A case of retinitis pigmentosa homozygous for a rare CNGA1 causal variant

Retinitis pigmentosa (RP) is a heterogenous hereditary disorder leading to blindness. Despite using next-generation sequencing technologies, causal variants in about 60% of RP cases remain unknown. The heterogeneous genetic inheritance pattern makes it difficult to pinpoint causal variants. Besides,...

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Bibliographic Details
Published in:Scientific reports 2021-02, Vol.11 (1), p.4681-4681, Article 4681
Main Authors: Saito, Kohei, Gotoh, Norimoto, Kang, Inyeop, Shimada, Toshio, Usui, Takeshi, Terao, Chikashi
Format: Article
Language:English
Subjects:
631/208
692/699/3161
692/699/3161/3175
Blindness
Consanguinity
Cyclic Nucleotide-Gated Cation Channels - genetics
Female
Genomes
Genotypes
Heredity
Homozygosity
Homozygote
Homozygotes
Humanities and Social Sciences
Humans
Japan
Male
multidisciplinary
Mutation
Mutation, Missense
Next-generation sequencing
Pedigree
Retinitis
Retinitis pigmentosa
Retinitis Pigmentosa - genetics
Science
Science (multidisciplinary)
Whole Genome Sequencing
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Summary:Retinitis pigmentosa (RP) is a heterogenous hereditary disorder leading to blindness. Despite using next-generation sequencing technologies, causal variants in about 60% of RP cases remain unknown. The heterogeneous genetic inheritance pattern makes it difficult to pinpoint causal variants. Besides, rare penetrating variants are hardly observed in general case–control studies. Thus, a family-based analysis, specifically in a consanguineous family, is a clinically and genetically valuable approach for RP. We analyzed a Japanese consanguineous family with a member suffering from RP with a typical autosomal recessive pattern. We sequenced five direct descendants and spouse using Whole-exome sequencing (WES) and Whole-genome sequencing (WGS). We identified a homozygous pathogenic missense variant in CNGA1 (NM_000087.3, c.839G > A, p.Arg280His) in the proband, while we found no homozygous genotypes in the other family members. CNGA1 was previously reported to be associated with RP. We confirmed the genotypes by the Sanger sequencing. Additionally, we assessed the homozygous genotype in the proband for the possibility of a founder mutation using homozygosity analysis. Our results suggested the two copies of the variant derived from a founder mutation. In conclusion, we found the homozygotes for c.839G > A in CNGA1 as causal for RP.
ISSN:2045-2322
2045-2322
DOI:10.1038/s41598-021-84098-9