Abstract
Five lactating cows were given benzydamine hydrochloride by rapid intravenous (0.45 mg/kg) and by intramuscular (0.45 and 1.2 mg/kg) injection in a crossover design. The bioavailability, pharmacokinetic parameters and excretion in milk of benzydamine were evaluated. After intravenous administration, the disposition kinetics of benzydamine was best described using a two-compartment open model. Drug disposition and elimination were fast (t 1/2α: 11.13±3.76 min;t 1/2β: 71.98±24.75 min; MRT 70.69±11.97 min). Benzydamine was widely distributed in the body fluids and tissues (V d(area): 3.549±1.301 L/kg) and characterized by a high value for body clearance (33.00±5.54 ml/kg per min). After intramuscular administration the serum concentration-time curves fitted a one-compartment open model. Following a dose of 0.45 mg/kg, theC max value was 38.13±4.2 ng/ml at at max of 67.13±4.00 min; MAT and MRT were 207.33±22.64 min and 278.01±12.22 min, respectively. Benzydamine bioavailability was very high (92.07%±7.08%). An increased intramuscular dose (1.2 mg/kg) resulted in longer serum persistence (MRT 420.34±86.39 min) of the drug, which was also detectable in milk samples collected from both the first and second milking after treatment.
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Abbreviations
- HPLC:
-
high-pressure liquid chromatography
- IC50:
-
concentration to inhibit the activity of an organism by 50%
- IM:
-
intramuscular(ly)
- IV:
-
intravenous(ly)
- NSAID:
-
non-steroidal antiinflammatory drugs
- pK a :
-
negative logarithm of the ionization constant (K a) of a drug; other abbreviations are listed in footnotes to tables
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Anfossi, P., Malvisi, J., Catraro, N. et al. Pharmacokinetics of benzydamine in dairy cows following intravenous or intramuscular administration. Vet Res Commun 17, 313–323 (1993). https://doi.org/10.1007/BF01839222
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DOI: https://doi.org/10.1007/BF01839222