Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos

Detalhes bibliográficos
Autor(a) principal: Macêdo, Luã Barbalho de
Data de Publicação: 2021
Tipo de documento: Tese
Idioma: por
Título da fonte: Repositório Digital da Universidade Federal Rural do Semi-Árido (RDU)
Texto Completo: https://repositorio.ufersa.edu.br/handle/prefix/6716
Resumo: The empirical extrapolation of the therapeutic protocols indicated for animals, although a routine practice, does not take into account the particularities of each species, increasing the risks of low efficacy in treatments, either by underdoses or by overdoses. The objective was to evaluate the pharmacokinetic profile of metamizole administered intravenously in isolation and in association with tramadol in donkeys. The ten animals were included in all study groups, with a 15-day rest period between treatments. The animals received four treatments. In the treatment M10 metamizole at a dose of 10 mg/kg, M25 - metamizole 25mg/kg and M10T2 - 10 mg/kg of metamizole combined with 2mg/kg of tramadol and in M25T2, 25 mg/kg metamizole with 2mg/kg tramadol. All treatments were performed in a single dose and intravenously. After predetermined times, blood samples were collected for further analysis. Plasma aliquots were processed and injected into the ultra-performance chromatographic system coupled to a mass spectrometer (UPLC-MS / MS). During the collections, the animals were observed for possible adverse manifestations. The parameters evaluated were: the maximum plasma concentration (Cmax), the time to reach the Cmax (Tmax), the area under the plasma concentration curve from time zero until the moment of the last measurable concentration (AUC0 → t) and the extrapolation of the AUC to infinity (AUC0 → ∞), apparent volume of distribution (Vz/F), apparent clearance (Cl/ F), elimination constant (Ke); elimination half-life (t1 / 2); Mean residual time until the last measurement (MRT0 → t), Mean residual time from zero to infinity (MRT0 → ∞), for drugs and their main metabolites. In groups M10 and M25, the parameters AUC0 → t, AUC0 → ∞, Cmax showed a significant increase in the two metabolites of metamizole in animals in the group M25. While Tmax, Vz / F and Cl / F had no statistical difference between groups. After intravenous administration of treatments M10T2 and M25T2, TRA, MAA, AA were detected within 24 hours of analysis and M1 up to 12 hours. Analyzing the TRA metabolite, it was observed that AUC0 → ∞ and CL / F were higher in the group treated with 10mg/kg of metamizole when compared to the 25mg/kg group. While the t ½; MRT0 → ∞; MRT0 → t are significantly higher in the M25T2 group. Regarding its by-product, M1, t 1/2; MRT0 → ∞; MRT0 → t were significantly higher in the second group. The Vz / F; MRT 0 → ∞, t1/2 of MAA and MRT0 → t of AA varied significantly between groups, being higher in animals that received 25mg/kg of Metamizole. Based on the results, it is possible to state that it was successful since it was possible to develop an analytical method capable of detecting and quantifying both drugs and their main metabolites in donkey blood for up to 48 hours. In addition, it proved that there are changes in some pharmacokinetic parameters when different doses of metamizole are administered and that they interfere with the metabolism of metamizole itself as well as tramadol and its most active metabolite, O-desmethyltramadol and that these findings may support future clinical trials for analgesic efficacy or even establish an appropriate dosage for donkeys
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spelling Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininosAnalgésicosEquídeosMetabólitosDipironaFarmacocinéticaAnalgesicsEquidaeMetabolitesDipyronePharmacokineticsCNPQ::CIENCIAS AGRARIAS::MEDICINA VETERINARIAThe empirical extrapolation of the therapeutic protocols indicated for animals, although a routine practice, does not take into account the particularities of each species, increasing the risks of low efficacy in treatments, either by underdoses or by overdoses. The objective was to evaluate the pharmacokinetic profile of metamizole administered intravenously in isolation and in association with tramadol in donkeys. The ten animals were included in all study groups, with a 15-day rest period between treatments. The animals received four treatments. In the treatment M10 metamizole at a dose of 10 mg/kg, M25 - metamizole 25mg/kg and M10T2 - 10 mg/kg of metamizole combined with 2mg/kg of tramadol and in M25T2, 25 mg/kg metamizole with 2mg/kg tramadol. All treatments were performed in a single dose and intravenously. After predetermined times, blood samples were collected for further analysis. Plasma aliquots were processed and injected into the ultra-performance chromatographic system coupled to a mass spectrometer (UPLC-MS / MS). During the collections, the animals were observed for possible adverse manifestations. The parameters evaluated were: the maximum plasma concentration (Cmax), the time to reach the Cmax (Tmax), the area under the plasma concentration curve from time zero until the moment of the last measurable concentration (AUC0 → t) and the extrapolation of the AUC to infinity (AUC0 → ∞), apparent volume of distribution (Vz/F), apparent clearance (Cl/ F), elimination constant (Ke); elimination half-life (t1 / 2); Mean residual time until the last measurement (MRT0 → t), Mean residual time from zero to infinity (MRT0 → ∞), for drugs and their main metabolites. In groups M10 and M25, the parameters AUC0 → t, AUC0 → ∞, Cmax showed a significant increase in the two metabolites of metamizole in animals in the group M25. While Tmax, Vz / F and Cl / F had no statistical difference between groups. After intravenous administration of treatments M10T2 and M25T2, TRA, MAA, AA were detected within 24 hours of analysis and M1 up to 12 hours. Analyzing the TRA metabolite, it was observed that AUC0 → ∞ and CL / F were higher in the group treated with 10mg/kg of metamizole when compared to the 25mg/kg group. While the t ½; MRT0 → ∞; MRT0 → t are significantly higher in the M25T2 group. Regarding its by-product, M1, t 1/2; MRT0 → ∞; MRT0 → t were significantly higher in the second group. The Vz / F; MRT 0 → ∞, t1/2 of MAA and MRT0 → t of AA varied significantly between groups, being higher in animals that received 25mg/kg of Metamizole. Based on the results, it is possible to state that it was successful since it was possible to develop an analytical method capable of detecting and quantifying both drugs and their main metabolites in donkey blood for up to 48 hours. In addition, it proved that there are changes in some pharmacokinetic parameters when different doses of metamizole are administered and that they interfere with the metabolism of metamizole itself as well as tramadol and its most active metabolite, O-desmethyltramadol and that these findings may support future clinical trials for analgesic efficacy or even establish an appropriate dosage for donkeysA extrapolação empírica dos protocolos terapêuticos indicados para animais, embora uma prática rotineira, não leva em consideração as particularidades de cada espécie, elevando os riscos de baixa eficácia nos tratamentos seja por subdoses seja por sobredoses. Objetivou-se avaliar o perfil farmacocinético do metamizol administrado por via intravenosa de forma isolada e em associação com tramadol em asininos. Foram utilizados 10 jumentos machos, saudáveis e inteiros. Os dez animais integraram todos os grupos do estudo, sendo realizado um período de descanso entre tratamentos de 15 dias. Os animais receberam quatro tratamentos. No tratamento M10 metamizol na dose de 10 mg/kg, M25 – metamizol 25mg/kg e M10T2 - 10 mg/kg de metamizol associado a 2mg/kg de tramadol e no M25T2, 25 mg/kg de metamizol com 2mg/kg de tramadol. Todos os tratamentos foram feitos em dose única e por via intravenosa. Após tempos pré-determinados, foram coletadas amostras de sangue para posterior análise. Alíquotas de plasmas foram processadas e injetadas no sistema cromatográfico de ultra performance acoplado a espectrômetro de massa (UPLC-MS/MS). Durante as coletas, os animais eram observados para possíveis manifestações adversas. Os parâmetros avaliados foram: a concentração plasmática máxima (Cmax), o tempo para atingir a Cmax (Tmax), a área sob a curva de concentração plasmática do tempo zero até ao momento da última concentração mensurável (AUC0→t) e a extrapolação da AUC até ao infinito (AUC0→ ∞), volume de distribuição aparente (Vz/F), depuração aparente (CL/F), constante de eliminação (Ke); meia-vida de eliminação (t1/2); Tempo médio residual até o momento da última mensuração (MRT0→ t ), Tempo médio residual do momento zero até o infinito(MRT0→ ∞), para os fármacos e seus principais metabólitos. Nos grupos M10 e M25, os parâmetros AUC0→t, AUC0→ ∞, Cmax apresentaram um aumento significativo nos dois metabólitos do metamizol nos animais do grupo M25. Enquanto que o Tmax, Vz/F e o Cl/F não tiveram diferença estatística entre os grupos. Após administração intravenosa dos tratamentos M10T2 e M25T2, o TRA, MAA, AA foram detectados em até 24 horas de análise e o M1 até 12 horas. Analisando o metabólito do TRA, observou-se que a AUC0→ ∞ e o CL/F foi maior no grupo tratado com 10mg/kg de metamizol quando comparado com o de 25 mg/kg. Enquanto o t ½; MRT0→ ∞; MRT0→ t apresentam-se significativa maiores no grupo M25T2. Em relação ao seu subproduto, o M1, o t1/2; MRT0→ ∞; MRT0→ t apresentaram-se significativamente maiores no segundo grupo. O Vz/F; MRT 0→ ∞, t 1/2 do MAA e o MRT0→ t do AA variou significativamente entre os grupos sendo maiores nos animais que receberam 25mg/kg de Metamizol. Com base nos resultados é possível afirmar que obteve êxito uma vez que foi possível desenvolver método analítico capaz de detectar e quantificar ambos os fármacos e seus principais metabolitos no sangue de asinino por até 48 horas. Além disso, comprovou que existem alterações em alguns parâmetros farmacocinéticos quando há administração de diferentes doses de metamizol e que as mesmas interferem no metabolismo do próprio metamizol como também tramadol e de seu metabólito mais ativo, o O-desmetiltramadol e que esses achados podem subsidiar futuros ensaios clínicos para eficácia analgésica ou mesmo estabelecer posologia adequada para jumentosCoordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPESUniversidade Federal Rural do Semi-ÁridoBrasilCentro de Ciências Agrárias - CCAUFERSAPrograma de Pós-Graduação em Ciência AnimalPaula, Valéria Veras de36261300372http://lattes.cnpq.br/9083821440600669Paula, Valéria Veras de36261300372http://lattes.cnpq.br/9083821440600669Silva, Gabriel Araujo da00885938518http://lattes.cnpq.br/8633733418545174Nunes, Talyta Lins06494007473http://lattes.cnpq.br/5769091133376552Barreto Júnior, Raimundo Alves43214363387http://lattes.cnpq.br/0516971232838494Moura, Carlos Eduardo Bezerra de3597959431http://lattes.cnpq.br/4717410137206021Macêdo, Luã Barbalho de2021-12-02T21:02:53Z2021-04-262021-12-02T21:02:53Z2021-02-26info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/doctoralThesisapplication/pdfMacêdo (2021) (MACÊDO, 2021)https://repositorio.ufersa.edu.br/handle/prefix/6716porMACêDO, Luã Barbalho de. Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos. 2021. 84 f. Tese (Doutorado em Ciência Animal), Universidade Federal Rural do Semi-Árido, Mossoró, 2021.CC-BY-SAhttps://creativecommons.org/licenses/by-sa/4.0/deed.pt_BRinfo:eu-repo/semantics/openAccessreponame:Repositório Digital da Universidade Federal Rural do Semi-Árido (RDU)instname:Universidade Federal Rural do Semi-Árido (UFERSA)instacron:UFERSA2023-10-30T20:27:24Zoai:repositorio.ufersa.edu.br:prefix/6716Repositório Institucionalhttps://repositorio.ufersa.edu.br/PUBhttps://repositorio.ufersa.edu.br/server/oai/requestrepositorio@ufersa.edu.br || admrepositorio@ufersa.edu.bropendoar:2023-10-30T20:27:24Repositório Digital da Universidade Federal Rural do Semi-Árido (RDU) - Universidade Federal Rural do Semi-Árido (UFERSA)false
dc.title.none.fl_str_mv Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos
title Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos
spellingShingle Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos
Macêdo, Luã Barbalho de
Analgésicos
Equídeos
Metabólitos
Dipirona
Farmacocinética
Analgesics
Equidae
Metabolites
Dipyrone
Pharmacokinetics
CNPQ::CIENCIAS AGRARIAS::MEDICINA VETERINARIA
title_short Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos
title_full Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos
title_fullStr Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos
title_full_unstemmed Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos
title_sort Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos
author Macêdo, Luã Barbalho de
author_facet Macêdo, Luã Barbalho de
author_role author
dc.contributor.none.fl_str_mv Paula, Valéria Veras de
36261300372
http://lattes.cnpq.br/9083821440600669
Paula, Valéria Veras de
36261300372
http://lattes.cnpq.br/9083821440600669
Silva, Gabriel Araujo da
00885938518
http://lattes.cnpq.br/8633733418545174
Nunes, Talyta Lins
06494007473
http://lattes.cnpq.br/5769091133376552
Barreto Júnior, Raimundo Alves
43214363387
http://lattes.cnpq.br/0516971232838494
Moura, Carlos Eduardo Bezerra de
3597959431
http://lattes.cnpq.br/4717410137206021
dc.contributor.author.fl_str_mv Macêdo, Luã Barbalho de
dc.subject.por.fl_str_mv Analgésicos
Equídeos
Metabólitos
Dipirona
Farmacocinética
Analgesics
Equidae
Metabolites
Dipyrone
Pharmacokinetics
CNPQ::CIENCIAS AGRARIAS::MEDICINA VETERINARIA
topic Analgésicos
Equídeos
Metabólitos
Dipirona
Farmacocinética
Analgesics
Equidae
Metabolites
Dipyrone
Pharmacokinetics
CNPQ::CIENCIAS AGRARIAS::MEDICINA VETERINARIA
description The empirical extrapolation of the therapeutic protocols indicated for animals, although a routine practice, does not take into account the particularities of each species, increasing the risks of low efficacy in treatments, either by underdoses or by overdoses. The objective was to evaluate the pharmacokinetic profile of metamizole administered intravenously in isolation and in association with tramadol in donkeys. The ten animals were included in all study groups, with a 15-day rest period between treatments. The animals received four treatments. In the treatment M10 metamizole at a dose of 10 mg/kg, M25 - metamizole 25mg/kg and M10T2 - 10 mg/kg of metamizole combined with 2mg/kg of tramadol and in M25T2, 25 mg/kg metamizole with 2mg/kg tramadol. All treatments were performed in a single dose and intravenously. After predetermined times, blood samples were collected for further analysis. Plasma aliquots were processed and injected into the ultra-performance chromatographic system coupled to a mass spectrometer (UPLC-MS / MS). During the collections, the animals were observed for possible adverse manifestations. The parameters evaluated were: the maximum plasma concentration (Cmax), the time to reach the Cmax (Tmax), the area under the plasma concentration curve from time zero until the moment of the last measurable concentration (AUC0 → t) and the extrapolation of the AUC to infinity (AUC0 → ∞), apparent volume of distribution (Vz/F), apparent clearance (Cl/ F), elimination constant (Ke); elimination half-life (t1 / 2); Mean residual time until the last measurement (MRT0 → t), Mean residual time from zero to infinity (MRT0 → ∞), for drugs and their main metabolites. In groups M10 and M25, the parameters AUC0 → t, AUC0 → ∞, Cmax showed a significant increase in the two metabolites of metamizole in animals in the group M25. While Tmax, Vz / F and Cl / F had no statistical difference between groups. After intravenous administration of treatments M10T2 and M25T2, TRA, MAA, AA were detected within 24 hours of analysis and M1 up to 12 hours. Analyzing the TRA metabolite, it was observed that AUC0 → ∞ and CL / F were higher in the group treated with 10mg/kg of metamizole when compared to the 25mg/kg group. While the t ½; MRT0 → ∞; MRT0 → t are significantly higher in the M25T2 group. Regarding its by-product, M1, t 1/2; MRT0 → ∞; MRT0 → t were significantly higher in the second group. The Vz / F; MRT 0 → ∞, t1/2 of MAA and MRT0 → t of AA varied significantly between groups, being higher in animals that received 25mg/kg of Metamizole. Based on the results, it is possible to state that it was successful since it was possible to develop an analytical method capable of detecting and quantifying both drugs and their main metabolites in donkey blood for up to 48 hours. In addition, it proved that there are changes in some pharmacokinetic parameters when different doses of metamizole are administered and that they interfere with the metabolism of metamizole itself as well as tramadol and its most active metabolite, O-desmethyltramadol and that these findings may support future clinical trials for analgesic efficacy or even establish an appropriate dosage for donkeys
publishDate 2021
dc.date.none.fl_str_mv 2021-12-02T21:02:53Z
2021-04-26
2021-12-02T21:02:53Z
2021-02-26
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/doctoralThesis
format doctoralThesis
status_str publishedVersion
dc.identifier.uri.fl_str_mv Macêdo (2021) (MACÊDO, 2021)
https://repositorio.ufersa.edu.br/handle/prefix/6716
identifier_str_mv Macêdo (2021) (MACÊDO, 2021)
url https://repositorio.ufersa.edu.br/handle/prefix/6716
dc.language.iso.fl_str_mv por
language por
dc.relation.none.fl_str_mv MACêDO, Luã Barbalho de. Perfil farmacocinético do metamizol isolado e associado ao tramadol após administração intravenosa em asininos. 2021. 84 f. Tese (Doutorado em Ciência Animal), Universidade Federal Rural do Semi-Árido, Mossoró, 2021.
dc.rights.driver.fl_str_mv CC-BY-SA
https://creativecommons.org/licenses/by-sa/4.0/deed.pt_BR
info:eu-repo/semantics/openAccess
rights_invalid_str_mv CC-BY-SA
https://creativecommons.org/licenses/by-sa/4.0/deed.pt_BR
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
dc.publisher.none.fl_str_mv Universidade Federal Rural do Semi-Árido
Brasil
Centro de Ciências Agrárias - CCA
UFERSA
Programa de Pós-Graduação em Ciência Animal
publisher.none.fl_str_mv Universidade Federal Rural do Semi-Árido
Brasil
Centro de Ciências Agrárias - CCA
UFERSA
Programa de Pós-Graduação em Ciência Animal
dc.source.none.fl_str_mv reponame:Repositório Digital da Universidade Federal Rural do Semi-Árido (RDU)
instname:Universidade Federal Rural do Semi-Árido (UFERSA)
instacron:UFERSA
instname_str Universidade Federal Rural do Semi-Árido (UFERSA)
instacron_str UFERSA
institution UFERSA
reponame_str Repositório Digital da Universidade Federal Rural do Semi-Árido (RDU)
collection Repositório Digital da Universidade Federal Rural do Semi-Árido (RDU)
repository.name.fl_str_mv Repositório Digital da Universidade Federal Rural do Semi-Árido (RDU) - Universidade Federal Rural do Semi-Árido (UFERSA)
repository.mail.fl_str_mv repositorio@ufersa.edu.br || admrepositorio@ufersa.edu.br
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