Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus)
| Autor(a) principal: | |
|---|---|
| Data de Publicação: | 2019 |
| Tipo de documento: | Dissertação |
| Idioma: | por |
| Título da fonte: | Repositório Digital da Universidade Federal Rural do Semi-Árido (RDU) |
| Texto Completo: | https://repositorio.ufersa.edu.br/handle/prefix/5318 |
Resumo: | Donkeys are rustic animals that quickly adapt to adverse conditions and intense traction work, and are constantly exposed to painful clinical conditions, so it is of paramount importance to treat them adequately through the use of appropriate analgesics. Tramadol is a centrally acting opioid analgesic widely used to treat acute and chronic pain in humans and animals. Its hepatic metabolization results in several metabolites, the main one being the active metabolite O-desmethyltramadol (M1), since it has higher affinity for opioid receptors. The aim of the present study was to describe the pharmacokinetics of tramadol and M1 following single intravenous administration of two distinct doses in donkeys. Ten adult, healthy, male and whole donkeys were used. In group T2, 8 animals received the 2 mg.kg-1 dose of tramadol and in group T4, the same 8 animals received the dose of 4 mg.kg-1, with an interval of 15 days between treatments. 10 ml of jugular vein blood were collected to obtain plasma and the samples were conditioned at -80 ° C for further pharmacokinetic analysis by ultra-efficient liquid chromatography coupled with a mass spectrometry detector (UPLC-MS/MS) using a non-compartmental model. Blood collection was performed at time 0 (prior to drug administration) and following the times: 5, 10, 20, 30, 40, 50 minutes, 1h, 1: 15h, 1: 30h, 1: 45h, 2h, 2:30 h, 3h, 4h, 6h, 8h, 12h, 24h and 48h. Adverse effects from drug administration were also observed. Tramadol and M1 were measured up to 48 hours and quantified up to 12 hours after administration. The 4 mg.kg-1 dose showed a significant increase in mean residual time (MRT0 → ∞) and time half-life elmmination (t1/2) for the metabolite. For tramadol, the mean maximum plasma concentration (Cmax), t1/2 and MRT0 → ∞ for 2 mg.kg-1 were 473,62ng/ml, 4,49h e 1,44 h, while at 4mg dose. kg-1 were 7553,93 ng/ml 5,99 h e 2,27 h. For M1, Cmax, t1/2, Tmax and MRT0 → ∞ for the lowest dose were 90,37 ng/ml, 2,50 h, 0,94 h e 3,88 h, while for the highest dose they were 109,62 ng/ml, 6,95h, 1,19 h e 7,42 h. At the lower dose, one animal presented ataxia and muscle spasms, while at the higher dose, seven animals presented these effects. Tramadol and M1 reached plasma concentrations considered effective for analgesia. Dosing intervals of approximately 2.5 and 6.9 hours are suggested for the 2 and 4 mg/kg-1 doses respectively. A longer tramadol administration time is required to avoid adverse effects. |
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Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus)EquídeosM1FarmacocinéticaAnalgesiaJumentos NordestinosEquinesM1PharmacokineticsAnalgesiaNortheast donkeysCNPQ::CIENCIAS AGRARIAS::MEDICINA VETERINARIADonkeys are rustic animals that quickly adapt to adverse conditions and intense traction work, and are constantly exposed to painful clinical conditions, so it is of paramount importance to treat them adequately through the use of appropriate analgesics. Tramadol is a centrally acting opioid analgesic widely used to treat acute and chronic pain in humans and animals. Its hepatic metabolization results in several metabolites, the main one being the active metabolite O-desmethyltramadol (M1), since it has higher affinity for opioid receptors. The aim of the present study was to describe the pharmacokinetics of tramadol and M1 following single intravenous administration of two distinct doses in donkeys. Ten adult, healthy, male and whole donkeys were used. In group T2, 8 animals received the 2 mg.kg-1 dose of tramadol and in group T4, the same 8 animals received the dose of 4 mg.kg-1, with an interval of 15 days between treatments. 10 ml of jugular vein blood were collected to obtain plasma and the samples were conditioned at -80 ° C for further pharmacokinetic analysis by ultra-efficient liquid chromatography coupled with a mass spectrometry detector (UPLC-MS/MS) using a non-compartmental model. Blood collection was performed at time 0 (prior to drug administration) and following the times: 5, 10, 20, 30, 40, 50 minutes, 1h, 1: 15h, 1: 30h, 1: 45h, 2h, 2:30 h, 3h, 4h, 6h, 8h, 12h, 24h and 48h. Adverse effects from drug administration were also observed. Tramadol and M1 were measured up to 48 hours and quantified up to 12 hours after administration. The 4 mg.kg-1 dose showed a significant increase in mean residual time (MRT0 → ∞) and time half-life elmmination (t1/2) for the metabolite. For tramadol, the mean maximum plasma concentration (Cmax), t1/2 and MRT0 → ∞ for 2 mg.kg-1 were 473,62ng/ml, 4,49h e 1,44 h, while at 4mg dose. kg-1 were 7553,93 ng/ml 5,99 h e 2,27 h. For M1, Cmax, t1/2, Tmax and MRT0 → ∞ for the lowest dose were 90,37 ng/ml, 2,50 h, 0,94 h e 3,88 h, while for the highest dose they were 109,62 ng/ml, 6,95h, 1,19 h e 7,42 h. At the lower dose, one animal presented ataxia and muscle spasms, while at the higher dose, seven animals presented these effects. Tramadol and M1 reached plasma concentrations considered effective for analgesia. Dosing intervals of approximately 2.5 and 6.9 hours are suggested for the 2 and 4 mg/kg-1 doses respectively. A longer tramadol administration time is required to avoid adverse effects.Os jumentos são animais rústicos que rapidamente se adaptam às condições adversas e ao intenso trabalho à tração, estando constantemente expostos a condições clínicas dolorosas e, por isso é de suma importância tratá-la adequadamente, por meio do uso de analgésicos apropriados. O tramadol é um analgésico opioide de ação central amplamente utilizado para tratamento da dor aguda e crônica em humanos e animais. Sua metabolização hepática resulta em diversos metabólitos, sendo o principal destes o metabólito ativo O-desmetiltramadol (M1), pois apresenta maior afinidade pelos receptores opioides. O objetivo do presente estudo foi descrever a farmacocinética do tramadol e do M1, após a administração intravenosa única de duas doses distintas em jumentos. Foram utilizados 8 asininos adultos, hígidos, machos e inteiros. Os 8 animais receberam a dose de 2 mg.kg-1 (T2) e 4 mg.kg-1 (T4) de tramadol, com intervalo de 15 dias entre os tratamentos. Foram coletados 10 ml de sangue da veia jugular para obtenção do plasma, realizados nos momentos 0 (antes da administração do fármaco) e seguindo os tempos: 5, 10, 20, 30, 40, 50 minutos, 1h, 1:15h, 1:30h, 1:45h, 2h, 2:30h, 3h, 4h, 6h, 8h, 12h, 24h e 48h. As amostras foram acondicionadas a -80°C para posterior análise farmacocinética por meio de cromatografia líquida de ultra eficiência acoplada a um detector de espectrometria de massas (CLUE-MS/MS), utilizando um modelo não compartimental. O tramadol e o M1 foram mensurados até 48 horas e quantificados até 12 horas após a administração. Os efeitos adversos decorrentes da administração do fármaco foram observados. A dose de 4 mg.kg-1 apresentou aumento significativo do tempo residual médio (TRM0→ ∞) e tempo de meia vida (t1/2) para o metabólito. Para o tramadol, a concentração plasmática máxima média (Cmáx), o t1/2 e TMR0→ ∞ para 2 mg.kg-1 foram de 473,62ng/ml, 4,49h e 1,44 h, enquanto na dose 4mg.kg-1 foram de 7553,93 ng/ml 5,99 h e 2,27 h. Para o M1, a Cmáx,t1/2, Tmáx e TRM0→ ∞ para a menor dose foram de 90,37 ng/ml, 2,50 h, 0,94 h e 3,88 h, enquanto para a maior dose foram de 109,62 ng/ml, 6,95h, 1,19 h e 7,42 h. Na menor dose, um animal apresentou ataxia e espasmos musculares, enquanto na maior dose, sete animais apresentaram esses efeitos. O tramadol e o M1 atingiram concentrações plasmáticas consideradas efetivas para analgesia. Sugere-se intervalo de administração de aproximadamente 2,5 e 6,9 horas para as doses de 2 e 4 mg.kg-1 respectivamente. Para evitar a ocorrência de efeitos adversos, é necessário administrar o fármaco em um tempo mais prolongado.Coordenação 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/9083821440600669Barrêto Júnior, Raimundo Alves43214363387http://lattes.cnpq.br/0516971232838494Abrantes, Maria Rociene05476448411http://lattes.cnpq.br/8581676690083096Mouta, Andressa Nunes2020-08-27T18:30:27Z2020-03-022020-08-27T18:30:27Z2019-12-12info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesisapplication/pdfCitação com autor incluído no texto: Mouta (2019) Citação com autor não incluído no texto: (MOUTA, 2019)https://repositorio.ufersa.edu.br/handle/prefix/5318porMOUTA, Andressa Nunes. Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus). 2019. 51 f. Dissertação (Mestrado em Ciência Animal), Universidade Federal Rural do Semi-Árido, Mossoró, 2019.CC-BY-SAinfo:eu-repo/semantics/openAccessreponame:Repositório Digital da Universidade Federal Rural do Semi-Árido (RDU)instname:Universidade Federal Rural do Semi-Árido (UFERSA)instacron:UFERSA2023-10-30T20:28:23Zoai:repositorio.ufersa.edu.br:prefix/5318Repositório Institucionalhttps://repositorio.ufersa.edu.br/PUBhttps://repositorio.ufersa.edu.br/server/oai/requestrepositorio@ufersa.edu.br || admrepositorio@ufersa.edu.bropendoar:2023-10-30T20:28:23Repositório 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 tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus) |
| title |
Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus) |
| spellingShingle |
Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus) Mouta, Andressa Nunes Equídeos M1 Farmacocinética Analgesia Jumentos Nordestinos Equines M1 Pharmacokinetics Analgesia Northeast donkeys CNPQ::CIENCIAS AGRARIAS::MEDICINA VETERINARIA |
| title_short |
Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus) |
| title_full |
Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus) |
| title_fullStr |
Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus) |
| title_full_unstemmed |
Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus) |
| title_sort |
Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus) |
| author |
Mouta, Andressa Nunes |
| author_facet |
Mouta, Andressa Nunes |
| author_role |
author |
| dc.contributor.none.fl_str_mv |
Paula, Valéria Veras de 36261300372 http://lattes.cnpq.br/9083821440600669 Barrêto Júnior, Raimundo Alves 43214363387 http://lattes.cnpq.br/0516971232838494 Abrantes, Maria Rociene 05476448411 http://lattes.cnpq.br/8581676690083096 |
| dc.contributor.author.fl_str_mv |
Mouta, Andressa Nunes |
| dc.subject.por.fl_str_mv |
Equídeos M1 Farmacocinética Analgesia Jumentos Nordestinos Equines M1 Pharmacokinetics Analgesia Northeast donkeys CNPQ::CIENCIAS AGRARIAS::MEDICINA VETERINARIA |
| topic |
Equídeos M1 Farmacocinética Analgesia Jumentos Nordestinos Equines M1 Pharmacokinetics Analgesia Northeast donkeys CNPQ::CIENCIAS AGRARIAS::MEDICINA VETERINARIA |
| description |
Donkeys are rustic animals that quickly adapt to adverse conditions and intense traction work, and are constantly exposed to painful clinical conditions, so it is of paramount importance to treat them adequately through the use of appropriate analgesics. Tramadol is a centrally acting opioid analgesic widely used to treat acute and chronic pain in humans and animals. Its hepatic metabolization results in several metabolites, the main one being the active metabolite O-desmethyltramadol (M1), since it has higher affinity for opioid receptors. The aim of the present study was to describe the pharmacokinetics of tramadol and M1 following single intravenous administration of two distinct doses in donkeys. Ten adult, healthy, male and whole donkeys were used. In group T2, 8 animals received the 2 mg.kg-1 dose of tramadol and in group T4, the same 8 animals received the dose of 4 mg.kg-1, with an interval of 15 days between treatments. 10 ml of jugular vein blood were collected to obtain plasma and the samples were conditioned at -80 ° C for further pharmacokinetic analysis by ultra-efficient liquid chromatography coupled with a mass spectrometry detector (UPLC-MS/MS) using a non-compartmental model. Blood collection was performed at time 0 (prior to drug administration) and following the times: 5, 10, 20, 30, 40, 50 minutes, 1h, 1: 15h, 1: 30h, 1: 45h, 2h, 2:30 h, 3h, 4h, 6h, 8h, 12h, 24h and 48h. Adverse effects from drug administration were also observed. Tramadol and M1 were measured up to 48 hours and quantified up to 12 hours after administration. The 4 mg.kg-1 dose showed a significant increase in mean residual time (MRT0 → ∞) and time half-life elmmination (t1/2) for the metabolite. For tramadol, the mean maximum plasma concentration (Cmax), t1/2 and MRT0 → ∞ for 2 mg.kg-1 were 473,62ng/ml, 4,49h e 1,44 h, while at 4mg dose. kg-1 were 7553,93 ng/ml 5,99 h e 2,27 h. For M1, Cmax, t1/2, Tmax and MRT0 → ∞ for the lowest dose were 90,37 ng/ml, 2,50 h, 0,94 h e 3,88 h, while for the highest dose they were 109,62 ng/ml, 6,95h, 1,19 h e 7,42 h. At the lower dose, one animal presented ataxia and muscle spasms, while at the higher dose, seven animals presented these effects. Tramadol and M1 reached plasma concentrations considered effective for analgesia. Dosing intervals of approximately 2.5 and 6.9 hours are suggested for the 2 and 4 mg/kg-1 doses respectively. A longer tramadol administration time is required to avoid adverse effects. |
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2019 |
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2019-12-12 2020-08-27T18:30:27Z 2020-03-02 2020-08-27T18:30:27Z |
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info:eu-repo/semantics/publishedVersion |
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Citação com autor incluído no texto: Mouta (2019) Citação com autor não incluído no texto: (MOUTA, 2019) https://repositorio.ufersa.edu.br/handle/prefix/5318 |
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Citação com autor incluído no texto: Mouta (2019) Citação com autor não incluído no texto: (MOUTA, 2019) |
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https://repositorio.ufersa.edu.br/handle/prefix/5318 |
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por |
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MOUTA, Andressa Nunes. Perfil farmacocinético do tramadol e o-desmetiltramadol após administração intravenosa em jumentos (equus asinus). 2019. 51 f. Dissertação (Mestrado em Ciência Animal), Universidade Federal Rural do Semi-Árido, Mossoró, 2019. |
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CC-BY-SA |
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openAccess |
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Universidade Federal Rural do Semi-Árido Brasil Centro de Ciências Agrárias - CCA UFERSA Programa de Pós-Graduação em Ciência Animal |
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Universidade Federal Rural do Semi-Árido Brasil Centro de Ciências Agrárias - CCA UFERSA Programa de Pós-Graduação em Ciência Animal |
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