Mechanistically distinct mouse models for CRX-associated retinopathy

Mechanistically distinct mouse models for CRX-associated retinopathy

Cone-rod homeobox (CRX) protein is a "paired-like" homeodomain transcription factor that is essential for regulating rod and cone photoreceptor transcription. Mutations in human CRX are associated with the dominant retinopathies Retinitis Pigmentosa (RP), Cone-Rod Dystrophy (CoRD) and Lebe...

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Veröffentlicht in:PLoS genetics 2014-02, Vol.10 (2), p.e1004111-e1004111
Hauptverfasser: Tran, Nicholas M, Zhang, Alan, Zhang, Xiaodong, Huecker, Julie B, Hennig, Anne K, Chen, Shiming
Format: Artikel
Sprache:eng
Schlagworte:
American Recovery & Reinvestment Act 2009-US
Animals
Biology
Care and treatment
Disease
Disease Models, Animal
Experiments
Frameshift Mutation
Gene expression
Gene mutations
Genetic aspects
Homeodomain Proteins - genetics
Homozygote
Humans
Leber Congenital Amaurosis - genetics
Leber Congenital Amaurosis - pathology
Medicine
Mice
Mutation
Otolaryngology
Phenotype
Photoreceptors
Physiological aspects
Proteins
Retina
Retinal Cone Photoreceptor Cells
Retinal Degeneration - genetics
Retinal diseases
Retinitis Pigmentosa - genetics
Retinitis Pigmentosa - pathology
Risk factors
Rodents
Studies
Trans-Activators - genetics
Transcription factors
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Zusammenfassung:Cone-rod homeobox (CRX) protein is a "paired-like" homeodomain transcription factor that is essential for regulating rod and cone photoreceptor transcription. Mutations in human CRX are associated with the dominant retinopathies Retinitis Pigmentosa (RP), Cone-Rod Dystrophy (CoRD) and Leber Congenital Amaurosis (LCA), with variable severity. Heterozygous Crx Knock-Out (KO) mice ("+/-") have normal vision as adults and fail to model the dominant human disease. To investigate how different mutant CRX proteins produce distinct disease pathologies, we generated two Crx Knock-IN (K-IN) mouse models: Crx(E168d2) ("E168d2") and Crx(R90W) ("R90W"). E168d2 mice carry a frameshift mutation in the CRX activation domain, Glu168del2, which is associated with severe dominant CoRD or LCA in humans. R90W mice carry a substitution mutation in the CRX homeodomain, Arg90Trp, which is associated with dominant mild late-onset CoRD and recessive LCA. As seen in human patients, heterozygous E168d2 ("E168d2/+") but not R90W ("R90W/+") mice show severely impaired retinal function, while mice homozygous for either mutation are blind and undergo rapid photoreceptor degeneration. E168d2/+ mice also display abnormal rod/cone morphology, greater impairment of CRX target gene expression than R90W/+ or +/- mice, and undergo progressive photoreceptor degeneration. Surprisingly, E168d2/+ mice express more mutant CRX protein than wild-type CRX. E168d2neo/+, a subline of E168d2 with reduced mutant allele expression, displays a much milder retinal phenotype, demonstrating the impact of Crx expression level on disease severity. Both CRX([E168d2]) and CRX([R90W]) proteins fail to activate transcription in vitro, but CRX([E168d2]) interferes more strongly with the function of wild type (WT) CRX, supporting an antimorphic mechanism. E168d2 and R90W are mechanistically distinct mouse models for CRX-associated disease that will allow the elucidation of molecular mechanisms and testing of novel therapeutic approaches for different forms of CRX-associated disease.
ISSN:1553-7404
1553-7390
1553-7404
DOI:10.1371/journal.pgen.1004111