Background Multidrug resistance in companion animals poses significant risks to animal and human health. Prolonged antimicrobial drug (AMD) treatment in animals is a potential source of selection pressure for antimicrobial resistance (AMR) including in the gastrointestinal microbiota. We performed a prospective study of dogs treated for septic peritonitis, pyometra, or bacterial pneumonia and collected repeated fecal samples over 60 days. Bacterial cultures and direct molecular analyses of fecal samples were performed including targeted resistance gene profiling. Results Resistant Escherichia coli increased after 1 week of treatment (D1:21.4% vs. D7:67.9% P < 0.001) and returned to baseline proportions by D60 (D7:67.9% vs D60:42.9%, P = 0.04). Dogs with septic peritonitis were hospitalized significantly longer than those with pneumonia or pyometra. Based on genetic analysis, Simpson’s diversity index significantly decreased after 1 week of treatment (D1 to D7, P = 0.008), followed by a gradual increase to day 60 (D1 and D60, P = 0.4). Detection of CTX-M was associated with phenotypic resistance to third-generation cephalosporins in E. coli (OR 12.1, 3.3–68.0, P < 0.001). Lincosamide and macrolide-resistance genes were more frequently recovered on days 14 and 28 compared to day 1 (P = 0.002 and P = 0.004 respectively). Conclusion AMR was associated with prescribed drugs but also developed against AMDs not administered during the study. Companion animals may be reservoirs of zoonotic multidrug resistant pathogens, suggesting that veterinary AMD stewardship and surveillance efforts should be prioritized. Graphical abstract
African giant pouched rats are of interest for their unique sense of smell and can be trained for a variety of applications including detection of explosives and infectious diseases. A colony housed at a university animal care facility developed abscesses associated with the jaw and eye in multiple animals. The predominant bacterial species in each case was a catalase-positive Actinomyces-like Gram-positive bacillus. The isolates from different sites and animals matched each other genetically but had sequences and biochemical profiles inconsistent with previously described species of this group. Based on whole genome sequence, biochemical characterization, and fatty acid profile, a novel species of the genus Actinomyces is proposed, namely Actinomyces cricetomys (type strain 186855T). The type strain is deposited at ATCC (TSD-310) and BCCM/LMG (LMG 32803).
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