Peer-reviewed veterinary case report
Treating gum disease in older dogs with COR388 drug
By Arastu-Kapur, Shirin et al.·Published in Pharmacology research & perspectives·2020·Cortexyme, United States·View original on PubMed →
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Original publication title: Treatment of Porphyromonas gulae infection and downstream pathology in the aged dog by lysine-gingipain inhibitor COR388.
- Species:
- dog
Plain-English summary
A group of older dogs with gum disease caused by a bacterial infection called Porphyromonas gulae were treated with a new medication called COR388 for 90 days. This treatment aimed to reduce the bacteria in their mouths and improve their overall health. The results showed that COR388 successfully lowered the bacterial levels and helped with the symptoms of periodontal disease. The dogs showed continuous improvement throughout the treatment period, suggesting that this medication could be beneficial for managing similar infections in dogs.
People also search for: dog gum disease treatment · Porphyromonas gulae infection in dogs · COR388 for dog periodontal disease
Abstract
COR388, a small-molecule lysine-gingipain inhibitor, is currently being investigated in a Phase 2/3 clinical trial for Alzheimer's disease (AD) with exploratory endpoints in periodontal disease. Gingipains are produced by two species of bacteria, Porphyromonas gingivalis and Porphyromonas gulae, typically associated with periodontal disease and systemic infections in humans and dogs, respectively. P. gulae infection in dogs is associated with periodontal disease, which provides a physiologically relevant model to investigate the pharmacology of COR388. In the current study, aged dogs with a natural oral infection of P. gulae and periodontal disease were treated with COR388 by oral administration for up to 90 days to assess lysine-gingipain target engagement and reduction of bacterial load and downstream pathology. In a 28-day dose-response study, COR388 inhibited the lysine-gingipain target and reduced P. gulae load in saliva, buccal cells, and gingival crevicular fluid. The lowest effective dose was continued for 90 days and was efficacious in continuous reduction of bacterial load and downstream periodontal disease pathology. In a separate histology study, dog brain tissue showed evidence of P. gulae DNA and neuronal lysine-gingipain, demonstrating that P. gulae infection is systemic and spreads beyond its oral reservoir, similar to recent observations of P. gingivalis in humans. Together, the pharmacokinetics and pharmacodynamics of COR388 lysine-gingipain inhibition, along with reduction of bacterial load and periodontal disease in naturally occurring P. gulae infection in the dog, support the use of COR388 in targeting lysine-gingipain and eliminating P. gingivalis infection in humans.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/31999052/