Diagnostic exome sequencing in 266 Dutch patients with visual impairment

Haer‐Wigman, Lonneke; Zelst-Stams, Wendy A. G. van; Pfundt, Rolph; Born, L. Ingeborgh van den; Klaver, Caroline C.W.; Verheij, Joanne; Hoyng, Carel B.; Breuning, Martijn H.; Boon, Camiel J F; Kievit, Anneke J.A.; Verhoeven, Virginie J M; Pott, Jan Willem R.; Sallevelt, Suzanne C E H; Hagen, Johanna M. van; Plomp, Astrid S.; Kroes, Hester Y.; Lelieveld, Stefan H.; Hehir-Kwa, Jayne Y.; Castelein, Steven; Nelen, Marcel; Scheffer, Hans; Lugtenberg, Dorien; Cremers, Frans P.M.; Hoefsloot, Lies H.; Yntema, Helger G.

doi:10.1038/ejhg.2017.9

Cited by 117 publications

(128 citation statements)

References 22 publications

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“…The two most frequently mutated genes in the Israeli IRD cohort are ABCA4 (14%) and USH2A (7%). These findings are similar to those found in large IRD cohorts from other populations (Carss et al, ; Dockery et al, ; Haer‐Wigman et al, ; Stone et al, ). However, some of our findings are unique.…”

Section: Discussionsupporting

confidence: 89%

“…Overall, we succeeded to identify the genetic basis of disease in 56% of the recruited families (64% among families recruited up to December 2015). This percentage is within the range of diagnostic rates reported recently in other large cohorts of IRD patients (Carss et al, ; Dockery et al, ; Haer‐Wigman et al, ; Stone et al, ). It should be noted that of the unsolved families, only 17% have undergone WES and only 0.5% have undergone WGS.…”

Section: Discussionsupporting

confidence: 84%

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A nationwide genetic analysis of inherited retinal diseases in Israel as assessed by the Israeli inherited retinal disease consortium (IIRDC)

et al. 2019

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Inherited retinal diseases (IRDs) cause visual loss due to dysfunction or progressive degeneration of photoreceptors. These diseases show marked phenotypic and genetic heterogeneity. The Israeli IRD consortium (IIRDC) was established in 2013 with the goal of performing clinical and genetic mapping of the majority of Israeli IRD patients. To date, we recruited 2,420 families including 3,413 individuals with IRDs. On the basis of our estimation, these patients represent approximately 40% of Israeli IRD patients. To the best of our knowledge, this is, by far, the largest reported IRD cohort, and one of the first studies addressing the genetic analysis of IRD patients on a nationwide scale. The most common inheritance pattern in our cohort is autosomal recessive (60% of families). The most common retinal phenotype is retinitis pigmentosa (43%), followed by Stargardt disease and cone/cone–rod dystrophy. We identified the cause of disease in 56% of the families. Overall, 605 distinct mutations were identified, of which 12% represent prevalent founder mutations. The most frequently mutated genes were ABCA4, USH2A, FAM161A, CNGA3, and EYS. The results of this study have important implications for molecular diagnosis, genetic screening, and counseling, as well as for the development of new therapeutic strategies for retinal diseases.

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Section: Discussionsupporting

confidence: 89%

Section: Discussionsupporting

confidence: 84%

A nationwide genetic analysis of inherited retinal diseases in Israel as assessed by the Israeli inherited retinal disease consortium (IIRDC)

et al. 2019

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“…WES was performed following our routine diagnostic procedures [15]. In essence, DNA was outsourced to BGI (Copenhagen, Denmark) where exomes were captured using Agilent Sureselect v4 and sequenced to a median coverage of 75-fold on an Illumina HiSeq instrument with 101-bp paired-end reads.…”

Section: Methodsmentioning

confidence: 99%

1 in 38 individuals at risk of a dominant medically actionable disease

et al. 2018

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Clinical genomic sequencing can identify pathogenic variants unrelated to the initial clinical question, but of medical relevance to the patients and their families. With ongoing discussions on the utility of disclosing or searching for such variants, it is of crucial importance to obtain unbiased insight in the prevalence of these incidental or secondary findings, in order to better weigh potential risks and benefits. Previous studies have reported a broad range of secondary findings ranging from 1 to 9%, merely attributable to differences in study design, cohorts tested, sequence technology used and genes analyzed. Here, we analyzed WES data of 1640 anonymized healthy Dutch individuals to establish the frequency of medically actionable disease alleles in an outbred population of European descent. Our study shows that 1 in 38 healthy individuals (2.7%) has a (likely) pathogenic variant in one of 59 medically actionable dominant disease genes for which the American College of Medical Genetics and Genomics (ACMG) recommends disclosure. Additionally, we identified 36 individuals (2.2%) to be a carrier of a recessive pathogenic disease allele. Whereas these frequencies of secondary findings are in line with what has been reported in the East-Asian population, the pathogenic variants are differently distributed across the 59 ACMG genes. Our results contribute to the debate on genetic risk factor screening in healthy individuals and the discussion whether the potential benefits of this knowledge and related preventive options, outweigh the risk of the emotional impact of the test result and possible stigmatization.

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“…In total, we collected information of 377 RP patients described in 43 papers (Abd El‐Aziz et al., ; Abd El‐Aziz et al., ; Abu‐Safieh et al., ; Arai et al., ; Audo et al., ; Audo et al., ; Bandah‐Rozenfeld et al., ; Barragan et al., ; Beryozkin et al., ; Bonilha et al., ; Chen, et al., ; Collin et al., ; Consugar et al., ; Di et al., ; Eisenberger et al., ; Ge et al., ; Glockle et al., ; Gonzalez‐del Pozo et al., ; Gu, Tian, Chen, & Zhao, ; Habibi, et al., ; Haer‐Wigman et al., ; Hashmi, et al., ; Hosono et al., ; Huang et al., ; Huang et al., ; Iwanami, Oshikawa, Nishida, Nakadomari, & Kato, ; Jinda et al., ; Kastner et al., ; Katagiri et al., ; Khan et al., ; Littink et al., ; Littink et al., ; Neveling et al., ; Nishiguchi et al., ; Oishi et al., ; O'Sullivan et al., ; Perez‐Carro et al., ; Pieras et al., ; Pierrottet et al., ; Siemiatkowska et al., ; Suto et al., ; Xu, et al., ; Yoon et al., ), in which 630 alleles with EYS variants were reported. In addition, we identified 26 novel variants found in 36 index patients that were not published previously (Table ).…”

Section: Eys Variantsmentioning

confidence: 99%

EYSmutation update: In silico assessment of 271 reported and 26 novel variants in patients with retinitis pigmentosa

et al. 2017

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Mutations in Eyes shut homolog (EYS) are one of the most common causes of autosomal recessive (ar) retinitis pigmentosa (RP), a progressive blinding disorder. The exact function of the EYS protein and the pathogenic mechanisms underlying EYS-associated RP are still poorly understood, which hampers the interpretation of the causality of many EYS variants discovered to date. We collected all reported EYS variants present in 377 arRP index cases published before June 2017, and uploaded them in the Leiden Open Variation Database (www.LOVD.nl/EYS). We also describe 36 additional index cases, carrying 26 novel variants. Of the 297 unique EYS variants identified, almost half (n = 130) are predicted to result in premature truncation of the EYS protein. Classification of all variants using the American College of Medical Genetics and Genomics guidelines revealed that the predicted pathogenicity of these variants cover the complete spectrum ranging from likely benign to pathogenic, although especially missense variants largely fall in the category of uncertain significance. Besides the identification of likely benign alleles previously reported as being probably pathogenic, our comprehensive analysis underscores the need of functional assays to assess the causality of EYS variants, in order to improve molecular diagnostics and counseling of patients with EYS-associated RP.

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Diagnostic exome sequencing in 266 Dutch patients with visual impairment

Cited by 117 publications

References 22 publications

A nationwide genetic analysis of inherited retinal diseases in Israel as assessed by the Israeli inherited retinal disease consortium (IIRDC)

A nationwide genetic analysis of inherited retinal diseases in Israel as assessed by the Israeli inherited retinal disease consortium (IIRDC)

1 in 38 individuals at risk of a dominant medically actionable disease

EYSmutation update: In silico assessment of 271 reported and 26 novel variants in patients with retinitis pigmentosa

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