Modeling of autosomal-dominant retinitis pigmentosa in <i>Caenorhabditis elegans</i> uncovers a nexus between global impaired functioning of certain splicing factors and cell type-specific apoptosis

Rubio-Peña, Karinna; Fontrodona, Laura; Aristizábal-Corrales, David; Torres, Silvia; Cornes, Eric; García‐Rodríguez, Francisco J.; Serrat, Xènia; González-Knowles, David; Foissac, Sylvain; Porta-de-la-Riva, Montserrat; Cerón, Julián

doi:10.1261/rna.053397.115

Cited by 8 publications

(9 citation statements)

References 64 publications

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“…Partial loss-of-function of prp-6 causes misregulation of several 100 genes, including the cadherin cdh-5 . 11 We found that overexpression of cdh-5 can partially suppress axonal defects in cdh-4 mutants, suggesting that cdh-5 can partially compensate for the loss of cdh-4 .…”

Section: Introductionmentioning

confidence: 60%

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Mutations in the Spliceosome Component prp-6 and Overexpression of cdh-5 Suppress Axon Guidance Defects of cdh-4 Mutants in Caenorhabditis elegans

2022

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During nervous system development, axons must navigate to specific target areas. In Caenorhabditis elegans, the cadherin CDH-4 is required for ventral nerve cord axonal navigation, and dorsal nerve cord fasciculation. How CDH-4 mediates axon navigation and fasciculation is currently unknown. To identify genes acting together with cdh-4, we isolated mutants suppressing the axon guidance defects of cdh-4 mutants. These suppressors showed partial suppression of axonal defects in the dorsal and ventral nerve cords seen in cdh-4 mutants. We identified one suppressor gene, prp-6, which encodes a component of the spliceosome. Complete loss-of-function alleles of prp-6 are lethal, suggesting that the mutation isolated in our suppressor screen is a partial loss-of-function allele. A previous study found that RNAi-induced suppression of prp-6 leads to changes in the expression of several 100 genes including the cadherin cdh-5. We found that overexpression of cdh-5 mimics the suppression seen in prp-6 mutants, suggesting that CDH-5 can partially compensate for the loss of CDH-4.

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Section: Introductionmentioning

confidence: 60%

“…This confirms that the suppression of axonal defects is caused by a mutation in prp-6 . Complete loss-of-function of prp-6 is lethal, 11 since splicing is an essential cellular process. Therefore, prp-6(hd170) is likely to be a partial loss-of-function allele.…”

Section: Resultsmentioning

confidence: 99%

Mutations in the Spliceosome Component prp-6 and Overexpression of cdh-5 Suppress Axon Guidance Defects of cdh-4 Mutants in Caenorhabditis elegans

2022

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“…We chose PRPF8 and SNRNP200 because these two proteins physically interact through the C-terminal region of PRPF8, where the s-adRP mutations are located (10). Moreover, RNAi of their orthologs in C. elegans, along with PRPF6, showed the most penetrant phenotypes (26). These three genes encode proteins of the U5 complex and, based on our previous RNAi experiments, would be more prone to harbor missense mutations with a strong phenotype than the other three splicing factors (PRP3, PRPF31 and PRPF4), which are part of the U4 complex.…”

Section: Discussionmentioning

confidence: 99%

“…Such extraordinary conservation would imply maintenance of the function and therefore the missense mutations could have similar consequences at the molecular level in humans and in nematodes. C. elegans has already been exploited as model for s-adRP (26) and would be further exploited in the future if functional replacement of C. elegans s-adRP genes at its endogenous locus can be achieved with their human counterparts. The challenge here would be to express a functional human splicing factor at endogenous levels without causing any phenotype in the nematode.…”

Section: Discussionmentioning

confidence: 99%

Splicing-related Retinitis Pigmentosa mutations mimicked in C. elegans allow the identification of disease modifiers and drug screens

Kukhtar

Rubio-Peña

Serrat

et al. 2019

Preprint

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CRISPR and the high conservation of the spliceosome components facilitate the mimicking of human pathological mutations in splicing factors of model organisms. The degenerative retinal disease Retinitis Pigmentosa (RP) is caused by mutations in distinct types of genes, including missense mutations in splicing factors that provoke RP in an autosomal dominant form (s-adRP). Using CRISPR in C. elegans, we generated mutant strains to mimic RP mutations reported in PRPF8 and SNRNP200. Whereas these inherited mutations are present in heterozygosis in patients, C. elegans allows the maintenance of these mutations in homozygosis, which is advantageous for genetic and drug screens. We found that snrp-200(cer23[V676L]) and prp-8(cer14 [H2302del]) display pleiotropic phenotypes, including a reduced fertility.However, snrp-200(cer24[S1080L]) and prp-8(cer22[R2303G]) are weak alleles suitable for RNAi screens to identify genetic interactions, which would uncover potential disease modifiers. We screened a collection of RNAi clones for splicing-related genes and identified three splicing factors, isy-1/ISY1, cyn-15/PPWD1 and mog-2/SNRPA1 whose partial inactivation may modify the course of the disease. Interestingly, these three genes were acting as modifiers of prp-8(cer22) but no snrp-200(cer24).Finally, the strong allele prp-8(cer14) was used in a screen with FDA-approved drugs to find molecules capable of alleviating the phenotype. Instead, we detected drugs, as Dequalinium Chloride, which exacerbated the phenotype and therefore are potentially harmful for s-adRP patients since they may accelerate the progression of the disease.

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“…These seven genes are PRPF3, PRPF4, PRPF6, PRPF8, PRPF31, SNRNP200 and RP9. All of them, except for RP9, encode highly conserved proteins between C. elegans and humans [114]. Photoreceptor cells are characterized by an intense transcriptional activity and metabolic rate [115] and, even though they are absent in C. elegans, the animal does present other cells that have similar increased metabolic rate and high transcriptional levels during the larval phase [116,117].…”

Section: Caenorhabditis Elegansmentioning

confidence: 99%

Application of CRISPR Tools for Variant Interpretation and Disease Modeling in Inherited Retinal Dystrophies

Fuster-García

García‐Bohórquez

Rodríguez-Muñoz

et al. 2020

Genes

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Inherited retinal dystrophies are an assorted group of rare diseases that collectively account for the major cause of visual impairment of genetic origin worldwide. Besides clinically, these vision loss disorders present a high genetic and allelic heterogeneity. To date, over 250 genes have been associated to retinal dystrophies with reported causative variants of every nature (nonsense, missense, frameshift, splice-site, large rearrangements, and so forth). Except for a fistful of mutations, most of them are private and affect one or few families, making it a challenge to ratify the newly identified candidate genes or the pathogenicity of dubious variants in disease-associated loci. A recurrent option involves altering the gene in in vitro or in vivo systems to contrast the resulting phenotype and molecular imprint. To validate specific mutations, the process must rely on simulating the precise genetic change, which, until recently, proved to be a difficult endeavor. The rise of the CRISPR/Cas9 technology and its adaptation for genetic engineering now offers a resourceful suite of tools to alleviate the process of functional studies. Here we review the implementation of these RNA-programmable Cas9 nucleases in culture-based and animal models to elucidate the role of novel genes and variants in retinal dystrophies.

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Modeling of autosomal-dominant retinitis pigmentosa in Caenorhabditis elegans uncovers a nexus between global impaired functioning of certain splicing factors and cell type-specific apoptosis

Cited by 8 publications

References 64 publications

Mutations in the Spliceosome Component prp-6 and Overexpression of cdh-5 Suppress Axon Guidance Defects of cdh-4 Mutants in Caenorhabditis elegans

Mutations in the Spliceosome Component prp-6 and Overexpression of cdh-5 Suppress Axon Guidance Defects of cdh-4 Mutants in Caenorhabditis elegans

Splicing-related Retinitis Pigmentosa mutations mimicked in C. elegans allow the identification of disease modifiers and drug screens

Application of CRISPR Tools for Variant Interpretation and Disease Modeling in Inherited Retinal Dystrophies

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