<i>FYCO1</i> Frameshift Deletion in Wirehaired Pointing Griffon Dogs with Juvenile Cataract
Different breed-specific inherited cataracts have been described in dogs. In this study, we investigated an inbred family of Wirehaired Pointing Griffon dogs in which three offspring were affected by juvenile cataract. The pedigree suggested monogenic autosomal recessive inheritance of the trait. Wh...
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MDPI AG
2022-02-01
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author | Gabriela Rudd Garces Matthias Christen Robert Loechel Vidhya Jagannathan Tosso Leeb |
author_facet | Gabriela Rudd Garces Matthias Christen Robert Loechel Vidhya Jagannathan Tosso Leeb |
author_sort | Gabriela Rudd Garces |
collection | DOAJ |
description | Different breed-specific inherited cataracts have been described in dogs. In this study, we investigated an inbred family of Wirehaired Pointing Griffon dogs in which three offspring were affected by juvenile cataract. The pedigree suggested monogenic autosomal recessive inheritance of the trait. Whole-genome sequencing of an affected dog revealed 12 protein-changing variants that were not present in 566 control genomes, of which two were located in functional candidate genes, <i>FYCO1</i> and <i>CRYGB</i>. Targeted genotyping of both variants in the investigated family excluded <i>CRYGB</i> and revealed perfect co-segregation of the <i>FYCO1</i> variant with the juvenile cataract phenotype. This variant, <i>FYCO1</i>:c.2024delG, represents a 1 bp frameshift deletion predicted to truncate ~50% of the open reading frame p.(Ser675Thrfs*5). <i>FYCO1</i> encodes the FYVE and coiled-coil domain autophagy adaptor 1, a known regulator of lens autophagy, which is required for the normal homeostasis in the eye. In humans, at least 37 pathogenic variants in <i>FYCO1</i> have been shown to cause autosomal recessive cataract. <i>Fcyo1<sup>−/−</sup></i> knockout mice also develop cataracts. Together with the current knowledge on <i>FYCO1</i> variants and their functional impact in humans and mice, our data strongly suggest <i>FYCO1</i>:c.2024delG as a candidate causative variant for the observed juvenile cataract in Wirehaired Pointing Griffon dogs. To the best of our knowledge, this study represents the first report of a <i>FYCO1</i>-related cataract in domestic animals. |
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spelling | doaj.art-041864b6ec224b29b8d6c3c6dce228982023-11-23T20:05:13ZengMDPI AGGenes2073-44252022-02-0113233410.3390/genes13020334<i>FYCO1</i> Frameshift Deletion in Wirehaired Pointing Griffon Dogs with Juvenile CataractGabriela Rudd Garces0Matthias Christen1Robert Loechel2Vidhya Jagannathan3Tosso Leeb4Institute of Genetics, Vetsuisse Faculty, University of Bern, 3001 Bern, SwitzerlandInstitute of Genetics, Vetsuisse Faculty, University of Bern, 3001 Bern, SwitzerlandVetGen, Ann Arbor, MI 48108, USAInstitute of Genetics, Vetsuisse Faculty, University of Bern, 3001 Bern, SwitzerlandInstitute of Genetics, Vetsuisse Faculty, University of Bern, 3001 Bern, SwitzerlandDifferent breed-specific inherited cataracts have been described in dogs. In this study, we investigated an inbred family of Wirehaired Pointing Griffon dogs in which three offspring were affected by juvenile cataract. The pedigree suggested monogenic autosomal recessive inheritance of the trait. Whole-genome sequencing of an affected dog revealed 12 protein-changing variants that were not present in 566 control genomes, of which two were located in functional candidate genes, <i>FYCO1</i> and <i>CRYGB</i>. Targeted genotyping of both variants in the investigated family excluded <i>CRYGB</i> and revealed perfect co-segregation of the <i>FYCO1</i> variant with the juvenile cataract phenotype. This variant, <i>FYCO1</i>:c.2024delG, represents a 1 bp frameshift deletion predicted to truncate ~50% of the open reading frame p.(Ser675Thrfs*5). <i>FYCO1</i> encodes the FYVE and coiled-coil domain autophagy adaptor 1, a known regulator of lens autophagy, which is required for the normal homeostasis in the eye. In humans, at least 37 pathogenic variants in <i>FYCO1</i> have been shown to cause autosomal recessive cataract. <i>Fcyo1<sup>−/−</sup></i> knockout mice also develop cataracts. Together with the current knowledge on <i>FYCO1</i> variants and their functional impact in humans and mice, our data strongly suggest <i>FYCO1</i>:c.2024delG as a candidate causative variant for the observed juvenile cataract in Wirehaired Pointing Griffon dogs. To the best of our knowledge, this study represents the first report of a <i>FYCO1</i>-related cataract in domestic animals.https://www.mdpi.com/2073-4425/13/2/334<i>Canis lupus familiaris</i>whole-genome sequenceophthalmologylensanimal modelprecision medicine |
spellingShingle | Gabriela Rudd Garces Matthias Christen Robert Loechel Vidhya Jagannathan Tosso Leeb <i>FYCO1</i> Frameshift Deletion in Wirehaired Pointing Griffon Dogs with Juvenile Cataract Genes <i>Canis lupus familiaris</i> whole-genome sequence ophthalmology lens animal model precision medicine |
title | <i>FYCO1</i> Frameshift Deletion in Wirehaired Pointing Griffon Dogs with Juvenile Cataract |
title_full | <i>FYCO1</i> Frameshift Deletion in Wirehaired Pointing Griffon Dogs with Juvenile Cataract |
title_fullStr | <i>FYCO1</i> Frameshift Deletion in Wirehaired Pointing Griffon Dogs with Juvenile Cataract |
title_full_unstemmed | <i>FYCO1</i> Frameshift Deletion in Wirehaired Pointing Griffon Dogs with Juvenile Cataract |
title_short | <i>FYCO1</i> Frameshift Deletion in Wirehaired Pointing Griffon Dogs with Juvenile Cataract |
title_sort | i fyco1 i frameshift deletion in wirehaired pointing griffon dogs with juvenile cataract |
topic | <i>Canis lupus familiaris</i> whole-genome sequence ophthalmology lens animal model precision medicine |
url | https://www.mdpi.com/2073-4425/13/2/334 |
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