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2. Optical genome mapping and revisiting short-read genome sequencing data reveal previously overlooked structural variants disrupting retinal disease-associated genes.

Author

Bruijn, S.E. de, Rodenburg, K., Corominas, J., Ben-Yosef, T., Reurink, J.A., Kremer, H., Whelan, L., Plomp, A.S., Berger, W., Farrar, G.J., Ferenc Kovács, Á., Fajardy, I., Hitti-Malin, R.J., Weisschuh, N., Weener, M.E., Sharon, D., Pennings, R.J.E., Haer-Wigman, L., Hoyng, C.B., Nelen, M.R., Vissers, L.E.L.M., Born, L.I. van den, Gilissen, C.F.H.A., Cremers, F.P.M., Hoischen, A., Neveling, K., Roosing, S., Bruijn, S.E. de, Rodenburg, K., Corominas, J., Ben-Yosef, T., Reurink, J.A., Kremer, H., Whelan, L., Plomp, A.S., Berger, W., Farrar, G.J., Ferenc Kovács, Á., Fajardy, I., Hitti-Malin, R.J., Weisschuh, N., Weener, M.E., Sharon, D., Pennings, R.J.E., Haer-Wigman, L., Hoyng, C.B., Nelen, M.R., Vissers, L.E.L.M., Born, L.I. van den, Gilissen, C.F.H.A., Cremers, F.P.M., Hoischen, A., Neveling, K., and Roosing, S.

Abstract

Item does not contain fulltext, PURPOSE: Structural variants (SVs) play an important role in inherited retinal diseases (IRD). Although the identification of SVs significantly improved upon the availability of genome sequencing, it is expected that involvement of SVs in IRDs is higher than anticipated. We revisited short-read genome sequencing data to enhance the identification of gene-disruptive SVs. METHODS: Optical genome mapping was performed to improve SV detection in short-read genome sequencing-negative cases. In addition, reanalysis of short-read genome sequencing data was performed to improve the interpretation of SVs and to re-establish SV prioritization criteria. RESULTS: In a monoallelic USH2A case, optical genome mapping identified a pericentric inversion (173 megabase), with 1 breakpoint disrupting USH2A. Retrospectively, the variant could be observed in genome sequencing data but was previously deemed false positive. Reanalysis of short-read genome sequencing data (427 IRD cases) was performed which yielded 30 pathogenic SVs affecting, among other genes, USH2A (n = 15), PRPF31 (n = 3), and EYS (n = 2). Eight of these (>25%) were overlooked during previous analyses. CONCLUSION: Critical evaluation of our findings allowed us to re-establish and improve our SV prioritization and interpretation guidelines, which will prevent missing pathogenic events in future analyses. Our data suggest that more attention should be paid to SV interpretation and the current contribution of SVs in IRDs is still underestimated.

Published
2023

3. Genotype and Phenotype Analyses of a Novel WFS1 Variant (c.2512C>T p.(Pro838Ser)) Associated with DFNA6/14/38.

Author

Velde, H.M., Huizenga, X.J.J., Yntema, H.G., Haer-Wigman, L., Beynon, A.J., Oostrik, J., Pegge, S.A.H., Kremer, H., Lanting, C.P., Pennings, R.J.E., Velde, H.M., Huizenga, X.J.J., Yntema, H.G., Haer-Wigman, L., Beynon, A.J., Oostrik, J., Pegge, S.A.H., Kremer, H., Lanting, C.P., and Pennings, R.J.E.

Abstract

Item does not contain fulltext, The aim of this study is to contribute to a better description of the genotypic and phenotypic spectrum of DFNA6/14/38 and aid in counseling future patients identified with this variant. Therefore, we describe the genotype and phenotype in a large Dutch-German family (W21-1472) with autosomal dominant non-syndromic, low-frequency sensorineural hearing loss (LFSNHL). Exome sequencing and targeted analysis of a hearing impairment gene panel were used to genetically screen the proband. Co-segregation of the identified variant with hearing loss was assessed by Sanger sequencing. The phenotypic evaluation consisted of anamnesis, clinical questionnaires, physical examination and examination of audiovestibular function. A novel likely pathogenic WFS1 variant (NM_006005.3:c.2512C>T p.(Pro838Ser)) was identified in the proband and found to co-segregate with LFSNHL, characteristic of DFNA6/14/38, in this family. The self-reported age of onset of hearing loss (HL) ranged from congenital to 50 years of age. In the young subjects, HL was demonstrated in early childhood. At all ages, an LFSNHL (0.25-2 kHz) of about 50-60 decibel hearing level (dB HL) was observed. HL in the higher frequencies showed inter-individual variability. The dizziness handicap inventory (DHI) was completed by eight affected subjects and indicated a moderate handicap in two of them (aged 77 and 70). Vestibular examinations (n = 4) showed abnormalities, particularly in otolith function. In conclusion, we identified a novel WFS1 variant that co-segregates with DFNA6/14/38 in this family. We found indications of mild vestibular dysfunction, although it is uncertain whether this is related to the identified WFS1 variant or is an incidental finding. We would like to emphasize that conventional neonatal hearing screening programs are not sensitive to HL in DFNA6/14/38 patients, because high-frequency hearing thresholds are initially preserved. Therefore, we suggest screening newborns in DFNA6/14/38 families with

Published
2023

4. Whole genome sequencing for USH2A-associated disease reveals several pathogenic deep-intronic variants that are amenable to splice correction

Author

Reurink, J.A., Weisschuh, Nicole, Garanto, A., Dockery, A., Born, L.I. van den, Fajardy, Isabelle, Haer-Wigman, L., Klaver, C.C.W., Smits, J.J., Pennings, R.J.E., Aben, M.J., Oostrik, J., Astuti, G.D.N, Corominas, J., Phan, M., Zelst-Stams, W.A.G. van, Bruijn, S.E. de, Li, C.H.Z., Hoyng, C.B., Gilissen, C.F.H.A., Vissers, L.E.L.M., Cremers, F.P.M., Kremer, H., WIjk, E. van, Roosing, S., Reurink, J.A., Weisschuh, Nicole, Garanto, A., Dockery, A., Born, L.I. van den, Fajardy, Isabelle, Haer-Wigman, L., Klaver, C.C.W., Smits, J.J., Pennings, R.J.E., Aben, M.J., Oostrik, J., Astuti, G.D.N, Corominas, J., Phan, M., Zelst-Stams, W.A.G. van, Bruijn, S.E. de, Li, C.H.Z., Hoyng, C.B., Gilissen, C.F.H.A., Vissers, L.E.L.M., Cremers, F.P.M., Kremer, H., WIjk, E. van, and Roosing, S.

Abstract

Item does not contain fulltext

Published
2023

5. Systematic analysis of paralogous regions in 41,755 exomes uncovers clinically relevant variation

Author

Steyaert, W.A.R., Haer-Wigman, L., Pfundt, R.P., Hellebrekers, D., Steehouwer, M., Hampstead, J.E., Boer, E. de, Yntema, H.G., Kamsteeg, E.J., Brunner, H.G., Hoischen, A., Gilissen, C.F.H.A., Steyaert, W.A.R., Haer-Wigman, L., Pfundt, R.P., Hellebrekers, D., Steehouwer, M., Hampstead, J.E., Boer, E. de, Yntema, H.G., Kamsteeg, E.J., Brunner, H.G., Hoischen, A., and Gilissen, C.F.H.A.

Abstract

Contains fulltext : 298929.pdf (Publisher’s version ) (Open Access)

Published
2023

6. Stable long-term outcomes after cochlear implantation in subjects with TMPRSS3 associated hearing loss:a retrospective multicentre study

Author

Fehrmann, M. L.A., Huinck, W. J., Thijssen, M. E.G., Haer-Wigman, L., Yntema, H. G., Rotteveel, L. J.C., Widdershoven, J. C.C., Goderie, T., van Dooren, M. F., Hoefsloot, E. H., Mylanus, E. A.M., Fehrmann, M. L.A., Huinck, W. J., Thijssen, M. E.G., Haer-Wigman, L., Yntema, H. G., Rotteveel, L. J.C., Widdershoven, J. C.C., Goderie, T., van Dooren, M. F., Hoefsloot, E. H., and Mylanus, E. A.M.

Abstract

Background: The spiral ganglion hypothesis suggests that pathogenic variants in genes preferentially expressed in the spiral ganglion nerves (SGN), may lead to poor cochlear implant (CI) performance. It was long thought that TMPRSS3 was particularly expressed in the SGNs. However, this is not in line with recent reviews evaluating CI performance in subjects with TMPRSS3-associated sensorineural hearing loss (SNHL) reporting overall beneficial outcomes. These outcomes are, however, based on variable follow-up times of, in general, 1 year or less. Therefore, we aimed to 1. evaluate long-term outcomes after CI implantation of speech recognition in quiet in subjects with TMPRSS3-associated SNHL, and 2. test the spiral ganglion hypothesis using the TMPRSS3-group. Methods: This retrospective, multicentre study evaluated long-term CI performance in a Dutch population with TMPRSS3-associated SNHL. The phoneme scores at 70 dB with CI in the TMPRSS3-group were compared to a control group of fully genotyped cochlear implant users with post-lingual SNHL without genes affecting the SGN, or severe anatomical inner ear malformations. CI-recipients with a phoneme score ≤ 70% at least 1-year post-implantation were considered poor performers and were evaluated in more detail. Results: The TMPRSS3 group consisted of 29 subjects (N = 33 ears), and the control group of 62 subjects (N = 67 ears). For the TMPRSS3-group, we found an average phoneme score of 89% after 5 years, which remained stable up to 10 years post-implantation. At both 5 and 10-year follow-up, no difference was found in speech recognition in quiet between both groups (p = 0.830 and p = 0.987, respectively). Despite these overall adequate CI outcomes, six CI recipients had a phoneme score of ≤ 70% and were considered poor performers. The latter was observed in subjects with residual hearing post-implantation or older age at implantation. Conclusion:

Published
2023

7. Development of a Genotype Assay for Age-Related Macular Degeneration The EYE-RISK Consortium

Author

Breuk, A. de, Acar, I.E., Kersten, E., Schijvenaars, M.M.V.A.P., Colijn, J.M., Haer-Wigman, L., Bakker, B., Jong, S. de, Hoyng, C.B., Coenen, M.J.H., Klaver, C.C.W., and Hollander, A.I. den

Subjects
All institutes and research themes of the Radboud University Medical Center, Inflammatory diseases Radboud Institute for Health Sciences [Radboudumc 5], Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12]
Abstract

Contains fulltext : 240741.pdf (Publisher’s version ) (Open Access)

Published
2021

8. Scrutinizing pathogenicity of the USH2A c.2276 G > T; p.(Cys759Phe) variant

Author

Reurink, J.A., Vrieze, E. de, Li, C.H.Z., Berkel, Emma van, Broekman, S., Aben, M.J., Peters, T.A., Oostrik, J., Neveling, K., Venselaar, H., Ramos, Mariana Guimarães, Gilissen, C.F.H.A., Astuti, G.D.N, Ockeloen, C.W., Haer-Wigman, L., Hoyng, C.B., Cremers, F.P.M., Kremer, H., Roosing, S., WIjk, E. van, Reurink, J.A., Vrieze, E. de, Li, C.H.Z., Berkel, Emma van, Broekman, S., Aben, M.J., Peters, T.A., Oostrik, J., Neveling, K., Venselaar, H., Ramos, Mariana Guimarães, Gilissen, C.F.H.A., Astuti, G.D.N, Ockeloen, C.W., Haer-Wigman, L., Hoyng, C.B., Cremers, F.P.M., Kremer, H., Roosing, S., and WIjk, E. van

Abstract

Item does not contain fulltext

Published
2022

9. Lessons learned from unsolicited findings in clinical exome sequencing of 16,482 individuals

Author

Schoot, V. van der, Haer-Wigman, L., Feenstra, I., Tammer, Femke, Oerlemans, A.J.M., Koolwijk, M.P. van, Agt, F. van, Arens, Y., Brunner, H.G., Vissers, L.E.L.M., Yntema, H.G., Schoot, V. van der, Haer-Wigman, L., Feenstra, I., Tammer, Femke, Oerlemans, A.J.M., Koolwijk, M.P. van, Agt, F. van, Arens, Y., Brunner, H.G., Vissers, L.E.L.M., and Yntema, H.G.

Abstract

Item does not contain fulltext, Unsolicited findings (UFs) are uncovered unintentionally and predispose to a disease unrelated to the clinical question. The frequency and nature of UFs uncovered in clinical practice remain largely unexplored. We here evaluated UFs identified during a 5-year period in which 16,482 index patients received clinical whole-exome sequencing (WES). UFs were identified in 0.58% (95/16,482) of index patients, indicating that the overall frequency of UFs in clinical WES is low. Fewer UFs were identified using restricted disease-gene panels (0.03%) than when using whole-exome/Mendeliome analysis (1.03%). The UF was disclosed to 86 of 95 individuals, for reasons of medical actionability. Only 61% of these UFs reside in a gene that is listed on the "ACMG59"-list, representing a list of 59 genes for which the American College of Medical Genetics recommends UF disclosure. The remaining 39% were grouped into four categories: disorders similar to "ACMG59"-listed disorders (25%); disorders for which disease manifestation could be influenced (7%); UFs providing reproductive options (2%); and UFs with pharmacogenetic implications (5%). Hence, our experience shows that UFs predisposing to medically actionable disorders affect a broader range of genes than listed on the "ACMG59", advocating that a pre-defined gene list is too restrictive, and that UFs may require ad hoc evaluation of medical actionability. While both the identification and disclosure of UFs depend on local policy, our lessons learned provide general essential insight into the nature and odds of UFs in clinical exome sequencing.

Published
2022

11. Usher syndrome type IV: clinically and molecularly confirmed by novel ARSG variants

Author

Velde, H.M., Reurink, J.A., Held, S., Li, C.H.Z., Yzer, S., Oostrik, J., Weeda, J.A., Haer-Wigman, L., Yntema, H.G., Roosing, S., Pauleikhoff, L., Lange, C de, Whelan, L., Dockery, A., Zhu, Z., Keegan, D.J., Farrar, G.J., Kremer, H., Lanting, C.P., Damme, M., Pennings, R.J.E., Velde, H.M., Reurink, J.A., Held, S., Li, C.H.Z., Yzer, S., Oostrik, J., Weeda, J.A., Haer-Wigman, L., Yntema, H.G., Roosing, S., Pauleikhoff, L., Lange, C de, Whelan, L., Dockery, A., Zhu, Z., Keegan, D.J., Farrar, G.J., Kremer, H., Lanting, C.P., Damme, M., and Pennings, R.J.E.

Abstract

Item does not contain fulltext, Usher syndrome (USH) is an autosomal recessively inherited disease characterized by sensorineural hearing loss (SNHL) and retinitis pigmentosa (RP) with or without vestibular dysfunction. It is highly heterogeneous both clinically and genetically. Recently, variants in the arylsulfatase G (ARSG) gene have been reported to underlie USH type IV. This distinct type of USH is characterized by late-onset RP with predominantly pericentral and macular changes, and late onset SNHL without vestibular dysfunction. In this study, we describe the USH type IV phenotype in three unrelated subjects. We identified three novel pathogenic variants, two novel likely pathogenic variants, and one previously described pathogenic variant in ARSG. Functional experiments indicated a loss of sulfatase activity of the mutant proteins. Our findings confirm that ARSG variants cause the newly defined USH type IV and support the proposed extension of the phenotypic USH classification.

Published
2022

12. Identification of a Complex Allele in IMPG2 as a Cause of Adult-Onset Vitelliform Macular Dystrophy

Author

Vazquez Dominguez, I., Li, C.H.Z., Fadaie, Zeinab, Haer-Wigman, L., Cremers, F.P.M., Garanto, A., Hoyng, C.B., Roosing, S., Vazquez Dominguez, I., Li, C.H.Z., Fadaie, Zeinab, Haer-Wigman, L., Cremers, F.P.M., Garanto, A., Hoyng, C.B., and Roosing, S.

Abstract

Contains fulltext : 251530.pdf (Publisher’s version ) (Open Access), PURPOSE: Inherited retinal diseases are a group of clinically and genetically heterogeneous disorders with approximately 270 genes involved. IMPG2 is associated with adult-onset vitelliform macular dystrophy. Here, we investigated two unrelated patients with vitelliform macular dystrophy to identify the underlying genetic cause. METHODS: Whole-exome sequencing identified a putative causal complex allele consisting of c.3023-15T>A and c.3023G>A (p.(Gly1008Asp)) in IMPG2 in both individuals. To assess its effect, in vitro splice assays in HEK293T and further characterization in patient-derived photoreceptor precursor cells (PPCs) were conducted. RESULTS: The results of the midigene splice assays in HEK293T showed that the complex allele causes a variety of splicing defects ranging from a small deletion to (multiple-)exon skipping. This finding was further validated using patient-derived PPCs that showed a significant increase of out-of-frame transcripts lacking one or multiple exons compared to control-derived PPCs. Overall, control PPCs consistently showed low levels of aberrantly spliced IMPG2 transcripts that were highly elevated in patient-derived PPCs. These differences were even more obvious upon inhibition of nonsense-mediated decay with cycloheximide. CONCLUSIONS: We report a heterozygous complex allele in IMPG2 causative for adult-onset vitelliform macular dystrophy in two unrelated individuals with mild visual loss and bilateral vitelliform lesions. The predicted causal missense mutation c.3023G>A, located in the consensus splice acceptor site, enhances the splicing effect of the upstream variant c.3023-15T>A, leading to the generation of aberrant transcripts that decrease the full-length IMPG2 levels. These results suggest a haploinsufficiency mechanism of action and highlight the complementarity of using different models to functionally assesses splicing defects.

Published
2022

13. Diagnostic analysis of the highly complex OPN1LW/OPN1MW gene cluster using long-read sequencing and MLPA

Author

Haer-Wigman, L., Ouden, A.P.M. den, Genderen, Maria m. van, Kroes, H.Y., Verheij, J., Smailhodzic, Dzenita, Blom, Jan, Derks, R.C., Yntema, H.G., Nelen, M.R., Vissers, L.E.L.M., Lugtenberg, D., Neveling, K., Haer-Wigman, L., Ouden, A.P.M. den, Genderen, Maria m. van, Kroes, H.Y., Verheij, J., Smailhodzic, Dzenita, Blom, Jan, Derks, R.C., Yntema, H.G., Nelen, M.R., Vissers, L.E.L.M., Lugtenberg, D., and Neveling, K.

Abstract

Contains fulltext : 285305.pdf (Publisher’s version ) (Open Access)

Published
2022

15. The need for widely available genomic testing in rare eye diseases: an ERN-EYE position statement

Author

Black G. C., Sergouniotis P., Sodi A., Leroy B. P., Van Cauwenbergh C., Liskova P., Gronskov K., Klett A., Kohl S., Taurina G., Sukys M., Haer-Wigman L., Nowomiejska K., Marques J. P., Leroux D., Cremers F. P. M., De Baere E., Dollfus H., Ashworth J., Audo I., Bacci G., Balciuniene V. J., Bargiacchi S., Bertelsen M., Black G., Boon C., Bremond-Gignac D., Buzzonetti L., Calvas P., Thomsen A. C., Chirita-Emandi A., Chokoshvili D., Cremers F., Daly A., Downes S., Fasolo A., Fasser C., Fischer D., Fortunato P., Gelzinis A., Hall G., Hamann S., Heon E., Iarossi G., Iberg C., Jouanjan G., Kaariainen H., Kahn K., Keegan D., Laengsfeld M., Leon A., Leroux B., Lorenz B., Maggi R., Mauring L., Melico P., Meunier I., Mohand-Said S., Monterosso C., Morandi P., Parmeggiani F., Passerini I., Pelletier V., Peluso F., Perdomo Y., Rapizzi E., Roos L., Roosing S., Rozet J. -M., Simonelli F., Sowden J., Stingl K., Suppiej A., Testa F., Tracewska A., Traficante G., Valeina S., Wheeler-Schilling T., Yu-Wai-Man P., Zeitz C., Zemaitiene R., Leroux, Dorothée [0000-0002-1412-6611], Apollo - University of Cambridge Repository, Ophthalmology, ANS - Complex Trait Genetics, Black, G. C., Sergouniotis, P., Sodi, A., Leroy, B. P., Van Cauwenbergh, C., Liskova, P., Gronskov, K., Klett, A., Kohl, S., Taurina, G., Sukys, M., Haer-Wigman, L., Nowomiejska, K., Marques, J. P., Leroux, D., Cremers, F. P. M., De Baere, E., Dollfus, H., Ashworth, J., Audo, I., Bacci, G., Balciuniene, V. J., Bargiacchi, S., Bertelsen, M., Black, G., Boon, C., Bremond-Gignac, D., Buzzonetti, L., Calvas, P., Thomsen, A. C., Chirita-Emandi, A., Chokoshvili, D., Cremers, F., Daly, A., Downes, S., Fasolo, A., Fasser, C., Fischer, D., Fortunato, P., Gelzinis, A., Hall, G., Hamann, S., Heon, E., Iarossi, G., Iberg, C., Jouanjan, G., Kaariainen, H., Kahn, K., Keegan, D., Laengsfeld, M., Leon, A., Leroux, B., Lorenz, B., Maggi, R., Mauring, L., Melico, P., Meunier, I., Mohand-Said, S., Monterosso, C., Morandi, P., Parmeggiani, F., Passerini, I., Pelletier, V., Peluso, F., Perdomo, Y., Rapizzi, E., Roos, L., Roosing, S., Rozet, J. -M., Simonelli, F., Sowden, J., Stingl, K., Suppiej, A., Testa, F., Tracewska, A., Traficante, G., Valeina, S., Wheeler-Schilling, T., Yu-Wai-Man, P., Zeitz, C., and Zemaitiene, R.

Subjects
0301 basic medicine, Eye Diseases, lcsh:Medicine, CHILDREN, Position statement, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], MOLECULAR-GENETICS, 0302 clinical medicine, HISTORY, Health care, Medicine and Health Sciences, Genetics(clinical), Pharmacology (medical), Child, Genetics (clinical), medicine.diagnostic_test, General Medicine, Genomics, Europe, TRIALS, ERN-EYE, Rare eye diseases, medicine.symptom, Genetic and genomic testing, Human, medicine.medical_specialty, Visual impairment, LEBER CONGENITAL AMAUROSIS, Socio-culturale, DIAGNOSIS, 03 medical and health sciences, Rare Diseases, medicine, Humans, Genetic Testing, Intensive care medicine, Genetic testing, business.industry, CLINICAL-FEATURES, lcsh:R, Rare eye disease, Eye Disease, Human genetics, Clinical trial, 030104 developmental biology, Genomic, 030221 ophthalmology & optometry, Personalized medicine, business, Rare disease
Abstract

Background Rare Eye Diseases (RED) are the leading cause of visual impairment and blindness for children and young adults in Europe. This heterogeneous group of conditions includes over 900 disorders ranging from relatively prevalent disorders such as retinitis pigmentosa to very rare entities such as developmental eye anomalies. A significant number of patients with RED have an underlying genetic etiology. One of the aims of the European Reference Network for Rare Eye Diseases (ERN–EYE) is to facilitate improvement in diagnosis of RED in European member states. Main body Technological advances have allowed genetic and genomic testing for RED. The outcome of genetic testing allows better understanding of the condition and allows reproductive and therapeutic options. The increase of the number of clinical trials for RED has provided urgency for genetic testing in RED. A survey of countries participating in ERN-EYE demonstrated that the majority are able to access some forms of genomic testing. However, there is significant variability, particularly regarding testing as part of clinical service. Some countries have a well-delineated rare disease pathway and have a national plan for rare diseases combined or not with a national plan for genomics in medicine. In other countries, there is a well-established organization of genetic centres that offer reimbursed genomic testing of RED and other rare diseases. Clinicians often rely upon research-funded laboratories or private companies. Notably, some member states rely on cross-border testing by way of an academic research project. Consequently, many clinicians are either unable to access testing or are confronted with long turnaround times. Overall, while the cost of sequencing has dropped, the cumulative cost of a genomic testing service for populations remains considerable. Importantly, the majority of countries reported healthcare budgets that limit testing. Short conclusion Despite technological advances, critical gaps in genomic testing remain in Europe, especially in smaller countries where no formal genomic testing pathways exist. Even within larger countries, the existing arrangements are insufficient to meet the demand and to ensure access. ERN-EYE promotes access to genetic testing in RED and emphasizes the clinical need and relevance of genetic testing in RED.

Published
2021

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

Author

Peeters, M.H.C.A., Khan, M., Rooijakkers, A., Mulders, T.W.F., Haer-Wigman, L., Boon, C.J.F., Klaver, C.C.W., Born, L.I. van den, Hoyng, C.B., Cremers, F.P.M., Hollander, A.I. den, Dhaenens, C.M., Collin, R.W.J., Peeters, M.H.C.A., Khan, M., Rooijakkers, A., Mulders, T.W.F., Haer-Wigman, L., Boon, C.J.F., Klaver, C.C.W., Born, L.I. van den, Hoyng, C.B., Cremers, F.P.M., Hollander, A.I. den, Dhaenens, C.M., and Collin, R.W.J.

Abstract

Contains fulltext : 244059.pdf (Publisher’s version ) (Open Access), 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.

Published
2021

17. Long-read technologies identify a hidden inverted duplication in a family with choroideremia

Author

Fadaie, Z., Neveling, K., Mantere, T., Derks, R.C., Haer-Wigman, L., Ouden, A. Den, Kwint, M.P., O’Gorman, L., Valkenburg, D., Hoyng, C.B., Gilissen, C., Vissers, L.E.L.M., Nelen, M.R., Cremers, F.P.M., Hoischen, A., Roosing, S., Fadaie, Z., Neveling, K., Mantere, T., Derks, R.C., Haer-Wigman, L., Ouden, A. Den, Kwint, M.P., O’Gorman, L., Valkenburg, D., Hoyng, C.B., Gilissen, C., Vissers, L.E.L.M., Nelen, M.R., Cremers, F.P.M., Hoischen, A., and Roosing, S.

Abstract

Contains fulltext : 244033.pdf (Publisher’s version ) (Open Access)

Published
2021

18. Whole genome sequencing and in vitro splice assays reveal genetic causes for inherited retinal diseases

Author

Fadaie, Z., Whelan, L., Ben-Yosef, Tamar, Dockery, A., Corradi, Z., Gilissen, C.F.H.A., Haer-Wigman, L., Corominas, J., Astuti, G.D.N, Farrar, G.J., Klaver, C.C.W., Hoyng, C.B., Cremers, F.P.M., Roosing, S., Rooij, Laura de, Fadaie, Z., Whelan, L., Ben-Yosef, Tamar, Dockery, A., Corradi, Z., Gilissen, C.F.H.A., Haer-Wigman, L., Corominas, J., Astuti, G.D.N, Farrar, G.J., Klaver, C.C.W., Hoyng, C.B., Cremers, F.P.M., Roosing, S., and Rooij, Laura de

Abstract

Contains fulltext : 241168.pdf (Publisher’s version ) (Open Access)

Published
2021

19. The need for widely available genomic testing in rare eye diseases: an ERN-EYE position statement.

Author

Black, G.C., Sergouniotis, P.I., Sodi, A., Leroy, B.P., Cauwenbergh, Caroline Van, Liskova, P., Gronskov, K., Klett, A., Kohl, S., Taurina, G., Sukys, M., Haer-Wigman, L., Kowomiejska, K., Marques, João Pedro, Leroux, D., Cremers, F.P.M., Roosing, S., Baere, E. de, Dollfus, H., Black, G.C., Sergouniotis, P.I., Sodi, A., Leroy, B.P., Cauwenbergh, Caroline Van, Liskova, P., Gronskov, K., Klett, A., Kohl, S., Taurina, G., Sukys, M., Haer-Wigman, L., Kowomiejska, K., Marques, João Pedro, Leroux, D., Cremers, F.P.M., Roosing, S., Baere, E. de, and Dollfus, H.

Abstract

Contains fulltext : 246089.pdf (Publisher’s version ) (Open Access)

Published
2021

21. Extending the Spectrum of EYS-Associated Retinal Disease to Macular Dystrophy

Author

Pierrache, L.H., Messchaert, M., Thiadens, A.A.H.J., Haer-Wigman, L., Jong-Hesse, Yvonne de, Zelst-Stams, W.A.G. van, Collin, R.W.J., Klaver, C.C.W., Born, L.I. van den, Pierrache, L.H., Messchaert, M., Thiadens, A.A.H.J., Haer-Wigman, L., Jong-Hesse, Yvonne de, Zelst-Stams, W.A.G. van, Collin, R.W.J., Klaver, C.C.W., and Born, L.I. van den

Abstract

Contains fulltext : 204215.pdf (publisher's version ) (Open Access)

Published
2019

22. Extending the Spectrum of EYS-Associated Retinal Disease to Macular Dystrophy

Author

Pierrache, L.H.M., Messchaert, M., Thiadens, A., Haer-Wigman, L, de Jong-Hesse, Y, van Zelst-Stams, W. A. G., Collin, R.W.J. (Rob), Klaver, C.C.W. (Caroline), Born, L.I. (Ingeborgh) van den, Pierrache, L.H.M., Messchaert, M., Thiadens, A., Haer-Wigman, L, de Jong-Hesse, Y, van Zelst-Stams, W. A. G., Collin, R.W.J. (Rob), Klaver, C.C.W. (Caroline), and Born, L.I. (Ingeborgh) van den

Abstract

PURPOSE. To assess the phenotypic variability and natural course of inherited retinal diseases (IRDs) caused by EYS mutations. METHODS. Multiethnic cohort study (N ¼ 30) with biallelic EYS variants from a clinical IRD database (retinitis pigmentosa [RP], N ¼ 27; cone-rod dystrophy [CRD], N ¼ 1; and macular dystrophy, N ¼ 2). In vitro minigene splice assay was performed to determine the effect on EYS pre-mRNA splicing of the c.1299þ5_1299þ8del variant in macular dystrophy patients. RESULTS. We found 27 different EYS variants in RP patients and 7 were novel. The rate of visual field loss of the V4e isopter area was 0.84 6 0.44 ln(deg2 ) per year, and the rate of visual acuity loss was 0.75 Early Treatment Diabetic Retinopathy Study letters per year. Ellipsoid zone width was correlated with area of the hyperautofluorescent ring, with rs ¼ 0.78 and P < 0.001. Rate of decline in ellipsoid zone width was 57 6 17 lm per year (P < 0.01) (n ¼ 14) or 3.69% 6 0.51% from baseline per year (P < 0.001). An isolated CRD patient carried a homozygous EYS variant (c.9405T>A), previously identified in RP patients. Two siblings with macular dystrophy carried compound heterozygous EYS variants: c.1299þ5_1299þ8del and c.6050G>T. The former was novel and shown to result in skipping of exon 8, and the latter was a known RP variant. CONCLUSIONS. We report on EYS-associated macular dystrophy, extending the spectrum of EYSassociated IRDs. We observed heterogeneity between RP patients in age of onset and disease progression. Identical EYS variants were found in cases with RP, CRD, and macular dystrophy. Screening for EYS variants in CRD and macular dystrophy patients might increase the diagnostic yield in previously unsolved cases.

Published
2019
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23. 1 in 38 individuals at risk of a dominant medically actionable disease

Author

Haer-Wigman, L., Schoot, Vyne van der, Feenstra, I., Vulto-van Silfhout, A.T., Gilissen, C.F., Brunner, H.G., Vissers, L.E.L.M., Yntema, H.G., Haer-Wigman, L., Schoot, Vyne van der, Feenstra, I., Vulto-van Silfhout, A.T., Gilissen, C.F., Brunner, H.G., Vissers, L.E.L.M., and Yntema, H.G.

Abstract

Contains fulltext : 200879.pdf (publisher's version ) (Closed access)

Published
2019

24. Extending the Spectrum of EYS-Associated Retinal Disease to Macular Dystrophy

Author

Pierrache, Laurence, Messchaert, M, Thiadens, Alberta, Haer-Wigman, L, de Jong-Hesse, Y, van Zelst-Stams, W A G, Collin, RWJ, Klaver, Caroline, van den Born, LI, Pierrache, Laurence, Messchaert, M, Thiadens, Alberta, Haer-Wigman, L, de Jong-Hesse, Y, van Zelst-Stams, W A G, Collin, RWJ, Klaver, Caroline, and van den Born, LI

Published
2019

25. Good cochlear implantation outcomes in subjects with mono-allelic <italic>WFS1-</italic>associated sensorineural hearing loss – a case series.

Author

Fehrmann, M. L. A., Lanting, C. P., Haer-Wigman, L., Mylanus, E. A. M., Huinck, W. J., and Pennings, R. J. E.

Subjects
*COCHLEAR implants, *SENSORINEURAL hearing loss, *ACOUSTIC stimulation, *SPEECH perception, *HEARING disorders, *AUDITORY neuropathy
Abstract

AbstractObjectiveDesignStudy sampleResultsConclusionThis study aimed to evaluate long-term cochlear implant (CI) outcomes in individuals with mono-allelic pathogenic variants in WFS1, which is associated with both Wolfram-like syndrome and DFNA6/14/38.Retrospective case series.Seven CI recipients, ranging from eight months to 58 years of age, were included in the study, including four with Wolfram-like syndrome and three with DFNA6/14/38. A total of ten cochlear implantations were performed among these subjects.At one-year post-implantation, a mean phoneme score of 90 ± 9% at 65 dB SPL in quiet was found, which remained stable up to ten years post-implantation with a mean phoneme score of 94 ± 6%. Despite these excellent outcomes, one subject achieved no speech recognition with CI and eventually became a non-user. This individual had a prolonged absence of auditory stimulation prior to implantation and encountered multiple challenges during rehabilitation.Individuals with Wolfram-like syndrome or DFNA6/14/38 demonstrate consistently good outcomes following implantation, which remain stable over time. These findings affirm cochlear implantation as an effective rehabilitation option for these individuals. Furthermore, the stable and good CI outcomes contradict the suggested link between WFS1-associated sensorineural hearing loss and auditory neuropathy. [ABSTRACT FROM AUTHOR]

Published
2024
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26. Identification of Inherited Retinal Disease-Associated Genetic Variants in 11 Candidate Genes

Author

Astuti, G.D.N, Born, L.I. van den, Khan, M.I., Hamel, C.P., Bocquet, B., Manes, G., Haer-Wigman, L., Hoyng, C.B., Cremers, F.P.M., Roosing, S., Astuti, G.D.N, Born, L.I. van den, Khan, M.I., Hamel, C.P., Bocquet, B., Manes, G., Haer-Wigman, L., Hoyng, C.B., Cremers, F.P.M., and Roosing, S.

Abstract

Contains fulltext : 183881.pdf (publisher's version ) (Open Access)

Published
2018

29. Missense mutations in the WD40 domain of AHI1 cause non-syndromic retinitis pigmentosa

Author

Nguyen, T.T.M., Hull, S., Roepman, R., Born, L.I. van den, Oud, M.M., Vrieze, E. de, Hetterschijt, L., Letteboer, S.J.F., Beersum, S.E.C. van, Blokland, E.A.W., Yntema, H.G., Cremers, F.P.M., Zwaag, P.A. van der, Arno, G., WIjk, E. van, Webster, A.R., Haer-Wigman, L., Nguyen, T.T.M., Hull, S., Roepman, R., Born, L.I. van den, Oud, M.M., Vrieze, E. de, Hetterschijt, L., Letteboer, S.J.F., Beersum, S.E.C. van, Blokland, E.A.W., Yntema, H.G., Cremers, F.P.M., Zwaag, P.A. van der, Arno, G., WIjk, E. van, Webster, A.R., and Haer-Wigman, L.

Abstract

Contains fulltext : 177221.pdf (Publisher’s version ) (Open Access), BACKGROUND: Recent findings suggesting that Abelson helper integration site 1 (AHI1) is involved in non-syndromic retinal disease have been debated, as the functional significance of identified missense variants was uncertain. We assessed whether AHI1 variants cause non-syndromic retinitis pigmentosa (RP). METHODS: Exome sequencing was performed in three probands with RP. The effects of the identified missense variants in AHI1 were predicted by three-dimensional structure homology modelling. Ciliary parameters were evaluated in patient's fibroblasts, and recombinant mutant proteins were expressed in ciliated retinal pigmented epithelium cells. RESULTS: In the three patients with RP, three sets of compound heterozygous variants were detected in AHI1 (c.2174G>A; p.Trp725* and c.2258A>T; p.Asp753Val, c.660delC; p.Ser221Glnfs*10 and c.2090C>T; p.Pro697Leu, c.2087A>G; p.His696Arg and c.2429C>T; p.Pro810Leu). All four missense variants were present in the conserved WD40 domain of Jouberin, the ciliary protein encoded by AHI1, with variable predicted implications for the domain structure. No significant changes in the percentage of ciliated cells, nor in cilium length or intraflagellar transport were detected. However, expression of mutant recombinant Jouberin in ciliated cells showed a significantly decreased enrichment at the ciliary base. CONCLUSIONS: This report confirms that mutations in AHI1 can underlie autosomal recessive RP. Moreover, it structurally and functionally validates the effect of the RP-associated AHI1 variants on protein function, thus proposing a new genotype-phenotype correlation for AHI1 mutation associated retinal ciliopathies.

Published
2017

30. Whole-Exome Sequencing Identifies Biallelic IDH3A Variants as a Cause of Retinitis Pigmentosa Accompanied by Pseudocoloboma

Author

Pierrache, L.H., Kimchi, A., Ratnapriya, R., Roberts, L., Astuti, G.D.N, Obolensky, A., Beryozkin, A., Tjon-Fo-Sang, M.J.H., Schuil, J., Klaver, C.C.W., Bongers, E.M.H.F., Haer-Wigman, L., Schalij, N., Breuning, M.H., Fischer, G.M., Banin, E., Ramesar, R.S., Swaroop, A., Born, L.I. van den, Sharon, D., Cremers, F.P.M., Pierrache, L.H., Kimchi, A., Ratnapriya, R., Roberts, L., Astuti, G.D.N, Obolensky, A., Beryozkin, A., Tjon-Fo-Sang, M.J.H., Schuil, J., Klaver, C.C.W., Bongers, E.M.H.F., Haer-Wigman, L., Schalij, N., Breuning, M.H., Fischer, G.M., Banin, E., Ramesar, R.S., Swaroop, A., Born, L.I. van den, Sharon, D., and Cremers, F.P.M.

Abstract

Item does not contain fulltext, PURPOSE: To identify the genetic cause of and describe the phenotype in 4 families with autosomal recessive retinitis pigmentosa (arRP) that can be associated with pseudocoloboma. DESIGN: Case series. PARTICIPANTS: Seven patients from 4 unrelated families with arRP, among whom 3 patients had bilateral early-onset macular pseudocoloboma. METHODS: We performed homozygosity mapping and whole-exome sequencing in 5 probands and 2 unaffected family members from 4 unrelated families. Subsequently, Sanger sequencing and segregation analysis were performed in additional family members. We reviewed the medical history of individuals carrying IDH3A variants and performed additional ophthalmic examinations, including full-field electroretinography, fundus photography, fundus autofluorescence imaging, and optical coherence tomography. MAIN OUTCOME MEASURES: IDH3A variants, age at diagnosis, visual acuity, fundus appearance, visual field, and full-field electroretinography, fundus autofluorescence, and optical coherence tomography findings. RESULTS: We identified 7 different variants in IDH3A in 4 unrelated families, that is, 5 missense, 1 nonsense, and 1 frameshift variant. All participants showed symptoms early in life, ranging from night blindness to decreased visual acuity, and were diagnosed between the ages of 1 and 11 years. Four participants with biallelic IDH3A variants displayed a typical arRP phenotype and 3 participants were diagnosed with arRP and pseudocoloboma of the macula. CONCLUSIONS: IDH3A variants were identified as a novel cause of typical arRP in some individuals associated with macular pseudocoloboma. We observed both phenotypes in 2 siblings carrying the same compound heterozygous variants, which could be explained by variable disease expression and warrants caution when making assertions about genotype-phenotype correlations.

Published
2017

31. Validation of the multiplex ligation-dependent probe amplification assay and its application on the distribution study of the major alleles of 17 blood group systems in Chinese donors from Guangzhou

Author

Ji, Y., Wen, J., Veldhuisen, B., Haer-Wigman, L., Wang, Z., Loden-van Straaten, M., Wei, L., Luo, G., Fu, Y., Schoot, C.E. van der, Ji, Y., Wen, J., Veldhuisen, B., Haer-Wigman, L., Wang, Z., Loden-van Straaten, M., Wei, L., Luo, G., Fu, Y., and Schoot, C.E. van der

Abstract

Item does not contain fulltext, BACKGROUND: Genotyping platforms for common red blood cell (RBC) antigens have been successfully applied in Caucasian and black populations but not in Chinese populations. In this study, a genotyping assay based on multiplex ligation-dependent probe amplification (MLPA) technology was applied in a Chinese population to validate the MLPA probes. Subsequently, the comprehensive distribution of 17 blood group systems also was obtained. STUDY DESIGN AND METHODS: DNA samples from 200 Chinese donors were extracted and genotyped using the blood-MLPA assay. To confirm the MLPA results, a second independent genotyping assay (ID Core+) was conducted in 40 donors, and serological typing of 14 blood-group antigens was performed in 91 donors. In donors who had abnormal copy numbers of an allele (DI and GYPB) determined by MLPA, additional experiments were performed (polymerase chain reaction, sequencing, and flow cytometry analysis). RESULTS: The genotyping results obtained using the blood-MLPA and ID Core+ assays were consistent. Serological data were consistent with the genotyping results except for one donor who had a Lu(a-b-) phenotype. Of the 17 blood group systems, the distribution of the MNS, Duffy, Kidd, Diego, Yt, and Dombrock systems was polymorphic. The Mur and Sta antigens of the MNS system were distributed with a frequency of 9% (18 of 200) and 2% (4 of 200), respectively. One donor with chimerism and one who carried a novel DI*02(A845V) allele, which predicts the depression of Dib antigen expression, were identified. CONCLUSIONS: The blood-MLPA assay could easily identify the common blood-group alleles and correctly predicted phenotype in the Chinese population. The Mur and Sta antigens were distributed with high frequency in a Southern Chinese Han population.

Published
2017

32. RHD genotype and zygosity analysis in the Chinese Southern Han D+, D- and D variant donors using the multiplex ligation-dependent probe amplification assay

Author

Ji, Y.L., Luo, H., Wen, J.Z., Haer-Wigman, L., Veldhuisen, B., Wei, L., Wang, Z., Ligthart, P., Loden-van Straaten, M., Fu, Y.S., Schoot, C.E. van der, Luo, G.P., Ji, Y.L., Luo, H., Wen, J.Z., Haer-Wigman, L., Veldhuisen, B., Wei, L., Wang, Z., Ligthart, P., Loden-van Straaten, M., Fu, Y.S., Schoot, C.E. van der, and Luo, G.P.

Abstract

Item does not contain fulltext, BACKGROUND AND OBJECTIVES: Several comprehensive genotyping platforms for determining red blood cell (RBC) antigens have been established and validated for use in the Caucasian and Black populations, but not for the Chinese. The multiplex ligation-dependent probe amplification (MLPA) assay was validated for RHD genotyping in the Chinese. MATERIALS AND METHODS: The blood samples of 200 D+, 200 D- and 62 D variant Chinese donors were collected. RhD antigen was routinely typed by serological method. D variant phenotype was determined by an anti-D panel (D-Screen), when RBCs were available. The RHD genotype and its zygosity were analysed with the RH-MLPA technique. When the MLPA was unable to identify a RHD variant, direct sequencing of all exons of the RHD gene was performed. RESULTS: In 200 D+ donors, DD (168/200, 84%), D (12/200, 6%), DDD genotype (1/200) and D variant allele carriers (19/200, 9.5%) were found. In 200 D- donors, six reported RHD alleles, RHD*01EL.01, RHD*01N.03, RHD*01N.05, RHD*01N.16, RHD*DFR2 and RHD*weak partial 15 and one novel RHD*1154T allele were identified in 36.5% (73/200) of them. In 62 D variant donors, three novel RHD alleles, RHD*79_81delCTC, RHD*710T and RHD*689A, and twelve reported alleles, RHD*DVI.3, RHD*weak partial 15, RHD*DVI.4, RHD*01EL.01, RHD*01N.03, RHD*DLO, RHD*DV.5, RHD*D-CE(2-10), RHD*730C, RHD*weak D type 25, 33 and 72, were identified, either alone or in combination. CONCLUSION: The RH-MLPA assay correctly identified the common RHD variant alleles in the Chinese population. However, DNA sequencing was required to identify certain alleles; probes to detect these alleles should be added into the assay.

Published
2017

33. Diagnostic exome sequencing in 266 Dutch patients with visual impairment

Author

Haer-Wigman, L., Zelst-Stams, W.A.G. van, Pfundt, R.P., Born, L.I. van den, Klaver, C.C.W., Verheij, J.B.G.M., Hoyng, C.B., Breuning, M.H., Boon, C.J.F., Kievit, A.J., Verhoeven, V.J., Pott, J.W., Sallevelt, S.C., Hagen, J.M. van, Plomp, A.S., Kroes, H.Y., Lelieveld, S.H., Hehir-Kwa, J.Y., Castelein, S., Nelen, M.R., Scheffer, H., Lugtenberg, D., Cremers, F.P.M., Hoefsloot, L., Yntema, H.G., Haer-Wigman, L., Zelst-Stams, W.A.G. van, Pfundt, R.P., Born, L.I. van den, Klaver, C.C.W., Verheij, J.B.G.M., Hoyng, C.B., Breuning, M.H., Boon, C.J.F., Kievit, A.J., Verhoeven, V.J., Pott, J.W., Sallevelt, S.C., Hagen, J.M. van, Plomp, A.S., Kroes, H.Y., Lelieveld, S.H., Hehir-Kwa, J.Y., Castelein, S., Nelen, M.R., Scheffer, H., Lugtenberg, D., Cremers, F.P.M., Hoefsloot, L., and Yntema, H.G.

Abstract

Contains fulltext : 174726.pdf (publisher's version ) (Open Access), Inherited eye disorders have a large clinical and genetic heterogeneity, which makes genetic diagnosis cumbersome. An exome-sequencing approach was developed in which data analysis was divided into two steps: the vision gene panel and exome analysis. In the vision gene panel analysis, variants in genes known to cause inherited eye disorders were assessed for pathogenicity. If no causative variants were detected and when the patient consented, the entire exome data was analyzed. A total of 266 Dutch patients with different types of inherited eye disorders, including inherited retinal dystrophies, cataract, developmental eye disorders and optic atrophy, were investigated. In the vision gene panel analysis (likely), causative variants were detected in 49% and in the exome analysis in an additional 2% of the patients. The highest detection rate of (likely) causative variants was in patients with inherited retinal dystrophies, for instance a yield of 63% in patients with retinitis pigmentosa. In patients with developmental eye defects, cataract and optic atrophy, the detection rate was 50, 33 and 17%, respectively. An exome-sequencing approach enables a genetic diagnosis in patients with different types of inherited eye disorders using one test. The exome approach has the same detection rate as targeted panel sequencing tests, but offers a number of advantages. For instance, the vision gene panel can be frequently and easily updated with additional (novel) eye disorder genes. Determination of the genetic diagnosis improved the clinical diagnosis, regarding the assessment of the inheritance pattern as well as future disease perspective.

Published
2017

34. Diagnostic exome sequencing in 266 Dutch patients with visual impairment

Author

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

Abstract

Inherited eye disorders have a large clinical and genetic heterogeneity, which makes genetic diagnosis cumbersome. An exome-sequencing approach was developed in which data analysis was divided into two steps: the vision gene panel and exome analysis. In the vision gene panel analysis, variants in genes known to cause inherited eye disorders were assessed for pathogenicity. If no causative variants were detected and when the patient consented, the entire exome data was analyzed. A total of 266 Dutch patients with different types of inherited eye disorders, including inherited retinal dystrophies, cataract, developmental eye disorders and optic atrophy, were investigated. In the vision gene panel analysis (likely), causative variants were detected in 49% and in the exome analysis in an additional 2% of the patients. The highest detection rate of (likely) causative variants was in patients with inherited retinal dystrophies, for instance a yield of 63% in patients with retinitis pigmentosa. In patients with developmental eye defects, cataract and optic atrophy, the detection rate was 50, 33 and 17%, respectively. An exome-sequencing approach enables a genetic diagnosis in patients with different types of inherited eye disorders using one test. The exome approach has the same detection rate as targeted panel sequencing tests, but offers a number of advantages. For instance, the vision gene panel can be frequently and easily updated with additional (novel) eye disorder genes. Determination of the genetic diagnosis improved the clinical diagnosis, regarding the assessment of the inheritance pattern as well as future disease perspective.

Published
2017
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35. An Expanded Multi-Organ Disease Phenotype Associated with Mutations in YARS

Author

Tracewska-Siemiatkowska, A., Haer-Wigman, L., Bosch, D.G.M., Nickerson, D., Bamshad, M.J., Vorst, J.M. van de, Rendtorff, N.D., Moller, C., Kjellstrom, U., Andreasson, S., Cremers, F.P.M., Tranebjaerg, L., Tracewska-Siemiatkowska, A., Haer-Wigman, L., Bosch, D.G.M., Nickerson, D., Bamshad, M.J., Vorst, J.M. van de, Rendtorff, N.D., Moller, C., Kjellstrom, U., Andreasson, S., Cremers, F.P.M., and Tranebjaerg, L.

Abstract

Contains fulltext : 182610.pdf (publisher's version ) (Open Access), Whole exome sequence analysis was performed in a Swedish mother-father-affected proband trio with a phenotype characterized by progressive retinal degeneration with congenital nystagmus, profound congenital hearing impairment, primary amenorrhea, agenesis of the corpus callosum, and liver disease. A homozygous variant c.806T > C, p.(F269S) in the tyrosyl-tRNA synthetase gene (YARS) was the only identified candidate variant consistent with autosomal recessive inheritance. Mutations in YARS have previously been associated with both autosomal dominant Charcot-Marie-Tooth syndrome and a recently reported autosomal recessive multiorgan disease. Herein, we propose that mutations in YARS underlie another clinical phenotype adding a second variant of the disease, including retinitis pigmentosa and deafness, to the spectrum of YARS-associated disorders.

Published
2017

36. Diagnostic exome sequencing in 266 Dutch patients with visual impairment

Author

Haer-Wigman, L, van Zelst-Stams, W A G, Pfundt, R, van den Born, LI, Klaver, Caroline, Verheij, J, Hoyng, CB, Breuning, MH, Boon, CJF, Kievit, Anneke, Verhoeven, Virginie, Pott, JWR, Sallevelt, S, van Hagen, JM, Plomp, AS, Kroes, HY, Lelieveld, SH, Hehir-Kwa, JY, Castelein, S, Nelen, M, Scheffer, H, Lugtenberg, D, Cremers, FPM, Hoefsloot, EH, Yntema, HG, Haer-Wigman, L, van Zelst-Stams, W A G, Pfundt, R, van den Born, LI, Klaver, Caroline, Verheij, J, Hoyng, CB, Breuning, MH, Boon, CJF, Kievit, Anneke, Verhoeven, Virginie, Pott, JWR, Sallevelt, S, van Hagen, JM, Plomp, AS, Kroes, HY, Lelieveld, SH, Hehir-Kwa, JY, Castelein, S, Nelen, M, Scheffer, H, Lugtenberg, D, Cremers, FPM, Hoefsloot, EH, and Yntema, HG

Published
2017

37. RHDgenotype and zygosity analysis in the Chinese Southern Han D+, D− and D variant donors using the multiplex ligation-dependent probe amplification assay

Author

Ji, Y. L., primary, Luo, H., additional, Wen, J. Z., additional, Haer-Wigman, L., additional, Veldhuisen, B., additional, Wei, L., additional, Wang, Z., additional, Ligthart, P., additional, Lodén-van Straaten, M., additional, Fu, Y. S., additional, van der Schoot, C. E., additional, and Luo, G. P., additional

Published
2017
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38. Stable long-term outcomes after cochlear implantation in subjects with TMPRSS3associated hearing loss: a retrospective multicentre study

Author

Fehrmann, M. L. A., Huinck, W. J., Thijssen, M. E. G., Haer-Wigman, L., Yntema, H. G., Rotteveel, L. J. C., Widdershoven, J. C. C., Goderie, T., van Dooren, M. F., Hoefsloot, E. H., van der Schroeff, M. P., Mylanus, E. A. M., Lanting, C. P., and Pennings, R. J. E.

Abstract

Background: The spiral ganglion hypothesis suggests that pathogenic variants in genes preferentially expressed in the spiral ganglion nerves (SGN), may lead to poor cochlear implant (CI) performance. It was long thought that TMPRSS3 was particularly expressed in the SGNs. However, this is not in line with recent reviews evaluating CI performance in subjects with TMPRSS3-associated sensorineural hearing loss (SNHL) reporting overall beneficial outcomes. These outcomes are, however, based on variable follow-up times of, in general, 1 year or less. Therefore, we aimed to 1. evaluate long-term outcomes after CI implantation of speech recognition in quiet in subjects with TMPRSS3-associated SNHL, and 2. test the spiral ganglion hypothesis using the TMPRSS3-group. Methods: This retrospective, multicentre study evaluated long-term CI performance in a Dutch population with TMPRSS3-associated SNHL. The phoneme scores at 70 dB with CI in the TMPRSS3-group were compared to a control group of fully genotyped cochlear implant users with post-lingual SNHL without genes affecting the SGN, or severe anatomical inner ear malformations. CI-recipients with a phoneme score ≤ 70% at least 1-year post-implantation were considered poor performers and were evaluated in more detail. Results: The TMPRSS3 groupconsisted of 29 subjects (N = 33 ears), and the control group of 62 subjects (N = 67 ears). For the TMPRSS3-group, we found an average phoneme score of 89% after 5 years, which remained stable up to 10 years post-implantation. At both 5 and 10-year follow-up, no difference was found in speech recognition in quiet between both groups (p= 0.830 and p= 0.987, respectively). Despite these overall adequate CI outcomes, six CI recipients had a phoneme score of ≤ 70% and were considered poor performers. The latter was observed in subjects with residual hearing post-implantation or older age at implantation. Conclusion: Subjects with TMPRSS3-associated SNHL have adequate and stable long-term outcomes after cochlear implantation, equal to the performance of genotyped patient with affected genes not expressed in the SGN. These findings are not in line with the spiral ganglion hypothesis. However, more recent studies showed that TMPRSS3 is mainly expressed in the hair cells with only limited SGN expression. Therefore, we cannot confirm nor refute the spiral ganglion hypothesis.

Published
2023
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39. Frequency and characterization of known and novel RHD variant alleles in 37 782 Dutch D-negative pregnant women

Author

Stegmann, T.C., Veldhuisen, B., Bijman, R., Thurik, F.F., Bossers, B., Cheroutre, G., Jonkers, R., Ligthart, P., Haas, M. de, Haer-Wigman, L., Schoot, C.E. van der, Stegmann, T.C., Veldhuisen, B., Bijman, R., Thurik, F.F., Bossers, B., Cheroutre, G., Jonkers, R., Ligthart, P., Haas, M. de, Haer-Wigman, L., and Schoot, C.E. van der

Abstract

Contains fulltext : 167810.pdf (publisher's version ) (Open Access), To guide anti-D prophylaxis, Dutch D- pregnant women are offered a quantitative fetal-RHD-genotyping assay to determine the RHD status of their fetus. This allowed us to determine the frequency of different maternal RHD variants in 37 782 serologically D- pregnant women. A variant allele is present in at least 0.96% of Dutch D- pregnant women The D- serology could be confirmed after further serological testing in only 54% of these women, which emphasizes the potential relevance of genotyping of blood donors. 43 different RHD variant alleles were detected, including 15 novel alleles (11 null-, 2 partial D- and 2 DEL-alleles). Of those novel null alleles, one allele contained a single missense mutation (RHD*443C>G) and one allele had a single amino acid deletion (RHD*424_426del). The D- phenotype was confirmed by transduction of human D- erythroblasts, consolidating that, for the first time, a single amino acid change or deletion causes the D- phenotype. Transduction also confirmed the phenotypes for the two new variant DEL-alleles (RHD*721A>C and RHD*884T>C) and the novel partial RHD*492C>A allele. Notably, in three additional cases the DEL phenotype was observed but sequencing of the coding sequence, flanking introns and promoter region revealed an apparently wild-type RHD allele without mutations.

Published
2016

40. Mutations in the polyglutamylase gene TTLL5, expressed in photoreceptor cells and spermatozoa, are associated with cone-rod degeneration and reduced male fertility

Author

Bedoni, N., Haer-Wigman, L., Vaclavik, Veronika, Tran, Viet H., Farinelli, P., Balzano, S., Hoyng, C.B., Bax, N.M., Klaver, C.C.W., Cremers, F.P.M., Munier, Francis L., Rivolta, C., Bedoni, N., Haer-Wigman, L., Vaclavik, Veronika, Tran, Viet H., Farinelli, P., Balzano, S., Hoyng, C.B., Bax, N.M., Klaver, C.C.W., Cremers, F.P.M., Munier, Francis L., and Rivolta, C.

Abstract

Item does not contain fulltext

Published
2016

41. Identification of a novel frequent RHCE*ce308T variant allele in Chinese D- individuals, resulting in a C+c- phenotype

Author

Stegmann, T.C., Ji, Y., Bijman, R., Wang, Z., Wen, J., Wei, L., Veldhuisen, B., Haer-Wigman, L., Lighthart, P., Loden-van Straaten, M., Luo, G., Schoot, C.E. van der, Stegmann, T.C., Ji, Y., Bijman, R., Wang, Z., Wen, J., Wei, L., Veldhuisen, B., Haer-Wigman, L., Lighthart, P., Loden-van Straaten, M., Luo, G., and Schoot, C.E. van der

Abstract

Item does not contain fulltext, BACKGROUND: The RHCE allele is highly polymorphic; more than 60 variants have been described leading to diminished expression of C, c, E, and e antigens. Not much is known about the prevalence of RHCE variants in the Chinese population. Individuals carrying a variant are at risk to develop alloantibodies in response to mismatched pregnancy or transfusion. In this study, phenotyping and genotyping of the RHCE allele in Chinese donors revealed a new clinically relevant mutation. STUDY DESIGN AND METHODS: Blood samples from 200 D- and 200 D+ Chinese donors were analyzed by the RH multiplex ligation-dependent probe amplification (MLPA) assay and compared to serologically typed RhCE phenotypes, when available. All exons of the RHCE gene were sequenced in samples with aberrant genotyping results. The phenotype of the new variant RHCE allele was tested by transducing cultured human erythroblasts. RESULTS: Aberrant copy numbers for Exon 2 of the RHCE gene were discovered by MLPA in six D- donors (6/200), but not in D+ donors (0/200). Sequencing of the RHCE gene in these six donors identified a new variant RHCE*ce308C>T (p.103Pro>Leu) allele with an allele frequency of 0.015 within the D- individuals in this study. This variant was not detected in D+ individuals showing linkage with the D- haplotype. Serologically weak C expression and loss of c expression was demonstrated on donor red blood cells. In vitro transfection studies of the RHCE*ce308T variant in cDe/ce and CDe/CDe erythroblasts confirmed that the variant is associated with anti-C reactivity while abolishing c expression. CONCLUSION: Genotyping of individuals carrying this variant by standard RHCE genotyping might falsely predict a C- phenotype or a c+ phenotype. This new variant should be taken into account in RHCE genotyping assays designed for the Chinese population.

Published
2016

42. Non-syndromic retinitis pigmentosa due to mutations in the mucopolysaccharidosis type IIIC gene, heparan-alpha-glucosaminide N-acetyltransferase (HGSNAT)

Author

Haer-Wigman, L., Newman, H., Leibu, R., Bax, N.M., Baris, H.N., Rizel, L., Banin, E., Massarweh, A., Roosing, S., Lefeber, D.J., Zonneveld-Vrieling, M.N., Isakov, O., Shomron, N., Sharon, D., Hollander, A.I. den, Hoyng, C.B., Cremers, F.P.M., Ben-Yosef, T., Haer-Wigman, L., Newman, H., Leibu, R., Bax, N.M., Baris, H.N., Rizel, L., Banin, E., Massarweh, A., Roosing, S., Lefeber, D.J., Zonneveld-Vrieling, M.N., Isakov, O., Shomron, N., Sharon, D., Hollander, A.I. den, Hoyng, C.B., Cremers, F.P.M., and Ben-Yosef, T.

Abstract

Contains fulltext : 153514.pdf (Publisher’s version ) (Open Access), Retinitis pigmentosa (RP), the most common form of inherited retinal degeneration, is clinically and genetically heterogeneous and can appear as syndromic or non-syndromic. Mucopolysaccharidosis type IIIC (MPS IIIC) is a lethal disorder, caused by mutations in the heparan-alpha-glucosaminide N-acetyltransferase (HGSNAT) gene and characterized by progressive neurological deterioration, with retinal degeneration as a prominent feature. We identified HGSNAT mutations in six patients with non-syndromic RP. Whole exome sequencing (WES) in an Ashkenazi Jewish Israeli RP patient revealed a novel homozygous HGSNAT variant, c.370A>T, which leads to partial skipping of exon 3. Screening of 66 Ashkenazi RP index cases revealed an additional family with two siblings homozygous for c.370A>T. WES in three Dutch siblings with RP revealed a complex HGSNAT variant, c.[398G>C; 1843G>A] on one allele, and c.1843G>A on the other allele. HGSNAT activity levels in blood leukocytes of patients were reduced compared with healthy controls, but usually higher than those in MPS IIIC patients. All patients were diagnosed with non-syndromic RP and did not exhibit neurological deterioration, or any phenotypic features consistent with MPS IIIC. Furthermore, four of the patients were over 60 years old, exceeding by far the life expectancy of MPS IIIC patients. HGSNAT is highly expressed in the mouse retina, and we hypothesize that the retina requires higher HGSNAT activity to maintain proper function, compared with other tissues associated with MPS IIIC, such as the brain. This report broadens the spectrum of phenotypes associated with HGSNAT mutations and highlights the critical function of HGSNAT in the human retina.

Published
2015

43. Homozygosity mapping and targeted sanger sequencing reveal genetic defects underlying inherited retinal disease in families from pakistan

Author

Maria, M., Ajmal, M., Azam, M., Waheed, N.K., Siddiqui, S.N., Mustafa, B., Ayub, H., Ali, L., Ahmad, S., Micheal, S., Hussain, A., Shah, S.T., Ali, S.H., Ahmed, W., Khan, Y.M., Hollander, A.I. den, Haer-Wigman, L., Collin, R.W.J., Khan, M.I., Qamar, R., Cremers, F.P.M., Maria, M., Ajmal, M., Azam, M., Waheed, N.K., Siddiqui, S.N., Mustafa, B., Ayub, H., Ali, L., Ahmad, S., Micheal, S., Hussain, A., Shah, S.T., Ali, S.H., Ahmed, W., Khan, Y.M., Hollander, A.I. den, Haer-Wigman, L., Collin, R.W.J., Khan, M.I., Qamar, R., and Cremers, F.P.M.

Abstract

Contains fulltext : 152997.PDF (publisher's version ) (Open Access), BACKGROUND: Homozygosity mapping has facilitated the identification of the genetic causes underlying inherited diseases, particularly in consanguineous families with multiple affected individuals. This knowledge has also resulted in a mutation dataset that can be used in a cost and time effective manner to screen frequent population-specific genetic variations associated with diseases such as inherited retinal disease (IRD). METHODS: We genetically screened 13 families from a cohort of 81 Pakistani IRD families diagnosed with Leber congenital amaurosis (LCA), retinitis pigmentosa (RP), congenital stationary night blindness (CSNB), or cone dystrophy (CD). We employed genome-wide single nucleotide polymorphism (SNP) array analysis to identify homozygous regions shared by affected individuals and performed Sanger sequencing of IRD-associated genes located in the sizeable homozygous regions. In addition, based on population specific mutation data we performed targeted Sanger sequencing (TSS) of frequent variants in AIPL1, CEP290, CRB1, GUCY2D, LCA5, RPGRIP1 and TULP1, in probands from 28 LCA families. RESULTS: Homozygosity mapping and Sanger sequencing of IRD-associated genes revealed the underlying mutations in 10 families. TSS revealed causative variants in three families. In these 13 families four novel mutations were identified in CNGA1, CNGB1, GUCY2D, and RPGRIP1. CONCLUSIONS: Homozygosity mapping and TSS revealed the underlying genetic cause in 13 IRD families, which is useful for genetic counseling as well as therapeutic interventions that are likely to become available in the near future.

Published
2015

44. Impact of genetic variation in the SMIM1 gene on Vel expression levels.

Author

Haer-Wigman, L., Stegmann, T.C., Solati, S., Ait Soussan, A., Beckers, E., Harst, P. van der, Hulst-Sundermeijer, M. van, Ligthart, P., Rhenen, D. van, Schepers, H., Haas, M. de, Schoot, C.E. van der, Haer-Wigman, L., Stegmann, T.C., Solati, S., Ait Soussan, A., Beckers, E., Harst, P. van der, Hulst-Sundermeijer, M. van, Ligthart, P., Rhenen, D. van, Schepers, H., Haas, M. de, and Schoot, C.E. van der

Abstract

Item does not contain fulltext

Published
2015

46. Non-syndromic retinitis pigmentosa due to mutations in the mucopolysaccharidosis type IIIC gene, heparan-alpha-glucosaminide N-acetyltransferase (HGSNAT)

Author

Haer-Wigman, L., primary, Newman, H., additional, Leibu, R., additional, Bax, N. M., additional, Baris, H. N., additional, Rizel, L., additional, Banin, E., additional, Massarweh, A., additional, Roosing, S., additional, Lefeber, D. J., additional, Zonneveld-Vrieling, M. N., additional, Isakov, O., additional, Shomron, N., additional, Sharon, D., additional, Den Hollander, A. I., additional, Hoyng, C. B., additional, Cremers, F. P. M., additional, and Ben-Yosef, T., additional

Published
2015
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47. Utilization of automated cilia analysis to characterize novel INPP5E variants in patients with non-syndromic retinitis pigmentosa.

Author

Whiting KR, Haer-Wigman L, Florijn RJ, van Beek R, Oud MM, Plomp AS, Boon CJF, Kroes HY, and Roepman R

Subjects
Humans, Male, Female, Phenotype, Fibroblasts metabolism, Fibroblasts pathology, Mutation, Adult, Retinitis Pigmentosa genetics, Retinitis Pigmentosa pathology, Cilia pathology, Cilia genetics, Phosphoric Monoester Hydrolases genetics
Abstract

INPP5E encodes inositol polyphosphate-5-phosphatase E, an enzyme involved in regulating the phosphatidylinositol (PIP) makeup of the primary cilium membrane. Pathogenic variants in INPP5E hence cause a variety of ciliopathies: genetic disorders caused by dysfunctional cilia. While the majority of these disorders are syndromic, such as the neuronal ciliopathy Joubert syndrome, in some cases patients will present with an isolated phenotype-most commonly non-syndromic retinitis pigmentosa (RP). Here, we report two novel variants in INPP5E identified in two patients with non-syndromic RP: patient 1 with compound heterozygous variants (c.1516C > T, p.(Q506*), and c.847G > A, p.(A283T)) and patient 2 with a homozygous variant (c.1073C > T, p.(P358L)). To determine whether these variants were causative for the phenotype in the patients, automated ciliary phenotyping of patient-derived dermal fibroblasts was performed for percent ciliation, cilium length, retrograde IFT trafficking, and INPP5E localization. In both patients, a decrease in ciliary length and loss of INPP5E localization in the primary cilia were seen. With these molecular findings, we can confirm functionally that the novel variants in INPP5E are causative for the RP phenotypes seen in both patients. Additionally, this study demonstrates the usefulness of utilizing ciliary phenotyping as an assistant in ciliopathy diagnosis and phenotyping., Competing Interests: Competing interests The authors declare no competing interests. Ethics approval Institutional ethics approval was not required. All individuals or their legal guardians provided informed written consent for genetic testing and publication of clinical details and images., (© 2024. The Author(s).)

Published
2024
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48. Long-Term Outcomes of Cochlear Implantation in Usher Syndrome.

Author

Fehrmann MLA, Lanting CP, Haer-Wigman L, Yntema HG, Mylanus EAM, Huinck WJ, and Pennings RJE

Subjects
Humans, Male, Female, Retrospective Studies, Adult, Child, Middle Aged, Adolescent, Young Adult, Treatment Outcome, Child, Preschool, Speech Perception, Hearing Loss, Sensorineural surgery, Hearing Loss, Sensorineural rehabilitation, Usher Syndromes surgery, Cochlear Implantation
Abstract

Objectives: Usher syndrome (USH), characterized by bilateral sensorineural hearing loss (SNHL) and retinitis pigmentosa (RP), prompts increased reliance on hearing due to progressive visual deterioration. It can be categorized into three subtypes: USH type 1 (USH1), characterized by severe to profound congenital SNHL, childhood-onset RP, and vestibular areflexia; USH type 2 (USH2), presenting with moderate to severe progressive SNHL and RP onset in the second decade, with or without vestibular dysfunction; and USH type 3 (USH3), featuring variable progressive SNHL beginning in childhood, variable RP onset, and diverse vestibular function. Previous studies evaluating cochlear implant (CI) outcomes in individuals with USH used varying or short follow-up durations, while others did not evaluate outcomes for each subtype separately. This study evaluates long-term CI performance in subjects with USH, at both short-term and long-term, considering each subtype separately., Design: This retrospective, observational cohort study identified 36 CI recipients (53 ears) who were categorized into four different groups: early-implanted USH1 (first CI at ≤7 years of age), late-implanted USH1 (first CI at ≥8 years of age), USH2 and USH3. Phoneme scores at 65 dB SPL with CI were evaluated at 1 year, ≥2 years (mid-term), and ≥5 years postimplantation (long-term). Each subtype was analyzed separately due to the significant variability in phenotype observed among the three subtypes., Results: Early-implanted USH1-subjects (N = 23 ears) achieved excellent long-term phoneme scores (100% [interquartile ranges {IQR} = 95 to 100]), with younger age at implantation significantly correlating with better CI outcomes. Simultaneously implanted subjects had significantly better outcomes than sequentially implanted subjects ( p = 0.028). Late-implanted USH1 subjects (N = 3 ears) used CI solely for sound detection and showed a mean phoneme discrimination score of 12% (IQR = 0 to 12), while still expressing satisfaction with ambient sound detection. In the USH2 group (N = 23 ears), a long-term mean phoneme score of 85% (IQR = 81 to 95) was found. Better outcomes were associated with younger age at implantation and higher preimplantation speech perception scores. USH3-subjects (N = 7 ears) achieved a mean postimplantation phoneme score of 71% (IQR = 45 to 91)., Conclusions: This study is currently one of the largest and most comprehensive studies evaluating CI outcomes in individuals with USH, demonstrating that overall, individuals with USH benefit from CI at both short- and long-term follow-up. Due to the considerable variability in phenotype observed among the three subtypes, each subtype was analyzed separately, resulting in smaller sample sizes. For USH1 subjects, optimal CI outcomes are expected with early simultaneous bilateral implantation. Late implantation in USH1 provides signaling function, but achieved speech recognition is insufficient for oral communication. In USH2 and USH3, favorable CI outcomes are expected, especially if individuals exhibit sufficient speech recognition with hearing aids and receive ample auditory stimulation preimplantation. Early implantation is recommended for USH2, given the progressive nature of hearing loss and concomitant severe visual impairment. In comparison with USH2, predicting outcomes in USH3 remains challenging due to the variability found. Counseling for USH2 and USH3 should highlight early implantation benefits and encourage hearing aid use., Competing Interests: The authors have no conflicts of interest to disclose., (Copyright © 2024 The Authors. Ear & Hearing is published on behalf of the American Auditory Society, by Wolters Kluwer Health, Inc.)

Published
2024
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49. Characteristics of autosomal dominant WFS1-associated optic neuropathy and its comparability to OPA1-associated autosomal dominant optic atrophy.

Author

de Muijnck C, Haer-Wigman L, van Everdingen JAM, Lushchyk T, Heutinck PAT, van Dooren MF, Kievit AJA, Verhoeven VJM, Simon MEH, Wasmann RA, Notting IC, De Baere E, Walraedt S, De Zaeytijd J, Van den Broeck F, Leroy BP, Boon CJF, and van Genderen MM

Subjects
Adolescent, Adult, Aged, Child, Female, Humans, Male, Middle Aged, Young Adult, Wolfram Syndrome genetics, GTP Phosphohydrolases genetics, Membrane Proteins genetics, Mutation, Optic Atrophy, Autosomal Dominant genetics, Optic Atrophy, Autosomal Dominant pathology, Phenotype
Abstract

This study aims to describe the ophthalmic characteristics of autosomal dominant (AD) WFS1-associated optic atrophy (AD WFS1-OA), and to explore phenotypic differences with dominant optic atrophy (DOA) caused by mutations in the OPA1-gene. WFS1-associated diseases, or 'wolframinopathies', exhibit a spectrum of ocular and systemic phenotypes, of which the autosomal recessive Wolfram syndrome has been the most extensively studied. AD mutations in WFS1 also cause various phenotypical changes including OA. The most common phenotype in AD WFS1-associated disease, the combination of OA and hearing loss (HL), clinically resembles the 'plus' phenotype of DOA. We performed a comprehensive medical record review across tertiary referral centers in the Netherlands and Belgium resulting in 22 patients with heterozygous WFS1 variants. Eighteen (82%) had HL in addition to OA. Diabetes mellitus was found in 7 (32%). Four patients had isolated OA. One patient had an unusual phenotype with anterior chamber abnormalities and malformations of the extremities. Compared to DOA, AD WFS1-OA patients had different color vision abnormalities (red-green vs blue-yellow in DOA), abnormal OPL lamination on macular OCT (absent in DOA), more generalized thinning of the retinal nerve fiber layer, and more reduced and delayed pattern reversal visual evoked potentials., (© 2024. The Author(s).)

Published
2024
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50. Uncovering recessive alleles in rare Mendelian disorders by genome sequencing of 174 individuals with monoallelic pathogenic variants.

Author

Schobers G, Pennings M, de Vries J, Kwint M, van Reeuwijk J, Corominas Galbany J, van Beek R, Kamping E, Timmermans R, Kamsteeg EJ, Haer-Wigman L, Cremers FPM, Roosing S, Gilissen C, Kremer H, Brunner HG, Yntema HG, and Vissers LELM

Abstract

Clinical exome sequencing (ES) has facilitated genetic diagnosis in individuals with a rare genetic disorder by analysis of all protein-coding sequences in a single experiment. However, in 40-60% of patients, a conclusive diagnosis remains elusive. In 2-5% of these individuals, ES does identify a disease-associated monoallelic variant in a recessive disorder. We hypothesized that short-read genome sequencing (GS) might uncover a pathogenic variant on the second allele, thereby increasing diagnostic yield. We performed GS for 174 individuals in whom ES identified a monoallelic pathogenic variant in a gene associated with recessive disease related to their phenotype. GS interpretation was limited to the (non-)coding parts of the gene in which this first pathogenic variant was identified, focusing on splice-disrupting variants. Firstly, we uncovered a second pathogenic variant affecting coding sequence in five individuals, including two SNV/indel variants, two copy number variants, and one insertion. Secondly, for 24 individuals, we identified a total of 31 rare non-coding intronic SNV/indel variants, all predicted to disrupt splicing. Using functional follow-up assays, we confirmed an effect on splicing for three of these variants (in ABCA4, POLR3A and COL4A4) in three individuals. In summary, we identified a (likely) pathogenic second variant in 4.6% (8/174), and a possible diagnosis for 12.1% (21/174) of our cohort. Hence, when performing GS as first-tier diagnostic test, including the interpretation of SVs and rare intronic variants in known recessive disease genes, the overall diagnostic yield of rare disease will increase. The added diagnostic value of GS for recessive disease In our cohort of 174 individuals (84 males and 90 females) with a monoallelic pathogenic variant in genes associated with a wide and diverse range of recessive diseases (pie chart), using genome sequencing (GS) and a systematic approach (methods), we identified eight new diagnoses (4.6%). We identified a second likely pathogenic variant in eight individuals (results); In two a second coding variant was found, in three others, a rare non-coding SNV anticipated to disrupt splicing was uncovered, and in three individuals a structural rearrangement was identified (two copy number variants (CNV), and one structural variant (SV))., (© 2024. The Author(s), under exclusive licence to European Society of Human Genetics.)

Published
2024
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