Late-Onset Stargardt Disease Due to Mild, Deep-Intronic <i>ABCA4</i> Alleles

Runhart, Esmee H.; Valkenburg, Dyon; Cornelis, Stéphanie S.; Khan, Mubeen; Sangermano, Riccardo; Albert, Silvia; Bax, Nathalie M.; Astuti, Galuh D.N.; Gilissen, Christian; Pott, Jan-Willem R.; Verheij, Joanne; Blokland, Ellen A.W.; Cremers, Frans P.M.; Born, L. Ingeborgh van den; Hoyng, Carel B.

doi:10.1167/iovs.19-27524

Cited by 28 publications

(38 citation statements)

References 29 publications

(49 reference statements)

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“…Although 76% of registrations related to Stargardt disease were in the working-age group, we found 10% were registered up to the age of 15 and 14% were registered at 65years or older, with a bimodal peak. This is consistent with the extreme variability in phenotype ranging from severe childhood-onset to late-onset disease, which has a median age of onset in the mid-50 with up to 11% of these individuals eligible for blindness registration (23,28). Another retrospective crosssectional study of 361 patients with Stargardt disease found 59% met the criteria for blindness registration and the median time to develop this degree of visual impairment varied from 22 to 29 years depending on the BCVA at the patient's initial visit (29).…”

Section: Discussionsupporting

confidence: 82%

Inherited retinal diseases are the most common cause of blindness in the working-age population in Australia

Jeffery

Mukhtar

McAllister

et al. 2021

Ophthalmic Genetics

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Background: This study examined the frequency of inherited retinal diseases (IRDs) as the reason for blindness registrations over the last two decades and the demographic and clinical phenotypes of inherited retinal disease (IRD)-related registrations. Materials and methods: Retrospective, observational study of individuals registered with a state-wide blind and vision-impaired registry. Low-vision or blindness-only (≤20/200 or ≤20°) certificates issued to children (0-15 years), working-age (16-64 years) and older-age (65 and older) adults were assessed. Sex and age distributions were examined for the top 20 reasons for certification. Demographic and clinical features of specific phenotypes of IRDs listed in the registry were examined. Results: Amongst 11824 low-vision certificates issued between July 1995 and January 2017, 679 (5.7%) listed an IRD as the reason for registration. In individuals with blindness-only certification (N=4919), IRDs was the second most common diagnosis (8.3%), overtaking glaucoma (8.1%) and diabetic retinopathy (5.4%). IRD was the second most common reason for low-vision certification amongst children (11.6%) and the most common reason amongst working-age population (23.3%). The mean±SD age for IRD-related blindness-only certification was 46±20 years. The top three phenotypes of IRD-related low-vision certification were non-syndromic retinitis pigmentosa (54%), Stargardt disease (12%) and macular dystrophy (8%). Conclusion: Our findings of IRDs as a common cause of blindness in all ages justify continued funding for providing low-vision services and developing treatments for these conditions.

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Section: Discussionsupporting

confidence: 82%

Inherited retinal diseases are the most common cause of blindness in the working-age population in Australia

Jeffery

Mukhtar

McAllister

et al. 2021

Ophthalmic Genetics

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“…32 It should also be noted, however, that evidence is emerging that some variants that were long considered pathogenic or benign by themselves, such as c.2588G>C; p.[G863A,G863del] and c.5603A>T; p.(N1868I), are fully penetrant only when in combination on the same allele. The same is true for the cis configuration of p.(N1868I) with a recently identified intronic mutation, c.769-784C>T. 9,33,34 In addition, modifier variants, either within or outside of ABCA4, as well as environmental factors will likely play a role in determining disease outcome. 9 Thus, care is warranted when attributing a severity score to individual alleles.…”

Section: Discussionmentioning

confidence: 91%

Detailed Phenotyping and Therapeutic Strategies for Intronic ABCA4 Variants in Stargardt Disease

Khan

Arno

Fakin

et al. 2020

Molecular Therapy - Nucleic Acids

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Stargardt disease is a progressive retinal disorder caused by biallelic mutations in the ABCA4 gene that encodes the ATPbinding cassette, subfamily A, member 4 transporter protein. Over the past few years, we and others have identified several pathogenic variants that reside within the introns of ABCA4, including a recurrent variant in intron 36 (c.5196+1137G>A) of which the pathogenicity so far remained controversial. Detailed clinical characterization of this variant confirmed its pathogenic nature, and classified it as an allele of intermediate severity. Moreover, we discovered several additional ABCA4 variants clustering in intron 36. Several of these variants resulted in aberrant splicing of ABCA4, i.e., the inclusion of pseudoexons, while the splicing defects caused by the recurrent c.5196+1137G>A variant strongly increased upon differentiation of patient-derived induced pluripotent stem cells into retina-like cells. Finally, all splicing defects could be rescued by the administration of antisense oligonucleotides that were designed to specifically block the pseudoexon insertion, including rescue in 3D retinal organoids harboring the c.5196+1137G>A variant. Our data illustrate the importance of intronic variants in ABCA4 and expand the therapeutic possibilities for overcoming splicing defects in Stargardt disease.

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“…A step further in genetic diagnosis has been attained when deep-intronic variants that alter the splicing pattern have been identified, as is the case in Stargardt disease, a macular disorder with a very well defined clinical phenotype and a major causative gene, ABCA4. In fact, the introduction of the whole ABCA4 locus in the target NGS panels clearly helps to increase the genetic yield in Stargardt disease patients [16,17].…”

Section: Discussionmentioning

confidence: 99%

Increasing the Genetic Diagnosis Yield in Inherited Retinal Dystrophies: Assigning Pathogenicity to Novel Non-canonical Splice Site Variants

Toulis

Cortés‐González

Castro-Miró

et al. 2020

Genes

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Aims: We aimed to validate the pathogenicity of genetic variants identified in inherited retinal dystrophy (IRD) patients, which were located in non-canonical splice sites (NCSS). Methods: After next generation sequencing (NGS) analysis (target gene panels or whole exome sequencing (WES)), NCSS variants were prioritized according to in silico predictions. In vivo and in vitro functional tests were used to validate their pathogenicity. Results: Four novel NCSS variants have been identified. They are located in intron 33 and 34 of ABCA4 (c.4774-9G>A and c.4849-8C>G, respectively), intron 2 of POC1B (c.101-3T>G) and intron 3 of RP2 (c.884-14G>A). Functional analysis detected different aberrant splicing events, including intron retention, exon skipping and intronic nucleotide addition, whose molecular effect was either the disruption or the elongation of the open reading frame of the corresponding gene. Conclusions: Our data increase the genetic diagnostic yield of IRD patients and expand the landscape of pathogenic variants, which will have an impact on the genotype–phenotype correlations and allow patients to opt for the emerging gene and cell therapies.

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Late-Onset Stargardt Disease Due to Mild, Deep-Intronic ABCA4 Alleles

Cited by 28 publications

References 29 publications

Inherited retinal diseases are the most common cause of blindness in the working-age population in Australia

Inherited retinal diseases are the most common cause of blindness in the working-age population in Australia

Detailed Phenotyping and Therapeutic Strategies for Intronic ABCA4 Variants in Stargardt Disease

Increasing the Genetic Diagnosis Yield in Inherited Retinal Dystrophies: Assigning Pathogenicity to Novel Non-canonical Splice Site Variants

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