenotype associations in a large
            <i>PRPH2</i>
            ‐related retinopathy cohort

Reeves, Melissa; Goetz, Kerry; Guan, Bin; Ullah, Ehsan; Blain, Delphine; Zein, Wadih M.; Tumminia, Santa J.; Hufnagel, Robert B.

doi:10.1002/humu.24065

Cited by 20 publications

(25 citation statements)

References 50 publications

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“…Previous reports have suggested association between the location of the variant in PRPH2 and clinical phenotype. Specifically, variants are mostly found in the D2 loop [13,43,[46][47][48], which is critical for protein-protein interactions. Variants that cause autosomal dominant RP tend to accumulate between Lys193 and Glu226 [3].…”

Section: Discussionmentioning

confidence: 99%

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Genetic and Phenotypic Landscape of PRPH2-Associated Retinal Dystrophy in Japan

Oishi

Fujinami

Mawatari

et al. 2021

Genes

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Peripherin-2 (PRPH2) is one of the causative genes of inherited retinal dystrophy. While the gene is relatively common in Caucasians, reports from Asian ethnicities are limited. In the present study, we report 40 Japanese patients from 30 families with PRPH2-associated retinal dystrophy. We identified 17 distinct pathogenic or likely pathogenic variants using next-generation sequencing. Variants p.R142W and p.V200E were relatively common in the cohort. The age of onset was generally in the 40’s; however, some patients had earlier onset (age: 5 years). Visual acuity of the patients ranged from hand motion to 1.5 (Snellen equivalent 20/13). The patients showed variable phenotypes such as retinitis pigmentosa, cone-rod dystrophy, and macular dystrophy. Additionally, intrafamilial phenotypic variability was observed. Choroidal neovascularization was observed in three eyes of two patients with retinitis pigmentosa. The results demonstrate the genotypic and phenotypic variations of the disease in the Asian cohort.

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Section: Discussionmentioning

confidence: 99%

“…Particularly, missense mutations in Pro210 to Pro216 cause autosomal dominant RP [3]. Patients diagnosed with CRD, RP, and STGD tend to have variants in exon 1, whereas patients with Best disease and pattern dystrophy tend to have variants in exon 2 [13,43]. Patients with p.Arg172Trp present earlier onset than those with other alleles [43].…”

Section: Discussionmentioning

confidence: 99%

Genetic and Phenotypic Landscape of PRPH2-Associated Retinal Dystrophy in Japan

Oishi

Fujinami

Mawatari

et al. 2021

Genes

View full text Add to dashboard Cite

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“…3 a) [36] . PRPH2 disease has genetic and phenotypic heterogeneity [36 , 37 , 46] . In CORD patients, mutations are most often associated with autosomal dominant inheritance [36 , 46] .…”

Section: Genes and Disease Mechanismsmentioning

confidence: 99%

“…PRPH2 disease has genetic and phenotypic heterogeneity [36 , 37 , 46] . In CORD patients, mutations are most often associated with autosomal dominant inheritance [36 , 46] . Although genotype-phenotype correlations have been elusive, the majority of PRPH2 -CORD patients have mutations in exon 1, and the D2 loop of the protein, important for mediating protein-protein interactions, is a mutational hotspot in exon 1.…”

Section: Genes and Disease Mechanismsmentioning

confidence: 99%

“…Although genotype-phenotype correlations have been elusive, the majority of PRPH2 -CORD patients have mutations in exon 1, and the D2 loop of the protein, important for mediating protein-protein interactions, is a mutational hotspot in exon 1. Additionally, p.Arg172Trp, a common mutation in PRPH2 that can cause a disease with early cone involvement, is generally associated with earlier age of onset compared to other PRPH2 variants [46] .…”

Section: Genes and Disease Mechanismsmentioning

confidence: 99%

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Childhood-onset genetic cone-rod photoreceptor diseases and underlying pathobiology

et al. 2021

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PRPH2 mutation update: In silico assessment of 245 reported and 7 novel variants in patients with retinal disease

et al. 2021

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Mutations in PRPH2, encoding peripherin‐2, are associated with the development of a wide variety of inherited retinal diseases (IRDs). To determine the causality of the many PRPH2 variants that have been discovered over the last decades, we surveyed all published PRPH2 variants up to July 2020, describing 720 index patients that in total carried 245 unique variants. In addition, we identified seven novel PRPH2 variants in eight additional index patients. The pathogenicity of all variants was determined using the ACMG guidelines. With this, 107 variants were classified as pathogenic, 92 as likely pathogenic, one as benign, and two as likely benign. The remaining 50 variants were classified as variants of uncertain significance. Interestingly, of the total 252 PRPH2 variants, more than half (n = 137) were missense variants. All variants were uploaded into the Leiden Open source Variation and ClinVar databases. Our study underscores the need for experimental assays for variants of unknown significance to improve pathogenicity classification, which would allow us to better understand genotype‐phenotype correlations, and in the long‐term, hopefully also support the development of therapeutic strategies for patients with PRPH2‐associated IRD.

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Genotype–phenotype associations in a large PRPH2 ‐related retinopathy cohort

Cited by 20 publications

References 50 publications

Genetic and Phenotypic Landscape of PRPH2-Associated Retinal Dystrophy in Japan

Genetic and Phenotypic Landscape of PRPH2-Associated Retinal Dystrophy in Japan

Childhood-onset genetic cone-rod photoreceptor diseases and underlying pathobiology

PRPH2 mutation update: In silico assessment of 245 reported and 7 novel variants in patients with retinal disease

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