The intravenous pharmacokinetics of diminazene in healthy dogs

Diminazene remains one of South Africa's most commonly used antiprotozoal agents for the management of babesiosis in dogs . Although the drug has been on the market for over 40 years, its intravenous pharmacokinetics are poorly known. To better understand the pharmacokinetics of the drug Bereni...

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Main Authors: V. Naidoo, M.S.G. Mulders, G.E. Swan
Format: Article
Language:English
Published: AOSIS 2009-05-01
Series:Journal of the South African Veterinary Association
Subjects:
Dog
Online Access:https://jsava.co.za/index.php/jsava/article/view/210
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spelling doaj-7e4e28f4c8254f44bf958b54c86902602020-11-24T21:02:29ZengAOSISJournal of the South African Veterinary Association1019-91282224-94352009-05-0180421521910.4102/jsava.v80i4.210169The intravenous pharmacokinetics of diminazene in healthy dogsV. NaidooM.S.G. MuldersG.E. SwanDiminazene remains one of South Africa's most commonly used antiprotozoal agents for the management of babesiosis in dogs . Although the drug has been on the market for over 40 years, its intravenous pharmacokinetics are poorly known. To better understand the pharmacokinetics of the drug Berenil®, it was reconstituted in sterile water and administered intravenously to 6 adult German shepherd dogs. All 6 dogs demonstrated the previously described secondary peak in the plasma concentration versus time profile. The plasma pharmacokinetics for diminazene are described by both non-compartmental and compartmental models. From non-compartmental analysis, the area under curve to the last sample point (AUClast), clearance (CL) and volume of distribution (Vz) were 4.65±1.95 ng/mℓ/h, 0.77±0.18 ℓ/kg/h and 2.28±0.60 ℓ/kg, respectively. For compartmental modelling, the plasma concentrations were fitted to both a 2-compartmental open model and a recirculatory enterohepatic model. From the recirculation model, the rate of release and re-entry into the central compartment varied markedly with the rate of release from the gall bladder (Ttom) being estimated at 27 ± 20.90 h. Once released, drug re-entry into the central compartment was variable at 9.70±5.48 h. With normal biliary excretion time being about 2 h, this indicates that the redistribution cannot be occurring physiologically from the bile. Although it was not possible to identify the site from which sequestration and delayed release is occurring, it is believed that it is most likely from the liver. The study therefore showed that the secondary peak described for the pharmacokinetics of intramuscular administered diminazene in the dog is not related to biphasic absorption.https://jsava.co.za/index.php/jsava/article/view/210Berenil®DogEnterohepaticIntravenousPharmacokineticsPK40Eecirculation
collection DOAJ
language English
format Article
sources DOAJ
author V. Naidoo
M.S.G. Mulders
G.E. Swan
spellingShingle V. Naidoo
M.S.G. Mulders
G.E. Swan
The intravenous pharmacokinetics of diminazene in healthy dogs
Journal of the South African Veterinary Association
Berenil®
Dog
Enterohepatic
Intravenous
Pharmacokinetics
PK40
Eecirculation
author_facet V. Naidoo
M.S.G. Mulders
G.E. Swan
author_sort V. Naidoo
title The intravenous pharmacokinetics of diminazene in healthy dogs
title_short The intravenous pharmacokinetics of diminazene in healthy dogs
title_full The intravenous pharmacokinetics of diminazene in healthy dogs
title_fullStr The intravenous pharmacokinetics of diminazene in healthy dogs
title_full_unstemmed The intravenous pharmacokinetics of diminazene in healthy dogs
title_sort intravenous pharmacokinetics of diminazene in healthy dogs
publisher AOSIS
series Journal of the South African Veterinary Association
issn 1019-9128
2224-9435
publishDate 2009-05-01
description Diminazene remains one of South Africa's most commonly used antiprotozoal agents for the management of babesiosis in dogs . Although the drug has been on the market for over 40 years, its intravenous pharmacokinetics are poorly known. To better understand the pharmacokinetics of the drug Berenil®, it was reconstituted in sterile water and administered intravenously to 6 adult German shepherd dogs. All 6 dogs demonstrated the previously described secondary peak in the plasma concentration versus time profile. The plasma pharmacokinetics for diminazene are described by both non-compartmental and compartmental models. From non-compartmental analysis, the area under curve to the last sample point (AUClast), clearance (CL) and volume of distribution (Vz) were 4.65±1.95 ng/mℓ/h, 0.77±0.18 ℓ/kg/h and 2.28±0.60 ℓ/kg, respectively. For compartmental modelling, the plasma concentrations were fitted to both a 2-compartmental open model and a recirculatory enterohepatic model. From the recirculation model, the rate of release and re-entry into the central compartment varied markedly with the rate of release from the gall bladder (Ttom) being estimated at 27 ± 20.90 h. Once released, drug re-entry into the central compartment was variable at 9.70±5.48 h. With normal biliary excretion time being about 2 h, this indicates that the redistribution cannot be occurring physiologically from the bile. Although it was not possible to identify the site from which sequestration and delayed release is occurring, it is believed that it is most likely from the liver. The study therefore showed that the secondary peak described for the pharmacokinetics of intramuscular administered diminazene in the dog is not related to biphasic absorption.
topic Berenil®
Dog
Enterohepatic
Intravenous
Pharmacokinetics
PK40
Eecirculation
url https://jsava.co.za/index.php/jsava/article/view/210
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