Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida
| Ano de defesa: | 2020 |
|---|---|
| Autor(a) principal: | |
| Orientador(a): | |
| Banca de defesa: | , |
| Tipo de documento: | Dissertação |
| Tipo de acesso: | Acesso aberto |
| Idioma: | por |
| Instituição de defesa: |
Universidade Estadual da Paraíba
|
| Programa de Pós-Graduação: |
Programa de Pós-Graduação em Ciências Farmacêuticas - PPGCF
|
| Departamento: |
Pró-Reitoria de Pós-Graduação e Pesquisa - PRPGP
|
| País: |
BR
|
| Palavras-chave em Português: | |
| Área do conhecimento CNPq: | |
| Link de acesso: | https://repositorio.uepb.edu.br/handle/123456789/73309 |
Resumo: | Therapeutic approaches to the treatment of inflammatory conditions are focused on suppressing, blocking or inhibiting inflammatory mediators. The drugs available on the market for these disorders, although effective, have as limitations gastrointestinal, renal, cardiovascular and metabolic disorders, making the development of new drugs necessary. The objective of this study was to develop, characterize and evaluate the in vitro and in vivo anti-inflammatory profile of the derivatives: 2-cyan N-phenylacetamide - JM-01; (E) -2-cyano-3- (1H-indol-3-yl) - N-phenylacrylamide - ICMD-01 and (E) -2-cyano-N,3-diphenylacrylamide -JMPR-01 and later determine the toxicological potential of the most promising compound. The compounds were obtained through an amidation reaction between substituted anilines and ethyl 2-cyanoacetate, followed by a Knoevenagel-type condensation reaction with substituted aldehydes, the structural elucidation being performed by spectroscopic and spectrometric techniques. To evaluate the anti-inflammatory potential in vitro, cell viability tests, cytokine and nitrite dosages in J774 macrophage cultures and in vivo: zymosan-induced peritonitis, edema, inflammatory hyperalgia, cytokine and prostaglandin E2 measurements CFA-induced. The antinociceptive effect and motor adaptive changes of animals treated with the compounds were evaluated by tail-flick and rota rod tests. The determination of safety of use was performed using single dose acute toxicity models, in vitro hemolytic activity and ulcerogenic susceptibility. Pharmacokinetic predictions were performed using the SwissADME and Xenosite platforms. The synthesis of the compounds JM-01, JMPR-01 and ICMD-01 proved feasible, with satisfactory yields easy to purify and with spectrometric and spectroscopic results consistent with the structure. In vitro results for the compounds showed significant inhibitions (p<0.05) of nitrite and cytokine production in concentrations up to 50 μM for JM-01 and JMPR-01 and 100 μM for ICMD-01. In the zymosan-induced peritonitis test all the derivatives showed inhibition of leukocyte migration at doses of (5, 10 and 50 mg kg^-1) significantly different from the control group (p<0.05) with activity higher than the group treated with indomethacin at doses of 10 mg kg^-1.In CFA-induced paw edema the compound with the best profile of antiedematogenic activity in times from 2 to 6 hours was the ICMD-01 (50 mg kg^-1), presenting respectively inhibition of 44.45, 57.14 and 67.34%. The ICMD-01 also showed a significant reduction (p<0.05) of local IL-1β and TNF-α and PGE2 levels when compared to the control group. For IL-1β and PGE2 inhibition promoted by the ICMD-01 is comparable to that of dexamethasone (2mg kg^-1), while for TNF-α the compound proved superior. Regarding the sedative, antinociceptive and central activity none of the compounds induced considerable effects. In the toxicological profile of ICMD-01, no relevant clinical signs or death were evidenced during the acute toxicity experiment, besides a good gastric tolerance. Also no excess degree of hemolytic activity was evidenced. In the pharmacokinetic predictions it was observed that the compounds JM-01, JMPR-01 and ICMD-01, are potentially well absorbed by the TGI and permeable to Hb in addition, have points susceptible to metabolization that can influence the pharmacological effect. These initial studies contribute to validate the biological potential of these derivatives, making them strong candidates for antiinflammatory drugs with low ulcerogenic potential. |
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2021-11-24T23:42:50Z2026-02-27T10:34:13Z2020-02-17SILVA, Pablo Rayff da. Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida. 2020. 111f. Dissertação (Programa de Pós-Graduação em Ciências Farmacêuticas - PPGCF) - Universidade Estadual da Paraíba, Campina Grande, 2021.https://repositorio.uepb.edu.br/handle/123456789/7330924004014014P8Therapeutic approaches to the treatment of inflammatory conditions are focused on suppressing, blocking or inhibiting inflammatory mediators. The drugs available on the market for these disorders, although effective, have as limitations gastrointestinal, renal, cardiovascular and metabolic disorders, making the development of new drugs necessary. The objective of this study was to develop, characterize and evaluate the in vitro and in vivo anti-inflammatory profile of the derivatives: 2-cyan N-phenylacetamide - JM-01; (E) -2-cyano-3- (1H-indol-3-yl) - N-phenylacrylamide - ICMD-01 and (E) -2-cyano-N,3-diphenylacrylamide -JMPR-01 and later determine the toxicological potential of the most promising compound. The compounds were obtained through an amidation reaction between substituted anilines and ethyl 2-cyanoacetate, followed by a Knoevenagel-type condensation reaction with substituted aldehydes, the structural elucidation being performed by spectroscopic and spectrometric techniques. To evaluate the anti-inflammatory potential in vitro, cell viability tests, cytokine and nitrite dosages in J774 macrophage cultures and in vivo: zymosan-induced peritonitis, edema, inflammatory hyperalgia, cytokine and prostaglandin E2 measurements CFA-induced. The antinociceptive effect and motor adaptive changes of animals treated with the compounds were evaluated by tail-flick and rota rod tests. The determination of safety of use was performed using single dose acute toxicity models, in vitro hemolytic activity and ulcerogenic susceptibility. Pharmacokinetic predictions were performed using the SwissADME and Xenosite platforms. The synthesis of the compounds JM-01, JMPR-01 and ICMD-01 proved feasible, with satisfactory yields easy to purify and with spectrometric and spectroscopic results consistent with the structure. In vitro results for the compounds showed significant inhibitions (p<0.05) of nitrite and cytokine production in concentrations up to 50 μM for JM-01 and JMPR-01 and 100 μM for ICMD-01. In the zymosan-induced peritonitis test all the derivatives showed inhibition of leukocyte migration at doses of (5, 10 and 50 mg kg^-1) significantly different from the control group (p<0.05) with activity higher than the group treated with indomethacin at doses of 10 mg kg^-1.In CFA-induced paw edema the compound with the best profile of antiedematogenic activity in times from 2 to 6 hours was the ICMD-01 (50 mg kg^-1), presenting respectively inhibition of 44.45, 57.14 and 67.34%. The ICMD-01 also showed a significant reduction (p<0.05) of local IL-1β and TNF-α and PGE2 levels when compared to the control group. For IL-1β and PGE2 inhibition promoted by the ICMD-01 is comparable to that of dexamethasone (2mg kg^-1), while for TNF-α the compound proved superior. Regarding the sedative, antinociceptive and central activity none of the compounds induced considerable effects. In the toxicological profile of ICMD-01, no relevant clinical signs or death were evidenced during the acute toxicity experiment, besides a good gastric tolerance. Also no excess degree of hemolytic activity was evidenced. In the pharmacokinetic predictions it was observed that the compounds JM-01, JMPR-01 and ICMD-01, are potentially well absorbed by the TGI and permeable to Hb in addition, have points susceptible to metabolization that can influence the pharmacological effect. These initial studies contribute to validate the biological potential of these derivatives, making them strong candidates for antiinflammatory drugs with low ulcerogenic potential.As abordagens terapêuticas para o tratamento de condições inflamatórias são focadas na supressão, bloqueio ou inibição de mediadores inflamatórios. Os medicamentos disponíveis no mercado para essas desordens apesar de efetivos, possuem como limitações os distúrbios gastrointestinais, renais, cardiovasculares e metabólicos, tornando o desenvolvimento de novos fármacos necessário. O objetivo desse estudo foi desenvolver, caracterizar e avaliar o perfil anti-inflamatório in vitro e in vivo dos derivados: 2-ciano N-fenilacetamida – JM-01; (E) -2- ciano-3- (1H-indol-3-il) -N-fenilacrilamida – ICMD-01 e (E) -2-ciano-N,3-difenilacrilamida – JMPR-01 e posteriormente determinar o potencial toxicológico do composto mais promissor. Os compostos foram obtidos por meio de uma reação de amidação entre anilinas substituídas e 2-cianoacetato de etila, seguido de uma reação de condensação do tipo Knoevenagel com aldeídos substituídos sendo a elucidação estrutural realizada por técnicas espectroscópicas e espectrométricas. Para avaliação do potencial anti-inflamatório in vitro foram realizados os ensaios de viabilidade celular, dosagens de citocinas e nitrito em culturas de macrófagos J774 e in vivo: peritonite induzida por zymosan, edema, hiperalgesia inflamatória, medições de citocinas e prostaglandina E2 induzido por CFA. O efeito antinociceptivo e as alterações adaptativas motoras dos animais tratados com os compostos foram avaliados pelos ensaios tail-flick e rota rod. A determinação da segurança de uso foi realizada empregando-se os modelos de toxicidade aguda de dose única, atividade hemolítica in vitro e suceptibilidade ulcerogênica. As predições farmacocinéticas foram realizadas utilizando as plataformas SwissADME e Xenosite. A síntese dos compostos JM-01, JMPR-01 e ICMD-01 mostrou-se viável, com rendimentos satisfatórios fácil purificação e com resultados espectroscópicos e espectrométricos condizentes a estrutura. Os resultados in vitro para os compostos apresentaram inibições significativas (p<0,05) da produção de nitrito e citocinas em concentrações de até 50 μM para o JM-01 e JMPR-01 e 100 μM para o ICMD-01. No teste de peritonite induzida por zymosan todos os derivados apresentaram inibição da migração leucocitária nas doses de (5, 10 e 50 mg kg^-1) significativamente diferente do grupo controle (p<0,05) com atividade superior ao grupo tratado com indometacina na dose de 10 mg kg^-1.No edema de pata induzido por CFA o composto com melhor perfil de atividade antiedematogênica nos tempos de 2 a 6h foi o ICMD-01 (50 mg kg^-1), apresentando respectivamente inibição de 44,45, 57,14 e 67,34%. O ICMD-01 também apresentou redução significativa (p< 0,05) dos níveis locais de IL-1β e TNF-α e PGE2 quando comparado ao grupo controle. Para a IL-1β e PGE2 inibição promovida pelo ICMD-01 é comparável ao da dexametasona (2mg kg^-1), enquanto para o TNF-α o composto mostrou-se superior. Com relação a atividade sedativa, antinociceptiva inflamatória e central nenhum dos compostos induziram efeitos consideráveis. No perfil toxicológico do ICMD-01, não foram evidenciados sinais clínicos relevantes nem morte durante a experimentação de toxicidade aguda, além de uma boa tolerabilidade gástrica. Também não foram evidenciados grau excedente de atividade hemolítica. Nas predições farmacocinéticas puderam-se observar que os compostos JM-01, JMPR-01 e ICMD-01, são potencialmente bem absorvidos pelo TGI e permeáveis a BHE além disso, apresentam pontos susceptíveis a metabolização que podem influenciar no efeito farmacológico. Esses estudos iniciais contribuem para validação do potencial biológico desses derivados, tornando-os fortes candidatos a fármacos anti-inflamatório com baixo potencial ulcerogênico.Fundação de Apoio à Pesquisa do Estado da Paraíba - FAPESQapplication/pdfUniversidade Estadual da ParaíbaPrograma de Pós-Graduação em Ciências Farmacêuticas - PPGCFUEPBBRPró-Reitoria de Pós-Graduação e Pesquisa - PRPGPPró-Reitoria de Pós-Graduação e Pesquisa - PRPGPCIENCIAS DA SAUDEFenilacrilamidaImunomodulaçãoInflamação agudaMediadores inflamatóriosSíntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamidainfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesisMoura, Ricardo Olímpio deCastellano, Lúcio Roberto CançadoPortela, Alyne da SilvaSantos, Vanda Lúcia dosSilva, Pablo Rayff dainfo:eu-repo/semantics/openAccessporreponame:Repositório Institucional da Universidade Estadual da Paraíba (UEPB)instname:Universidade Estadual da Paraíba (UEPB)instacron:UEPBLICENSElicense.txtlicense.txttext/plain; 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| dc.title.none.fl_str_mv |
Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida |
| title |
Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida |
| spellingShingle |
Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida Silva, Pablo Rayff da CIENCIAS DA SAUDE Fenilacrilamida Imunomodulação Inflamação aguda Mediadores inflamatórios |
| title_short |
Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida |
| title_full |
Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida |
| title_fullStr |
Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida |
| title_full_unstemmed |
Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida |
| title_sort |
Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida |
| author |
Silva, Pablo Rayff da |
| author_facet |
Silva, Pablo Rayff da |
| author_role |
author |
| dc.contributor.advisor-co1.fl_str_mv |
Moura, Ricardo Olímpio de |
| dc.contributor.referee1.fl_str_mv |
Castellano, Lúcio Roberto Cançado |
| dc.contributor.referee2.fl_str_mv |
Portela, Alyne da Silva |
| dc.contributor.advisor1.fl_str_mv |
Santos, Vanda Lúcia dos |
| dc.contributor.author.fl_str_mv |
Silva, Pablo Rayff da |
| contributor_str_mv |
Moura, Ricardo Olímpio de Castellano, Lúcio Roberto Cançado Portela, Alyne da Silva Santos, Vanda Lúcia dos |
| dc.subject.cnpq.fl_str_mv |
CIENCIAS DA SAUDE |
| topic |
CIENCIAS DA SAUDE Fenilacrilamida Imunomodulação Inflamação aguda Mediadores inflamatórios |
| dc.subject.por.fl_str_mv |
Fenilacrilamida Imunomodulação Inflamação aguda Mediadores inflamatórios |
| description |
Therapeutic approaches to the treatment of inflammatory conditions are focused on suppressing, blocking or inhibiting inflammatory mediators. The drugs available on the market for these disorders, although effective, have as limitations gastrointestinal, renal, cardiovascular and metabolic disorders, making the development of new drugs necessary. The objective of this study was to develop, characterize and evaluate the in vitro and in vivo anti-inflammatory profile of the derivatives: 2-cyan N-phenylacetamide - JM-01; (E) -2-cyano-3- (1H-indol-3-yl) - N-phenylacrylamide - ICMD-01 and (E) -2-cyano-N,3-diphenylacrylamide -JMPR-01 and later determine the toxicological potential of the most promising compound. The compounds were obtained through an amidation reaction between substituted anilines and ethyl 2-cyanoacetate, followed by a Knoevenagel-type condensation reaction with substituted aldehydes, the structural elucidation being performed by spectroscopic and spectrometric techniques. To evaluate the anti-inflammatory potential in vitro, cell viability tests, cytokine and nitrite dosages in J774 macrophage cultures and in vivo: zymosan-induced peritonitis, edema, inflammatory hyperalgia, cytokine and prostaglandin E2 measurements CFA-induced. The antinociceptive effect and motor adaptive changes of animals treated with the compounds were evaluated by tail-flick and rota rod tests. The determination of safety of use was performed using single dose acute toxicity models, in vitro hemolytic activity and ulcerogenic susceptibility. Pharmacokinetic predictions were performed using the SwissADME and Xenosite platforms. The synthesis of the compounds JM-01, JMPR-01 and ICMD-01 proved feasible, with satisfactory yields easy to purify and with spectrometric and spectroscopic results consistent with the structure. In vitro results for the compounds showed significant inhibitions (p<0.05) of nitrite and cytokine production in concentrations up to 50 μM for JM-01 and JMPR-01 and 100 μM for ICMD-01. In the zymosan-induced peritonitis test all the derivatives showed inhibition of leukocyte migration at doses of (5, 10 and 50 mg kg^-1) significantly different from the control group (p<0.05) with activity higher than the group treated with indomethacin at doses of 10 mg kg^-1.In CFA-induced paw edema the compound with the best profile of antiedematogenic activity in times from 2 to 6 hours was the ICMD-01 (50 mg kg^-1), presenting respectively inhibition of 44.45, 57.14 and 67.34%. The ICMD-01 also showed a significant reduction (p<0.05) of local IL-1β and TNF-α and PGE2 levels when compared to the control group. For IL-1β and PGE2 inhibition promoted by the ICMD-01 is comparable to that of dexamethasone (2mg kg^-1), while for TNF-α the compound proved superior. Regarding the sedative, antinociceptive and central activity none of the compounds induced considerable effects. In the toxicological profile of ICMD-01, no relevant clinical signs or death were evidenced during the acute toxicity experiment, besides a good gastric tolerance. Also no excess degree of hemolytic activity was evidenced. In the pharmacokinetic predictions it was observed that the compounds JM-01, JMPR-01 and ICMD-01, are potentially well absorbed by the TGI and permeable to Hb in addition, have points susceptible to metabolization that can influence the pharmacological effect. These initial studies contribute to validate the biological potential of these derivatives, making them strong candidates for antiinflammatory drugs with low ulcerogenic potential. |
| publishDate |
2020 |
| dc.date.issued.fl_str_mv |
2020-02-17 |
| dc.date.accessioned.fl_str_mv |
2021-11-24T23:42:50Z 2026-02-27T10:34:13Z |
| dc.type.status.fl_str_mv |
info:eu-repo/semantics/publishedVersion |
| dc.type.driver.fl_str_mv |
info:eu-repo/semantics/masterThesis |
| format |
masterThesis |
| status_str |
publishedVersion |
| dc.identifier.citation.fl_str_mv |
SILVA, Pablo Rayff da. Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida. 2020. 111f. Dissertação (Programa de Pós-Graduação em Ciências Farmacêuticas - PPGCF) - Universidade Estadual da Paraíba, Campina Grande, 2021. |
| dc.identifier.uri.fl_str_mv |
https://repositorio.uepb.edu.br/handle/123456789/73309 |
| dc.identifier.capesdegreeprogramcode.none.fl_str_mv |
24004014014P8 |
| identifier_str_mv |
SILVA, Pablo Rayff da. Síntese e perfil anti-inflamatório in vitro e in vivo de derivados fenilacetamida e fenilacrilamida. 2020. 111f. Dissertação (Programa de Pós-Graduação em Ciências Farmacêuticas - PPGCF) - Universidade Estadual da Paraíba, Campina Grande, 2021. 24004014014P8 |
| url |
https://repositorio.uepb.edu.br/handle/123456789/73309 |
| dc.language.iso.fl_str_mv |
por |
| language |
por |
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Universidade Estadual da Paraíba |
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Programa de Pós-Graduação em Ciências Farmacêuticas - PPGCF |
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UEPB |
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BR |
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Pró-Reitoria de Pós-Graduação e Pesquisa - PRPGP Pró-Reitoria de Pós-Graduação e Pesquisa - PRPGP |
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Universidade Estadual da Paraíba |
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UEPB |
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