Exposure to benzylpenicillin after different dosage regimens in growing pigs

Marie Sjölund; Carl Ekstrand; Per Wallgren; Ulf Bondesson; Märit Pringle; Björn Bengtsson

doi:10.1186/s13028-020-00552-0

Exposure to benzylpenicillin after different dosage regimens in growing pigs

Acta Vet Scand. 2020 Sep 17;62(1):55. doi: 10.1186/s13028-020-00552-0.

Authors

Marie Sjölund¹, Carl Ekstrand², Per Wallgren¹, Ulf Bondesson³, Märit Pringle¹, Björn Bengtsson¹

Affiliations

¹ Department of Animal Health and Antimicrobial Strategies, National Veterinary Institute, SVA, 751 89, Uppsala, Sweden.
² Department of Biomedical Sciences and Veterinary Public Health, Faculty of Veterinary Medicine and Animal Husbandry, Swedish University of Agricultural Sciences, Box 7028, 750 07, Uppsala, Sweden. carl.ekstrand@slu.se.
³ Department of Chemistry, Environment and Feed Hygiene, National Veterinary Institute, SVA, 751 89, Uppsala, Sweden.

Abstract

Background: Penicillin is important for treatment of pigs, but data on its absorption and disposition in pigs are sparse. This is reflected by the variation in recommended dosages in the literature. Inadequate dosage may lead to treatment failure and selection of resistant bacteria. To optimize treatment regimens, plasma exposure to benzylpenicillin for two sustained release formulations of procaine benzylpenicillin for intramuscular administration was studied in growing pigs by means of tandem mass spectrometry (UPLC-MS/MS). One formulation was an aqueous suspension, Ethacilin® vet (ETH), and the other an oily suspension, Ultrapen vet (UPA). Benzylpenicillin exposure after intravenous administration of potassium benzylpenicillin was also explored. Exposure profiles were first studied after single administrations of the approved dosages in healthy pigs and then after repeated administration of different dosages in pigs inoculated intranasally with an Actinobacillus pleuropneumoniae serotype 2 strain.

Results: After intravenous administration of benzylpenicillin (n = 6), maximum plasma concentration (C_max), 1860-9318 µg/L, was observed after 15 min. At four h, plasma concentrations decreased to 15-76 µg/L. After intramuscular administration of ETH (n = 6) C_max, 1000-4270 µg/L, was observed within one h (t_max) in 5 pigs but at four h in one pig. C_max for UPA (n = 6), 910-3220 µg/L, was observed within one h in three pigs, but at four or 24 h in three pigs. For both ETH and UPA, the terminal phase was characterized by slow decline compared with intravenous administration. Repeated administration of different dosages of ETH and UPA in pigs inoculated with A. pleuropneumoniae (n = 54) showed that the approved dose for UPA (30 mg/kg, qd) but not for ETH (20 mg/kg, qd) gave adequate plasma exposure for bacteria with a penicillin MIC of 500 µg/L. However, more frequent dosing of ETH (bid) or increased dosage gave an adequate exposure.

Conclusions: The approved dosage of ETH provided insufficient plasma exposure for adequate therapy of infections caused by A. pleuropneumoniae or other bacteria with a penicillin MIC of 500 µg/L. More frequent ETH dosing (bid) or an increased dosage would improve exposure. The approved dosage of UPA however provided adequate exposure.

Keywords: Actinobacillus pleuropneumoniae; Benzylpenicillin; Dosage regimen; Exposure profile; Pig; Plasma concentration.

MeSH terms

Actinobacillus Infections / drug therapy
Actinobacillus Infections / veterinary
Actinobacillus pleuropneumoniae / drug effects
Actinobacillus pleuropneumoniae / physiology
Animals
Anti-Bacterial Agents / pharmacokinetics*
Dose-Response Relationship, Drug
Female
Injections, Intramuscular / veterinary
Male
Penicillin G / pharmacokinetics*
Sus scrofa / metabolism*

Substances

Anti-Bacterial Agents
Penicillin G

Grants and funding

942-2015-768/Svenska Forskningsrådet Formas