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Peer-reviewed veterinary case report

Vision loss and eye damage in dogs with CLN5 brain disease

By Kick, Grace Robinson et al.·Published in Experimental eye research·2021·University of Missouri, United States·View original on PubMed

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Original publication title: Visual system pathology in a canine model of CLN5 neuronal ceroid lipofuscinosis.

Species:
dog
Canine GlaucomaBrain & nervesDogs

Plain-English summary

Five Golden Retriever littermates were found to have severe vision problems and neurological decline due to a hereditary condition called CLN5 neuronal ceroid lipofuscinosis. By 21-22 months old, they showed significant visual impairment and changes in their retinal function, although their retinas appeared normal under imaging. The disease caused a buildup of harmful substances in their retinal cells and brain, affecting their ability to process visual signals. Unfortunately, the dogs could not be observed into later stages of the disease due to worsening symptoms. This research suggests that treatments aimed at preserving vision could be effective if started early in the disease process.

People also search for: Golden Retriever vision problems · CLN5 disease in dogs · dog hereditary neurological decline

Abstract

CLN5 neuronal ceroid lipofuscinosis is a hereditary neurodegenerative disease characterized by progressive neurological decline, vision loss and seizures. Visual impairment in children with CLN5 disease is attributed to a progressive decline in retinal function accompanied by retinal degeneration as well as impaired central nervous system function associated with global brain atrophy. We studied visual system pathology in five Golden Retriever littermates homozygous for the CLN5 disease allele previously identified in the breed. The dogs exhibited signs of pronounced visual impairment by 21-22 months of age. Electroretinogram recordings showed a progressive decline in retinal function primarily affecting cone neural pathways. Altered visual evoked potential recordings indicated that disease progression affected visual signal processing in the brain. Aside from several small retinal detachment lesions, no gross retinal abnormalities were observed with in vivo ocular imaging and histologically the retinas did not exhibit apparent abnormalities by 23 months of age. However, there was extensive accumulation of autofluorescent membrane-bound lysosomal storage bodies in almost all retinal layers, as well as in the occipital cortex, by 20 months of age. In the retina, storage was particularly pronounced in retinal ganglion cells, the retinal pigment epithelium and in photoreceptor cells just interior to the outer limiting membrane. The visual system pathology of CLN5-affected Golden Retrievers is similar to that seen early in the human disease. It was not possible to follow the dogs to an advanced stage of disease progression due to the severity of behavioral and motor disease signs by 23 months of age. The findings reported here indicate that canine CLN5 disease will be a useful model of visual system disease in CLN5 neuronal ceroid lipofuscinosis. The baseline data obtained in this investigation will be useful in future therapeutic intervention studies. The findings indicate that there is a fairly broad time frame after disease onset within which treatments could be effective in preserving vision.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/34216614/