The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study

The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study

The safety of a single oral dose of carprofen (11.5 mg/kg), flunixin (1 mg/kg) and phenylbutazone (1.7 mg/kg) was evaluated in the Cape Vulture (Gyps coprotheres) by means of a four-way parallel study, using two birds per treatment. Clinical observations, clinical pathology and necropsy examinati...

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Main Author: Fourie, Tamsyn Ann
Other Authors: Naidoo, Vinny
Language:en
Published: University of Pretoria 2015
Subjects:
UCTD
Online Access:http://hdl.handle.net/2263/46035
Fourie, TA 2014, The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study, MMedVet Dissertation, University of Pretoria, Pretoria, viewed yymmdd <http://hdl.handle.net/2263/46035>
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spelling ndltd-netd.ac.za-oai-union.ndltd.org-up-oai-repository.up.ac.za-2263-460352020-06-02T03:18:21Z The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study Fourie, Tamsyn Ann Naidoo, Vinny UCTD The safety of a single oral dose of carprofen (11.5 mg/kg), flunixin (1 mg/kg) and phenylbutazone (1.7 mg/kg) was evaluated in the Cape Vulture (Gyps coprotheres) by means of a four-way parallel study, using two birds per treatment. Clinical observations, clinical pathology and necropsy examinations were determining factors. Clinical signs of lethargy and depression were noted in one of the carprofen (CRP), two of the flunixin (FXN) and one of the phenylbutazone (PBZ) treated birds. Serum alanine transferase (ALT), albumin, sodium, calcium, potassium and uric acid (UA) concentrations were monitored up to 48 hours post dosing. Mild reversible inhibition of UA excretion was evident in all three groups, although UA remained within population reference intervals. All treatment groups had a drug concentration responsive ALT increase. No pathological lesions where noted on histopathology. Oral absorption of CRP, FXN and PBZ was characterised by a maximum plasma concentration of 1051.8 ± 620.7 ng/ml, 335.9 ± 36.3 ng/ml and 11150 ± 2474.9 ng/ml obtained in 4 ± 4.3, 0.45 ± 0.02 and 5.3 ± 5.2 hours respectively and a half-life of elimination of 13.3 ±5, 1.8±1 and 18.7 ±11.4 hours respectively. The volume of distribution was 13.62 ± 9.91 L/kg (CRP); 3.29± 0.75 L/kg (FXN) and 0.13 ± 0.03 L/kg (PBZ). Area under the curve until the last time point was 21.72± 20.10; 0.78± 0.28 and 263.35 ±68.69 μg/mL*h for CRP, FXN and PBZ respectively. Glucuronidation was identified in FXN and CRP treated birds. The long half-life of PBZ and CRP creates concern that accumulative toxicity may occur. Both FXN and PBZ are potentially hepatotoxic indicating that clinical use or the presence thereof in the food-chain should be avoided. CRP may be of clinical benefit in the vulture, but only as a single treatment. This drug should also be safe in the case of possible contamination of the food chain, as it is unlikely that vultures will be exposed to the drug often enough for it to be cumulative Dissertation (MMedVet)--University of Pretoria, 2014. tm2015 Paraclinical Sciences MMedVet Unrestricted 2015-07-02T11:06:35Z 2015-07-02T11:06:35Z 2015/04/22 2014 Dissertation http://hdl.handle.net/2263/46035 Fourie, TA 2014, The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study, MMedVet Dissertation, University of Pretoria, Pretoria, viewed yymmdd <http://hdl.handle.net/2263/46035> A2015 4180933 en © 2015 University of Pretoria. All rights reserved. The copyright in this work vests in the University of Pretoria. No part of this work may be reproduced or transmitted in any form or by any means, without the prior written permission of the University of Pretoria. University of Pretoria
collection NDLTD
language en
sources NDLTD
topic UCTD
spellingShingle UCTD
Fourie, Tamsyn Ann
The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study
description The safety of a single oral dose of carprofen (11.5 mg/kg), flunixin (1 mg/kg) and phenylbutazone (1.7 mg/kg) was evaluated in the Cape Vulture (Gyps coprotheres) by means of a four-way parallel study, using two birds per treatment. Clinical observations, clinical pathology and necropsy examinations were determining factors. Clinical signs of lethargy and depression were noted in one of the carprofen (CRP), two of the flunixin (FXN) and one of the phenylbutazone (PBZ) treated birds. Serum alanine transferase (ALT), albumin, sodium, calcium, potassium and uric acid (UA) concentrations were monitored up to 48 hours post dosing. Mild reversible inhibition of UA excretion was evident in all three groups, although UA remained within population reference intervals. All treatment groups had a drug concentration responsive ALT increase. No pathological lesions where noted on histopathology. Oral absorption of CRP, FXN and PBZ was characterised by a maximum plasma concentration of 1051.8 ± 620.7 ng/ml, 335.9 ± 36.3 ng/ml and 11150 ± 2474.9 ng/ml obtained in 4 ± 4.3, 0.45 ± 0.02 and 5.3 ± 5.2 hours respectively and a half-life of elimination of 13.3 ±5, 1.8±1 and 18.7 ±11.4 hours respectively. The volume of distribution was 13.62 ± 9.91 L/kg (CRP); 3.29± 0.75 L/kg (FXN) and 0.13 ± 0.03 L/kg (PBZ). Area under the curve until the last time point was 21.72± 20.10; 0.78± 0.28 and 263.35 ±68.69 μg/mL*h for CRP, FXN and PBZ respectively. Glucuronidation was identified in FXN and CRP treated birds. The long half-life of PBZ and CRP creates concern that accumulative toxicity may occur. Both FXN and PBZ are potentially hepatotoxic indicating that clinical use or the presence thereof in the food-chain should be avoided. CRP may be of clinical benefit in the vulture, but only as a single treatment. This drug should also be safe in the case of possible contamination of the food chain, as it is unlikely that vultures will be exposed to the drug often enough for it to be cumulative === Dissertation (MMedVet)--University of Pretoria, 2014. === tm2015 === Paraclinical Sciences === MMedVet === Unrestricted
author2 Naidoo, Vinny
author_facet Naidoo, Vinny
Fourie, Tamsyn Ann
author Fourie, Tamsyn Ann
author_sort Fourie, Tamsyn Ann
title The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study
title_short The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study
title_full The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study
title_fullStr The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study
title_full_unstemmed The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study
title_sort safety of carprofen, flunixin and phenylbutazone in the cape vulture (gyps coprotheres) – a pilot study
publisher University of Pretoria
publishDate 2015
url http://hdl.handle.net/2263/46035
Fourie, TA 2014, The safety of carprofen, flunixin and phenylbutazone in the Cape Vulture (Gyps coprotheres) – a pilot study, MMedVet Dissertation, University of Pretoria, Pretoria, viewed yymmdd <http://hdl.handle.net/2263/46035>
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AT fourietamsynann safetyofcarprofenflunixinandphenylbutazoneinthecapevulturegypscoprotheresapilotstudy
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