Hunter, Robert P, MaryAnn Radlinsky, David E Koch, Matthew Corse, Marie A. Pellerin, and Jennifer Halstead. (2024) 2005. “Plasma pharmacokinetics and synovial fluid concentrations after oral administration of single and multiple doses of celecoxib in Greyhounds”. American Journal of Veterinary Research 66 (8): 1441-45. https://doi.org/10.2460/ajvr.2005.66.1441.
Publications
2005
Heeb, H. L., R. Chun, D. E. Koch, L. MOORE, M. RADLINSKY, M. CORSE, M. A. PELLERIN, L. GARRETT, and R. P. HUNTER. (2024) 2005. “Multiple dose pharmacokinetics and acute safety of piroxicam and cimetidine in the cat”. Journal of Veterinary Pharmacology and Therapeutics 28 (5): 447-52. https://doi.org/10.1111/j.1365-2885.2005.00682.x.
Xu, Fangxiang, David E. Koch, In Chul Kong, Robert P. Hunter, and Alok Bhandari. (2024) 2005. “Peroxidase-mediated oxidative coupling of 1-naphthol: Characterization of polymerization products”. Water Research 39 (11): 2358-68. https://doi.org/10.1016/j.watres.2005.04.010.
Rush, Elizabeth Marie, Robert P. Hunter, Mark Papich, Bonnie L. Raphael, Paul P. Calle, Tracy L. Clippinger, and Robert A. Cook. (2024) 2005. “Pharmacokinetics and Safety of Acyclovir in Tragopans (Tragopan species)”. Journal of Avian Medicine and Surgery 19 (4): 271-76. https://doi.org/10.1647/2004-026.1.
2004
Hunter, R P, R Isaza, D E Koch, C C Dodd, and M A Goatley. (2004) 2004. “The Pharmacokinetics of Topical Doramectin in Llamas (Lama Glama) and Alpacas (Lama Pacos)”. Journal of Veterinary Pharmacology and Therapeutics 27 (3): 187-9.
Hunter, Robert P, Ramiro Isaza, James W Carpenter, and David E Koch. (2004) 2004. “Clinical Effects and Plasma Concentrations of Fentanyl After Transmucosal Administration in Three Species of Great Ape”. Journal of Zoo and Wildlife Medicine : Official Publication of the American Association of Zoo Veterinarians 35 (2): 162-6.
Fentanyl is approved for transmucosal use in the United States as a preanesthetic agent in human pediatric patients and in adults for breakthrough cancer pain. Using this formulation in three species of great ape, including eight orangutans (Pongo pygmaeus), nine chimpanzees (Pan troglodytes), and two gorillas (Gorilla gorilla), fentanyl was offered transmucosally at an intended dose of 10-15 microg/kg based on estimated body weight. The animals were trained to accept and suck slowly on a piece of placebo candy, given as a treat, after an overnight fast. On the day of the study, the animals were given the lollipop formulation of fentanyl. The resulting plasma concentrations of fentanyl supported transmucosal absorption, similar to that reported in humans. This study provides an alternative sedative regimen and yielded half-life data of transmucosal fentanyl in great apes. Although transmucosal fentanyl was a useful adjunct for sedating orangutans and gorillas, its acceptance by chimpanzees before chemical immobilization was suboptimal and unpredictable.
Mutlow, Adrian, Ramiro Isaza, James W Carpenter, David E Koch, and Robert P Hunter. (2004) 2004. “Pharmacokinetics of Carfentanil and Naltrexone in Domestic Goats (Capra Hircus)”. Journal of Zoo and Wildlife Medicine : Official Publication of the American Association of Zoo Veterinarians 35 (4): 489-96.
Using a crossover study design, the pharmacokinetics of carfentanil and naltrexone after i.v., i.m., and s.c. administration were determined in eight domestic goats (Capra hircus). Serial blood samples were taken up to 120 hr after carfentanil administration, and the plasma drug concentrations were determined using liquid chromatography and mass spectroscopy. All goats were immobilized with 40 microg/kg carfentanil i.m., although the resulting neurologic effects varied considerably. Plasma profiles showed rapid carfentanil absorption and a simple biphasic decline for 12-48 hr. Naltrexone given at 100 mg naltrexone/mg carfentanil 30 min after carfentanil administration produced rapid reversal of immobilization after all routes of administration. Variable fluctuations in the naltrexone plasma concentrations during the first 2.5-3.5 hr were observed, followed by a more consistent biphasic decline. The time to standing was significantly shorter after i.v. compared with s.c. naltrexone, although the time difference (1 min) had little clinical relevance. No statistically significant differences between the naltrexone pharmacokinetic parameters measured for the three routes of naltrexone administration were identified, although the recoveries after i.m. administration were, subjectively, the smoothest. The carfentanil half-life did not differ significantly in the goats given naltrexone by different routes. Although it is currently recommended that the naltrexone dose be divided into s.c. and i.v. portions, this practice does not appear to offer any benefit.
Isaza, Ramiro, and Robert Hunter. (2024) 2004. “Drug Delivery to Captive Asian Elephants - Treating Goliath”. Current Drug Delivery 1 (3): 291-98. https://doi.org/10.2174/1567201043334641.
Hunter, R.P. 2004. “Assessment of multiple cardiocentesis in ball pythons (Python regius)”. Contemporary Topics in Laboratory Animal Science.
Koch, D.E., R. Isaza, J.W. Carpenter, and R.P. Hunter. (2024) 2004. “Simultaneous extraction and quantitation of fentanyl and norfentanyl from primate plasma with LC/MS detection”. Journal of Pharmaceutical and Biomedical Analysis 34 (3): 577-84. https://doi.org/10.1016/s0731-7085(03)00652-6.