Identification of Arhgef12 and Prkci as genetic modifiers of retinal dysplasia in the Crb1(rd8) mouse model

Mutations in the apicobasal polarity gene CRB1 lead to diverse retinal diseases, such as Leber congenital amaurosis, cone-rod dystrophy, retinitis pigmentosa (with and without Coats-like vasculopathy), foveal retinoschisis, macular dystrophy, and pigmented paravenous chorioretinal atrophy. Limited c...

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Autores principales: Weatherly, Sonia M., Collin, Gayle B., Charette, Jeremy R., Stone, Lisa, Damkham, Nattaya, Hyde, Lillian F., Peterson, James G., Hicks, Wanda, Carter, Gregory W., Naggert, Jürgen K., Krebs, Mark P., Nishina, Patsy M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9212170/
https://www.ncbi.nlm.nih.gov/pubmed/35675330
http://dx.doi.org/10.1371/journal.pgen.1009798
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author Weatherly, Sonia M.
Collin, Gayle B.
Charette, Jeremy R.
Stone, Lisa
Damkham, Nattaya
Hyde, Lillian F.
Peterson, James G.
Hicks, Wanda
Carter, Gregory W.
Naggert, Jürgen K.
Krebs, Mark P.
Nishina, Patsy M.
author_facet Weatherly, Sonia M.
Collin, Gayle B.
Charette, Jeremy R.
Stone, Lisa
Damkham, Nattaya
Hyde, Lillian F.
Peterson, James G.
Hicks, Wanda
Carter, Gregory W.
Naggert, Jürgen K.
Krebs, Mark P.
Nishina, Patsy M.
author_sort Weatherly, Sonia M.
collection PubMed
description Mutations in the apicobasal polarity gene CRB1 lead to diverse retinal diseases, such as Leber congenital amaurosis, cone-rod dystrophy, retinitis pigmentosa (with and without Coats-like vasculopathy), foveal retinoschisis, macular dystrophy, and pigmented paravenous chorioretinal atrophy. Limited correlation between disease phenotypes and CRB1 alleles, and evidence that patients sharing the same alleles often present with different disease features, suggest that genetic modifiers contribute to clinical variation. Similarly, the retinal phenotype of mice bearing the Crb1 retinal degeneration 8 (rd8) allele varies with genetic background. Here, we initiated a sensitized chemical mutagenesis screen in B6.Cg-Crb1(rd8)/Pjn, a strain with a mild clinical presentation, to identify genetic modifiers that cause a more severe disease phenotype. Two models from this screen, Tvrm266 and Tvrm323, exhibited increased retinal dysplasia. Genetic mapping with high-throughput exome and candidate-gene sequencing identified causative mutations in Arhgef12 and Prkci, respectively. Epistasis analysis of both strains indicated that the increased dysplastic phenotype required homozygosity of the Crb1(rd8) allele. Retinal dysplastic lesions in Tvrm266 mice were smaller and caused less photoreceptor degeneration than those in Tvrm323 mice, which developed an early, large diffuse lesion phenotype. At one month of age, Müller glia and microglia mislocalization at dysplastic lesions in both modifier strains was similar to that in B6.Cg-Crb1(rd8)/Pjn mice but photoreceptor cell mislocalization was more extensive. External limiting membrane disruption was comparable in Tvrm266 and B6.Cg-Crb1(rd8)/Pjn mice but milder in Tvrm323 mice. Immunohistological analysis of mice at postnatal day 0 indicated a normal distribution of mitotic cells in Tvrm266 and Tvrm323 mice, suggesting normal early development. Aberrant electroretinography responses were observed in both models but functional decline was significant only in Tvrm323 mice. These results identify Arhgef12 and Prkci as modifier genes that differentially shape Crb1-associated retinal disease, which may be relevant to understanding clinical variability and underlying disease mechanisms in humans.
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spelling pubmed-92121702022-06-22 Identification of Arhgef12 and Prkci as genetic modifiers of retinal dysplasia in the Crb1(rd8) mouse model Weatherly, Sonia M. Collin, Gayle B. Charette, Jeremy R. Stone, Lisa Damkham, Nattaya Hyde, Lillian F. Peterson, James G. Hicks, Wanda Carter, Gregory W. Naggert, Jürgen K. Krebs, Mark P. Nishina, Patsy M. PLoS Genet Research Article Mutations in the apicobasal polarity gene CRB1 lead to diverse retinal diseases, such as Leber congenital amaurosis, cone-rod dystrophy, retinitis pigmentosa (with and without Coats-like vasculopathy), foveal retinoschisis, macular dystrophy, and pigmented paravenous chorioretinal atrophy. Limited correlation between disease phenotypes and CRB1 alleles, and evidence that patients sharing the same alleles often present with different disease features, suggest that genetic modifiers contribute to clinical variation. Similarly, the retinal phenotype of mice bearing the Crb1 retinal degeneration 8 (rd8) allele varies with genetic background. Here, we initiated a sensitized chemical mutagenesis screen in B6.Cg-Crb1(rd8)/Pjn, a strain with a mild clinical presentation, to identify genetic modifiers that cause a more severe disease phenotype. Two models from this screen, Tvrm266 and Tvrm323, exhibited increased retinal dysplasia. Genetic mapping with high-throughput exome and candidate-gene sequencing identified causative mutations in Arhgef12 and Prkci, respectively. Epistasis analysis of both strains indicated that the increased dysplastic phenotype required homozygosity of the Crb1(rd8) allele. Retinal dysplastic lesions in Tvrm266 mice were smaller and caused less photoreceptor degeneration than those in Tvrm323 mice, which developed an early, large diffuse lesion phenotype. At one month of age, Müller glia and microglia mislocalization at dysplastic lesions in both modifier strains was similar to that in B6.Cg-Crb1(rd8)/Pjn mice but photoreceptor cell mislocalization was more extensive. External limiting membrane disruption was comparable in Tvrm266 and B6.Cg-Crb1(rd8)/Pjn mice but milder in Tvrm323 mice. Immunohistological analysis of mice at postnatal day 0 indicated a normal distribution of mitotic cells in Tvrm266 and Tvrm323 mice, suggesting normal early development. Aberrant electroretinography responses were observed in both models but functional decline was significant only in Tvrm323 mice. These results identify Arhgef12 and Prkci as modifier genes that differentially shape Crb1-associated retinal disease, which may be relevant to understanding clinical variability and underlying disease mechanisms in humans. Public Library of Science 2022-06-08 /pmc/articles/PMC9212170/ /pubmed/35675330 http://dx.doi.org/10.1371/journal.pgen.1009798 Text en © 2022 Weatherly et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Weatherly, Sonia M.
Collin, Gayle B.
Charette, Jeremy R.
Stone, Lisa
Damkham, Nattaya
Hyde, Lillian F.
Peterson, James G.
Hicks, Wanda
Carter, Gregory W.
Naggert, Jürgen K.
Krebs, Mark P.
Nishina, Patsy M.
Identification of Arhgef12 and Prkci as genetic modifiers of retinal dysplasia in the Crb1(rd8) mouse model
title Identification of Arhgef12 and Prkci as genetic modifiers of retinal dysplasia in the Crb1(rd8) mouse model
title_full Identification of Arhgef12 and Prkci as genetic modifiers of retinal dysplasia in the Crb1(rd8) mouse model
title_fullStr Identification of Arhgef12 and Prkci as genetic modifiers of retinal dysplasia in the Crb1(rd8) mouse model
title_full_unstemmed Identification of Arhgef12 and Prkci as genetic modifiers of retinal dysplasia in the Crb1(rd8) mouse model
title_short Identification of Arhgef12 and Prkci as genetic modifiers of retinal dysplasia in the Crb1(rd8) mouse model
title_sort identification of arhgef12 and prkci as genetic modifiers of retinal dysplasia in the crb1(rd8) mouse model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9212170/
https://www.ncbi.nlm.nih.gov/pubmed/35675330
http://dx.doi.org/10.1371/journal.pgen.1009798
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