Reanalysis of Association of Pro50Leu Substitution in Guanylate Cyclase Activating Protein-1 With Dominant Retinal Dystrophy

Mahroo, Omar A.; Arno, Gavin; Ba-Abbad, Rola; Downes, Susan M.; Bird, Alan C.; Webster, Andrew R.

doi:10.1001/jamaophthalmol.2019.4959

Cited by 7 publications

(2 citation statements)

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“…In order to fully refute false attributions of pathogenicity to particular genetic variants, it is important to identify the correct pathogenic variant in the original cases. 1 – 3 …”

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confidence: 99%

Dominant Cone Rod Dystrophy, Previously Assigned to a Missense Variant in RIMS1, Is Fully Explained by Co-Inheritance of a Dominant Allele of PROM1

Martin-Gutierrez

Schiff

Wright

et al. 2022

Invest. Ophthalmol. Vis. Sci.

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Purpose Autosomal dominant cone rod dystrophy 7 (CORD7) was initially linked to the gene RIMS1 and reported in a 4-generation British family in 1998. The purpose of this study was to investigate the legitimacy of this association, and to correctly characterize the genetic cause of this condition. Methods The allele frequency of RIMS1 c.2459G>A, p.Arg820His, was investigated in the Genomes Aggregation Dataset (gnomAD) datasets and whole genome sequencing (WGS) was performed for 4 members of the CORD7 family with filtering of rare pathogenic variants in a virtual gene panel comprising all genes known to be associated with inherited retinal dystrophy (IRD). Cytogenetic analysis was performed to rule out interchromosomal translocation. Results RIMS1 p.Arg820His has a maximal carrier frequency of >1:5000 in Europeans. A previously well-characterized PROM1 variant: c.1118C>T, p.Arg373Cys, was detected in 9 affected members of the CORD7 family who underwent WGS or direct sequencing. One affected family member is now known to have macular dystrophy in the absence of RIMS1 p.Arg820His. Clinical analysis of affected family members and 27 individuals with retinopathy associated with the same – PROM1 – variant showed consistent phenotypes. Conclusions The case for pathogenicity of RIMS1 p.Arg820His is not strong based on its presence on 10 alleles in the gnomAD dataset and absence from additional CORD affected individuals. The finding of a known pathogenic variant in PROM1 correlates well with the phenotypic characteristics of the affected individuals, and is likely to account for the condition. Clear evidence of association between RIMS1 and a retinal dystrophy is yet to be described.

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“…In order to fully refute false attributions of pathogenicity to particular genetic variants, it is important to identify the correct pathogenic variant in the original cases. 1 – 3 …”

mentioning

confidence: 99%

Dominant Cone Rod Dystrophy, Previously Assigned to a Missense Variant in RIMS1, Is Fully Explained by Co-Inheritance of a Dominant Allele of PROM1

Martin-Gutierrez

Schiff

Wright

et al. 2022

Invest. Ophthalmol. Vis. Sci.

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“…In the Brief Report titled “Reanalysis of Association of Pro50Leu Substitution in Guanylate Cyclase Activating Protein-1 With Dominant Retinal Dystrophy,” published in the February issue of JAMA Ophthalmology , the authors updated the status of the article so that it is now Open Access. This article has been corrected online.…”

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confidence: 99%

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2020

JAMA Ophthalmol

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Establishment of the Clinical Genome Resource (ClinGen) X-Linked Inherited Retinal Disease Variant Curation Expert Panel

Huang,

Wang,

Lee

et al. 2024

Essentials in Ophthalmology

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Reanalysis of Association of Pro50Leu Substitution in Guanylate Cyclase Activating Protein-1 With Dominant Retinal Dystrophy

Cited by 7 publications

References 11 publications

Dominant Cone Rod Dystrophy, Previously Assigned to a Missense Variant in RIMS1, Is Fully Explained by Co-Inheritance of a Dominant Allele of PROM1

Dominant Cone Rod Dystrophy, Previously Assigned to a Missense Variant in RIMS1, Is Fully Explained by Co-Inheritance of a Dominant Allele of PROM1

Update to Open Access Status

Establishment of the Clinical Genome Resource (ClinGen) X-Linked Inherited Retinal Disease Variant Curation Expert Panel

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