Peer-reviewed veterinary case report
Gene mutation linked to brain disease in American Bulldogs
By Awano, Tomoyuki et al.Ā·Published in Molecular genetics and metabolismĀ·2006Ā·Department of Veterinary Pathobiology, United StatesĀ·View original on PubMed ā
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Original publication title: A mutation in the cathepsin D gene (CTSD) in American Bulldogs with neuronal ceroid lipofuscinosis.
- Species:
- dog
Plain-English summary
A group of American Bulldogs was found to have a genetic mutation linked to a serious brain disease called neuronal ceroid lipofuscinosis (NCL), which causes neurodegeneration. This condition was confirmed through tests that showed abnormal structures in their brain and eyes. The affected Bulldogs had a specific mutation in the cathepsin D gene, which is important for brain function. While the disease was severe, it was less intense than similar conditions seen in other animals and humans. Unfortunately, there is no cure for this genetic condition, and affected dogs may require supportive care as their symptoms progress.
People also search for: American Bulldog brain disease Ā· NCL in dogs Ā· cathepsin D mutation in Bulldogs
Abstract
We obtained DNA, brains, and eyes from American Bulldogs with neurodegeneration due to neuronal ceroid lipofuscinosis (NCL). The diagnosis of NCL was confirmed by detection of autofluorescent cytoplasmic inclusions within neurons throughout the brains, in retinal ganglion cells, and along outer limiting membranes of the retinas. Electron microscopy revealed that the inclusions had coarsely granular matrices surrounding well-delineated spherical structures and that the inclusions near the retinal outer limiting membranes were within photoreceptor cells, mostly cones. Affected American Bulldogs were homozygous for the A allele of a G to A transition in the cathepsin D gene (CTSD), which predicts the conversion of methionine-199 to an isoleucine. Only the G allele was detected in DNA samples from 131 randomly selected dogs representing 108 breeds other than American Bulldog; however, the A allele had a frequency of 0.28 among 123 genotyped American Bulldogs. Transmission analysis in a 99 dog pedigree of American Bulldogs indicated a probability of less than 10(-7) that alleles from any mutation unlinked to CTSD would be concordant with the pedigree and phenotypes of the dogs. Brain samples from affected dogs had 36% of the cathepsin D-specific enzymatic activity found in control dog brains; whereas, specific enzymatic activities of 15 other lysosomal enzymes were unchanged or increased. Compared to previously described NCLs in mice and sheep that completely lack cathepsin D activity, the clinical course of NCL in the American Bulldogs was less severe and more closely resembled that of many human NCLs.
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Search related cases āOriginal publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/16386934/