Subcellular localization of mutant P23H rhodopsin in an RFP fusion knock-in mouse model of retinitis pigmentosa

MA Robichaux, V Nguyen, F Chan… - Disease Models & …, 2022 - journals.biologists.com
MA Robichaux, V Nguyen, F Chan, L Kailasam, F He, JH Wilson, TG Wensel
Disease Models & Mechanisms, 2022journals.biologists.com
The P23H mutation in rhodopsin (Rho), the rod visual pigment, is the most common allele
associated with autosomal-dominant retinitis pigmentosa (adRP). The fate of misfolded
mutant Rho in rod photoreceptors has yet to be elucidated. We generated a new mouse
model, in which the P23H-Rho mutant allele is fused to the fluorescent protein Tag-RFP-T
(P23HhRhoRFP). In heterozygotes, outer segments formed, and wild-type (WT) rhodopsin
was properly localized, but mutant P23H-Rho protein was mislocalized in the inner …
Abstract
The P23H mutation in rhodopsin (Rho), the rod visual pigment, is the most common allele associated with autosomal-dominant retinitis pigmentosa (adRP). The fate of misfolded mutant Rho in rod photoreceptors has yet to be elucidated. We generated a new mouse model, in which the P23H-Rho mutant allele is fused to the fluorescent protein Tag-RFP-T (P23HhRhoRFP). In heterozygotes, outer segments formed, and wild-type (WT) rhodopsin was properly localized, but mutant P23H-Rho protein was mislocalized in the inner segments. Heterozygotes exhibited slowly progressing retinal degeneration. Mislocalized P23HhRhoRFP was contained in greatly expanded endoplasmic reticulum (ER) membranes. Quantification of mRNA for markers of ER stress and the unfolded protein response revealed little or no increases. mRNA levels for both the mutant human rhodopsin allele and the WT mouse rhodopsin were reduced, but protein levels revealed selective degradation of the mutant protein. These results suggest that the mutant rods undergo an adaptative process that prolongs survival despite unfolded protein accumulation in the ER. The P23H-Rho-RFP mouse may represent a useful tool for the future study of the pathology and treatment of P23H-Rho and adRP.
This article has an associated First Person interview with the first author of the paper.
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