Novel variants identified with next-generation sequencing in Polish patients with cone-rod dystrophy

PURPOSE: The aim of this study was to identify the molecular genetic basis of cone-rod dystrophy in 18 unrelated families of Polish origin. Cone-rod dystrophy is one of the inherited retinal dystrophies, which constitute a highly heterogeneous group of disorders characterized by progressive dysfunct...

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Autores principales: Wawrocka, Anna, Skorczyk-Werner, Anna, Wicher, Katarzyna, Niedziela, Zuzanna, Ploski, Rafal, Rydzanicz, Malgorzata, Sykulski, Maciej, Kociecki, Jaroslaw, Weisschuh, Nicole, Kohl, Susanne, Biskup, Saskia, Wissinger, Bernd, Krawczynski, Maciej R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Molecular Vision 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5937672/
https://www.ncbi.nlm.nih.gov/pubmed/29769798
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author Wawrocka, Anna
Skorczyk-Werner, Anna
Wicher, Katarzyna
Niedziela, Zuzanna
Ploski, Rafal
Rydzanicz, Malgorzata
Sykulski, Maciej
Kociecki, Jaroslaw
Weisschuh, Nicole
Kohl, Susanne
Biskup, Saskia
Wissinger, Bernd
Krawczynski, Maciej R.
author_facet Wawrocka, Anna
Skorczyk-Werner, Anna
Wicher, Katarzyna
Niedziela, Zuzanna
Ploski, Rafal
Rydzanicz, Malgorzata
Sykulski, Maciej
Kociecki, Jaroslaw
Weisschuh, Nicole
Kohl, Susanne
Biskup, Saskia
Wissinger, Bernd
Krawczynski, Maciej R.
author_sort Wawrocka, Anna
collection PubMed
description PURPOSE: The aim of this study was to identify the molecular genetic basis of cone-rod dystrophy in 18 unrelated families of Polish origin. Cone-rod dystrophy is one of the inherited retinal dystrophies, which constitute a highly heterogeneous group of disorders characterized by progressive dysfunction of photoreceptors and retinal pigment epithelium (RPE) cells. METHODS: The study group was composed of four groups of patients representing different Mendelian inheritance of the disease: autosomal dominant (AD), autosomal recessive (AR), X-linked recessive (XL), and autosomal recessive or X-linked recessive (AR/XL). The combined molecular strategy included Sanger sequencing of the RPGR-ORF15 gene (three families with XL and three families with the AR/XL mode of inheritance), mutation-specific microarray analysis of the ABCA4 gene (five families with the AR mode of inheritance and two families with the AR/XL mode of inheritance), targeted next-generation sequencing (NGS) of inherited retinal disease–associated (IRD) genes (seven families with the AD mode of inheritance and five families with the AR mode of inheritance), and whole exome sequencing, performed in select families who had been mutation-negative in the analysis with the targeted NGS panel (one family with the AD mode of inheritance, one family with the AR mode of inheritance, and two families with the AR/XL mode of inheritance). RESULTS: Based on this combined strategy, we managed to identify potentially causative variants in seven out of 18 families with CRD. Five of these variants are novel: c.3142_3143dupAA, p.(Glu1049Argfs*41) in the RPGR-ORF15 gene, two variants: c.1612delT, p.(Trp538Glyfs*15) and c.2389dupG, p.(Ile798Hisfs*20) in the PROM1 gene in one family, c.592A>C, p.(Ser198Arg) in the PRPH2 gene and the variant c.1691A>G, p.(Asp564Gly) in the ATF6 gene that we have already reported to be pathogenic. NGS on the IRD panel allowed the molecular basis of CRD to be identified in four out of 14 families with a total detection rate of 38%. WES allowed identification of the molecular genetic basis of CRD in one family. CONCLUSIONS: This is the first report on the spectrum of disease genes and pathogenic variants causing CRD in the Polish population. The study presents five novel variants identified in four genes and therefore, broadens the spectrum of probable pathogenic variants associated with CRD.
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spelling pubmed-59376722018-05-16 Novel variants identified with next-generation sequencing in Polish patients with cone-rod dystrophy Wawrocka, Anna Skorczyk-Werner, Anna Wicher, Katarzyna Niedziela, Zuzanna Ploski, Rafal Rydzanicz, Malgorzata Sykulski, Maciej Kociecki, Jaroslaw Weisschuh, Nicole Kohl, Susanne Biskup, Saskia Wissinger, Bernd Krawczynski, Maciej R. Mol Vis Research Article PURPOSE: The aim of this study was to identify the molecular genetic basis of cone-rod dystrophy in 18 unrelated families of Polish origin. Cone-rod dystrophy is one of the inherited retinal dystrophies, which constitute a highly heterogeneous group of disorders characterized by progressive dysfunction of photoreceptors and retinal pigment epithelium (RPE) cells. METHODS: The study group was composed of four groups of patients representing different Mendelian inheritance of the disease: autosomal dominant (AD), autosomal recessive (AR), X-linked recessive (XL), and autosomal recessive or X-linked recessive (AR/XL). The combined molecular strategy included Sanger sequencing of the RPGR-ORF15 gene (three families with XL and three families with the AR/XL mode of inheritance), mutation-specific microarray analysis of the ABCA4 gene (five families with the AR mode of inheritance and two families with the AR/XL mode of inheritance), targeted next-generation sequencing (NGS) of inherited retinal disease–associated (IRD) genes (seven families with the AD mode of inheritance and five families with the AR mode of inheritance), and whole exome sequencing, performed in select families who had been mutation-negative in the analysis with the targeted NGS panel (one family with the AD mode of inheritance, one family with the AR mode of inheritance, and two families with the AR/XL mode of inheritance). RESULTS: Based on this combined strategy, we managed to identify potentially causative variants in seven out of 18 families with CRD. Five of these variants are novel: c.3142_3143dupAA, p.(Glu1049Argfs*41) in the RPGR-ORF15 gene, two variants: c.1612delT, p.(Trp538Glyfs*15) and c.2389dupG, p.(Ile798Hisfs*20) in the PROM1 gene in one family, c.592A>C, p.(Ser198Arg) in the PRPH2 gene and the variant c.1691A>G, p.(Asp564Gly) in the ATF6 gene that we have already reported to be pathogenic. NGS on the IRD panel allowed the molecular basis of CRD to be identified in four out of 14 families with a total detection rate of 38%. WES allowed identification of the molecular genetic basis of CRD in one family. CONCLUSIONS: This is the first report on the spectrum of disease genes and pathogenic variants causing CRD in the Polish population. The study presents five novel variants identified in four genes and therefore, broadens the spectrum of probable pathogenic variants associated with CRD. Molecular Vision 2018-04-26 /pmc/articles/PMC5937672/ /pubmed/29769798 Text en Copyright © 2018 Molecular Vision. http://creativecommons.org/licenses/by-nc-nd/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited, used for non-commercial purposes, and is not altered or transformed.
spellingShingle Research Article
Wawrocka, Anna
Skorczyk-Werner, Anna
Wicher, Katarzyna
Niedziela, Zuzanna
Ploski, Rafal
Rydzanicz, Malgorzata
Sykulski, Maciej
Kociecki, Jaroslaw
Weisschuh, Nicole
Kohl, Susanne
Biskup, Saskia
Wissinger, Bernd
Krawczynski, Maciej R.
Novel variants identified with next-generation sequencing in Polish patients with cone-rod dystrophy
title Novel variants identified with next-generation sequencing in Polish patients with cone-rod dystrophy
title_full Novel variants identified with next-generation sequencing in Polish patients with cone-rod dystrophy
title_fullStr Novel variants identified with next-generation sequencing in Polish patients with cone-rod dystrophy
title_full_unstemmed Novel variants identified with next-generation sequencing in Polish patients with cone-rod dystrophy
title_short Novel variants identified with next-generation sequencing in Polish patients with cone-rod dystrophy
title_sort novel variants identified with next-generation sequencing in polish patients with cone-rod dystrophy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5937672/
https://www.ncbi.nlm.nih.gov/pubmed/29769798
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