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1. SÍNTESE, ESTUDO DE DOCAGEM E AVALIAÇÃO BIOLÓGICA DE DERIVADOS DA 4-AMINOANTIPIRINA-ISONIAZIDA COMO AGENTES HÍBRIDOS ANTIBACTERIANOS E ANALGÉSICOS.

Author

MOHAMMAD, Abeer Essa, MUHAMMAD-ALI, Munther Abduljaleel, and JASIM, Ekhlas Qanber

Subjects
*CHEMICAL synthesis, *BINDING energy, *ANTIBACTERIAL agents, *DRUG standards, *CHEMICAL reactions, *PYRAZOLONES, *TETRAZOLES
Abstract

Background: 4-aminoantipyrine is one of the pyrazolone derivatives, it has been exposed to a large range of biological activities as an antimicrobial, analgesic, antiviral, anti-inflammatory, and anticancer compound. One of the important derivatives is the hybrid pyrazolone which includes two organic or inorganic drugs attached to give new pharmaceutical agents which may be the same or different activity from the original drugs. Aim: This research aimed to synthesize novel compounds derived from 4-aminoantipyrine and test their biological activity. Methods: Synthesis of 4-aminoantipyrine derivatives, which contain structurally two heterocyclic moieties, pyrazolone with oxadiazole, triazole, or tetrazole rings. The structures of the compounds were identified by 1H-NMR and FT-IR spectroscopy. The in vitro, developed compounds were screened for their analgesic activity and antibacterial activity against medically important gram (+) and gram (-) bacterial strains. Results: The antibacterial evaluation tests showed that some compounds gave good activity and others had no activity. The analgesic activity referred that the synthesized compounds had promising potency. The free binding energy (S) of the compounds with the protein 6B73 were -4.90 to -8.76 kcal/mol, whereas free energy (S) with the protein 5C1M gave -4.94 to -9.21 kcal/mol. Discussion: Among the tested compounds, it was found that compounds 1a, 4b, and 5a had more potent antibacterial activity. The analgesic activity showed that compounds 1b, 4b, and 5a gave the best activity using hot plate methods compared with the standard drug. On the other hand, compounds 1a, 4b, and 5b gave good activity using the writhing test method. Conclusions: Potent, good, or moderate analgesic and antibacterial agents were synthesized using simple and high-yield chemical reactions. The chemical reactions include the synthesis of hybrid antibacterial and analgesic agents using pyrazolone compounds. [ABSTRACT FROM AUTHOR]

Published
2022
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2. CONCENTRAÇÃO DA SOLUÇÃO DE TETRAZÓLIO E PERÍODO DE COLORAÇÃO DO TESTE PARA SEMENTES DE MAMONEIRA.

Author

GASPAR-OLIVEIRA, CAROLINA MARIA, MARTINS, CIBELE CHALITA, and NAKAGAWA, JOÃO

Subjects
*TETRAZOLES, *CASTOR beans, *OILSEEDS, *TETRAZOLIUM, *RICIN, *CASTOR oil plant, *PLANT physiology, *GERMINATION, *SEEDS
Abstract

The objective of this research was to study the tetrazolium solution concentration and staining period for the evaluation of the physiological quality of castor bean seeds (Ricinus communis L.) by the tetrazolium test, standardizing the nomenclature of the observed colors in seeds after staining. The treatments of tetrazolium solution concentration and staining period were: 0.075% and 0.1% for 120, 180 and 240 minutes, 0.2% for 60, 120 and 180 minutes, 0.5% for 60, 90 and 120 minutes and 1.0% for 30, 60 and 90 minutes. The results were compared to the germination test. The seed color after the tetrazolium test in each treatment was evaluated by comparing with the Munsell book of color, and the percentage of seeds observed in each color was established. A randomized complete block design was used and the means were compared by the Tukey test at the 0.05 level of probability. To evaluate physiological quality by the tetrazolium test, castor bean seeds should be placed in tetrazolium solution at the concentration 0.2% for 120 minutes, at 35°C, for staining development, and in this treatment, the viable seeds after the staining in tetrazolium solution showed predominantly the colors pink and dark pink in their essential structures. Thus these colors can be considered as the characteristics colors for the tetrazolium test in castor bean seeds. [ABSTRACT FROM AUTHOR]

Published
2009
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3. AVALIAÇÃO DA VIABILIDADE DE SEMENTES DE PINHÃO MANSO PELOS TESTES DE TETRAZÓLIO E DE RAIOS X.

Author

PINTO, TAIS LEITE FERREIRA, FILHO, JULIO MARCOS, FORTI, VICTOR AUGUSTO, DE CARVALHO, CRISTIANE, and GOMES, JUNIOR, FRANCISCO GUILHIEN

Subjects
*JATROPHA, *EUPHORBIACEAE, *SEED viability, *TETRAZOLIUM, *TETRAZOLES, *SEED quality, *GERMINATION, *PLANT physiology, *X-rays
Abstract

The Jatropha-curcas L. presents a great potential for fuel, but there are few studies to assess seed quality of this species. Therefore, this research aimed to study the performance of the tetrazolium salt test procedures and to verify the efficiency of the X-ray test to evaluate the seed viability of this species. Seeds were hydrated between paper towel and immersed in water to reach 30 and 40% m.c.. Following, seed coat was removed manually and seeds were immersed in 0,075 and 0,5% tetrazolium solutions for 120 mm., respectively, at 40°C. Best results of tetrazolium test comprised the hydration between paper, until the seeds reach 30% m.c. and coloration in contact with a solution of 0,5%. The Jatropha curcas L. seeds were also submitted to X-ray test, in intensity of the 25Kv for 60s. Results of tetrazolium and X-ray tests were compared to germination and it was shown that both are efficient to assess Jatropha curcas L. seeds viability. [ABSTRACT FROM AUTHOR]

Published
2009
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4. TESTE DE TETRAZÓLIO PARA AVALIAÇÃO DA QUALIDADE DE SEMENTES DE CLITOREA TERNATEA L.

Author

DEMINICIS, BRUNO BORGES, VIEIRA, HENRIQUE DUARTE, and DA SILVA, ROBERTO FERREIRA

Subjects
*SEED quality, *SEED physiology, *TETRAZOLIUM, *ORGANONITROGEN compounds, *CENTROSEMA, *LEGUMES, *GERMINATION, *PLANT physiology, *TETRAZOLES
Abstract

This research verified different methods of pre-conditioning and concentrations of tetrazolium solutions for quality evaluation of Butterfly pea seed. Seeds collected in Seropédica county (RJ) e Fortaleza county (CE) were submitted to the following methods of pre-conditioning: a) scarification with sandpaper and immersion in water at 25°C for 14 hours; and b) immersion in water at 95°C and left in the same water to rest without heating for 24 hours at 25°C. The teguments of the seeds were removed and the seeds were immerged in 0,1; 0,3 e 1% tetrazolium solution during 2 hours and 30 minutes at 25°C. To verify the reliability of the results through the tetrazolium test, germination test, first counting and index of germination velocity were done. Scarification with sadpaper and immersion in water at 25°C for 14 hours were the most efficient in pre-conditioning Butterfly pea seeds and 0,3% tetrazolium solution for 2 hours and 30 minutes at 25°C allow evaluating seeds of this species. [ABSTRACT FROM AUTHOR]

Published
2009
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5. Synthesis and biological evaluation of chalcogen oxadiazoles and chalcogen tetrazoles

Author

Sauer, André Carpes, Dornelles, Luciano, Braga, Antonio Luiz, Fantinel, Leonardo, Ilha, Vinicius, and Rodrigues, Oscar Endrigo Dorneles

Subjects
Oxadiazoles, Organochalcogens, Tetrazóis, CIENCIAS EXATAS E DA TERRA::QUIMICA [CNPQ], Tetrazoles, Oxadiazóis, Organocalcogênios
Abstract

This work first describes the synthesis of the starting materials, the 1,2,4- and 1,3,4-oxadiazoles, from arylamidoximes and arylhydrazides derivatives, respectively. These two precursors were previously reacted with the 2-chloroacetyl chloride, and after cyclodehydration formed the desired heterocycles in satisfactory yields (10 examples, 67-99 %). The heterocyclic starting materials were submitted to aliphatic nucleophilic substitution reactions (SN2) against calcogenolates derived from arylic and alkylic disselenides and thiols. The selenolates were obtained in reducing medium of NaBH4 and anhydrous ethanol, whereas the thiolates were formed by treatment of thiols in basic medium of Et3N, so that the products from these substitutions were obtained in good yields (41 examples, 25-99 %). Some aspects of the methodologies employed were also studied, and some statements are possible, because when using tellurium don’t occurred the formation of the desired products, and also the formation of by-products unwanted. Secondly, the heterocyclic starting materials were re-subsumed to the SN2 reactions, but now, against potassium chalcogenocyanates (KSCN and KSeCN) in acetonitrile and the presence of an ammonium salt (TBAB), which aimed to catalyze reactions of aliphatic substitutions. The molecules from these reactions were obtained in excellent yields (12 examples, 69-92 %), which were subsequently submitted to the cycloaddition reactions (3+2) with NaN3, in a solution of toluene and Et3N.HCl, to form the respective 1H-tetrazoles (12 examples, 49-99 %). The products obtained contain, in the same molecule, the oxadiazolic, tetrazolic and chalcogen core. Chalcogencyanates and tetrazoles were further evaluated in vitro for their antioxidant properties by reducing the DPPH radical and Mo (VI) to Mo (V), so that two chalcogencyanates and one tetrazole presented good results for the phosphomolibidenium test. The cyclic voltammetry technique was also used to evaluate the redox potential of these compounds. Some compounds obtained in the first stage of this work are under evaluation of their antioxidant properties, but preliminary tests presented promising results for the molecules in question. Este trabalho descreve, inicialmente, a síntese dos materiais de partida, os 1,2,4- e 1,3,4-oxadiazóis, derivados de arilamidoximas e arilhidrazidas, respectivamente. Estes dois precursores reagiram previamente com o cloreto de 2-cloroacetila e após ciclodesidratação formaram os heterociclos desejados em rendimentos satisfatórios (10 exemplos, 67-99%). Os materiais de partida heterocíclicos foram submetidos às reações de substituição nucleofílica alifática (SN2) frente aos calcogenolatos derivados de disselenetos e tióis arílicos e alquílicos. Os selenolatos foram obtidos em meio redutor de NaBH4 e etanol anidro, já os tiolatos formam-se pelo tratamento de tióis em meio básico de Et3N, de modo que os produtos provenientes destas substituições foram obtidos em bons rendimentos (41 exemplos, 25-99%). Foram ainda, estudados alguns aspectos das metodologias empregadas, e algumas afirmações são possíveis, pois quando se utilizaram reagentes de telúrio não ocorreu a formação dos produtos desejados, e ainda se constatando a formação de subprodutos indesejados. Em um segundo momento, os materiais de partida heterocíclicos foram submetidos novamente às reações SN2, porém agora frente à calcogenocianatos de potássio (KSCN e KSeCN), em acetonitrila e na presença de um sal de amônio (TBAB), que teve como finalidade catalisar as reações de substituições alifáticas. As moléculas provenientes destas reações foram obtidas em excelentes rendimentos (12 exemplos, 69-92%), sendo que estes foram posteriormente submetidos às reações de cicloadição (3+2) com NaN3, em uma solução de tolueno e Et3N.HCl, formando os respectivos 1H-tetrazóis (12 exemplos, 49-99%). Os produtos obtidos contêm, em uma mesma molécula, os núcleos oxadiazólico, tetrazólico e calcogênio. Os calcogenocianatos e os tetrazóis foram ainda submetidos à avaliação de suas propriedades antioxidantes in vitro, por meio da redução do radical DPPH e do Mo (VI) à Mo (V), de forma que dentre os compostos avaliados, dois calcogenocianatos e um tetrazol exibiram bons resultados para o teste de fosfomolibidênio. Foi ainda utilizada a técnica de voltametria cíclica com o intuito de avaliar o potencial redox desses compostos. Alguns compostos obtidos, na primeira etapa deste trabalho, estão sob avaliação de suas propriedades antioxidantes, porém testes preliminares apresentaram resultados promissores para as moléculas em questão.

Published
2017

7. Maximal Oxygen Uptake and Ventilation Improvement Following Sacubitril-Valsartan Therapy.

Author

Gonçalves AV, Pereira-da-Silva T, Galrinho A, Rio P, Soares R, Feliciano J, Moreira RI, Silva S, Alves S, Capilé E, and Ferreira RC

Subjects
Aged, Aminobutyrates, Angiotensin Receptor Antagonists, Biphenyl Compounds, Drug Combinations, Humans, Middle Aged, Oxygen, Prospective Studies, Stroke Volume, Tetrazoles, Treatment Outcome, Valsartan, Heart Failure drug therapy, Ventricular Function, Left
Abstract

Background: Sacubitril/valsartan had its prognosis benefit confirmed in the PARADIGM-HF trial. However, data on cardiopulmonary exercise testing (CPET) changes with sacubitril-valsartan therapy are scarce., Objective: This study aimed to compare CPET parameters before and after sacubitril-valsartan therapy., Methods: Prospective evaluation of chronic heart failure (HF) patients with left ventricular ejection fraction ≤40% despite optimized standard of care therapy, who started sacubitril-valsartan therapy, expecting no additional HF treatment. CPET data were gathered in the week before and 6 months after sacubitril-valsartan therapy. Statistical differences with a p-value <0.05 were considered significant., Results: Out of 42 patients, 35 (83.3%) completed the 6-month follow-up, since 2 (4.8%) patients died and 5 (11.9%) discontinued treatment for adverse events. Mean age was 58.6±11.1 years. New York Heart Association class improved in 26 (74.3%) patients. Maximal oxygen uptake (VO2max) (14.4 vs. 18.3 ml/kg/min, p<0.001), VE/VCO2slope (36.7 vs. 31.1, p<0.001), and exercise duration (487.8 vs. 640.3 sec, p<0.001) also improved with sacubitril-valsartan. Benefit was maintained even with the 24/26 mg dose (13.5 vs. 19.2 ml/kg/min, p=0.018) of sacubitril-valsartan, as long as this was the highest tolerated dose., Conclusions: Sacubitril-valsartan therapy is associated with marked CPET improvement in VO2max, VE/VCO2slope, and exercise duration. (Arq Bras Cardiol. 2020; [online].ahead print, PP.0-0).

Published
2020
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10. The historical evolution of knowledge of the involvement of neurohormonal systems in the pathophysiology and treatment of heart failure.

Author

Polónia J and Gonçalves FR

Subjects
Aminobutyrates, Angiotensin Receptor Antagonists, Biphenyl Compounds, Drug Combinations, Humans, Tetrazoles, Valsartan, Vasopressins, Heart Failure, Neurosecretory Systems, Renin-Angiotensin System, Sympathetic Nervous System
Abstract

Our knowledge of the pathophysiology of heart failure (HF) underwent profound changes during the 1980s. Once thought to be of exclusively structural origin, HF began to be seen as the consequence of hormonal imbalance. A number of seminal studies were published in that decade focusing on the impact of neurohormonal activation in HF. Presently, eight neurohormonal systems are known to have a key role in HF development: four stimulate vasoconstriction and sodium/water retention (the sympathetic nervous system, the renin-angiotensin-aldosterone system [RAAS], endothelin, and the vasopressin-arginine system), while the other four stimulate vasodilation and natriuresis (the prostaglandin system, nitric oxide, the dopaminergic system, and the natriuretic peptide system [NPS]). These systems are strongly interconnected and are subject to intricate regulation, functioning together in a delicate homeostasis. Disruption of this homeostasis is characteristic of HF. This review explores the historical development of knowledge on the impact of the neurohormonal systems on HF pathophysiology, from the first studies to current understanding. In addition, the therapeutic potential of each of these systems is discussed, and currently used neurohormonal antagonists are characterized. Special emphasis is given to the latest drug approved for use in HF with reduced ejection fraction, sacubitril/valsartan. This drug combines two different molecules, acting on two different systems (RAAS and NPS) simultaneously., (Copyright © 2019 Sociedade Portuguesa de Cardiologia. Publicado por Elsevier España, S.L.U. All rights reserved.)

Published
2019
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11. N-glycosylation of 5-(1-(3-fluorophenyl)-1H-pyrazol-4-yl)-1H-tetrazole catalyzed by free and immobilized fungal cells of Cunninghamella echinulata ATCC 9244

Author

Souza, Paula Letícia de Melo, Oliveira, Valéria de, Oliveira, Brás Heleno de, and Pazini, Francine

Subjects
Biotransformação, N-glicosilação, Tetrazóis, Tetrazoles, N-glycosylation, Cunninghamella echinulata, Biotransformation, FARMACIA [CIENCIAS DA SAUDE]
Abstract

As biotransformações são ferramentas poderosas para otimização de compostos ativos, modificação e diversificação estrutural, além da manipulação de compostos não-funcionalizados inviável por métodos químicos tradicionais. A versatilidade dos sistemas microbiano, nesse contexto, e as inúmeras vantagens atribuídas aos fungos filamentosos alavancaram o uso das biotransformações com microorganismos. As glicosilações são um dos mais importantes e comuns processos de modificação e o uso de biocatalisadores tem configurado uma estratégia favorável a esse tipo de reação. Espécies de Cunninghamella, por seu arsenal enzimático, são extensamente aplicadas, principalmente por viabilizarem a produção de novos derivados de fármacos e a imobilização celular é evidenciada como uma estratégia para expressar essa atividade enzimática. Frente à relevância dos aminoaçúcares e seu enorme potencial terapêutico, o objetivo deste estudo foi produzir derivados do 5-(1-(3-fluorofenil)-1H-pirazol-4-il)-1H-tetrazol (LQFM 021), que contém anéis tetrazólico e pirazólico, a partir da biotransformação por células fúngicas livres e imobilizadas de Cunninghamella echinulata ATCC 9244. Para tanto, foram desenvolvidas metodologias para análise da cinética de biotransformação do LQFM 021, bem como empregadas técnicas de caracterização (Ressonância Magnética Nuclear (RMN) e Espectrometria de Massas com Ressonância Ciclotrônica de Íons (FTICR-MS) do produto obtido. Foram realizadas incubações de 96 horas com células livres de Cunninghamella echinulata ATCC 9244, em meio de cultura PDSM e com células imobilizadas em três experimentos distintos: biofilme incubado em tampão PBS, biofilme incubado em meio de cultura PDSM e reutilização dos biofilmes, em que foi obtido um derivado do LQFM 021.A proposta estrutural para o derivado obtido, purificado em quantidades suficientes, é de um 1-(5-(1-(3-fluorofenil)-1H-pirazol-4-il)-2H-tetrazol-2-il)pentano-1,2,3,4,5-pentaol. Biotransformations are powerful tools for optimization of active compounds, diversification and structural modifications, in addition to handling non-functionalized compounds unfeasible by chemical conventional methods. The versatility of microbial systems, in this context, and the numerous entitlements of filamentous fungi have leveraged the use of biotransformations with microorganisms. Glycosylations ate one of the most important and commom modification processes and the use of biocatalysts have set a favorable strategy to this type of reaction. Cunninghamella species, for its enzimatic arsenal, are widely applied, especially for enabling the production of novel drug and cell immobilization hás been evidenced as a tool to express its enzimatic activity.Considering the relevance of amino sugars and their enormous potential in various therapies, the aim of this study was to produce 5-(1-(3-fluorophenyl)-1H-pyrazol-4-yl)-1H-tetrazole (LQFM 021) derivatives, which contains tetrazole and pyrazole rings, by biotransformation with free and immobilized fungi cells of Cunninghamella echinulata ATCC 9244. Therefore, CLAE methodologies were developed for the analysis of biotransformation kinectics and characterization techniques employed (Nuclear Magnetic Resonance (NMR) and Mass Spectrometry with Ion cyclotron Resonance (FTICR-MS)) of the product. 96-hour incubations were proceeded with free cell Cunninghamella echinulata ATCC 9244, in the PDSM culture medium and immobilized cells in three separate experiments: biofilm incubated in PBS buffer, biofilm incubated in PDSM medium culture and reuse of biofilms, where one derivative was obtained. The structural characterization for the purified derivative obtained in sufficient quantities is a 1-(5-(1-(3-fluorophenyl)-1H-pyrazol-4-yl)-2H-tetrazol-2-yl)pentane-1,2,3,4,5-pentaol. Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES

Published
2015

13. Olmesartan decreases IL-1β and TNF-α levels; downregulates MMP-2, MMP-9, COX-2, and RANKL; and upregulates OPG in experimental periodontitis

Author

Karoline S. Aragão, Graziene Lopes de Souza, Maria do Socorro Costa Feitosa Alves, Raimundo Fernandes de Araújo, Yriu Lourenço, Tatiana Oliveira Souza, Aurigena Antunes de Araújo, Gerly Anne de Castro Brito, and Caroline Addison Carvalho Xavier de Medeiros

Subjects
musculoskeletal diseases, Male, medicine.medical_specialty, Interleukin-1beta, Alveolar Bone Loss, Anti-Inflammatory Agents, Gingiva, Tetrazoles, Osteoprotegerin, Internal medicine, Malondialdehyde, medicine, Animals, Immunohistochemical, Olmesartan, Rats, Wistar, Lipid peroxidant, Receptor, Periodontitis, Peroxidase, Pharmacology, biology, Receptor Activator of Nuclear Factor-kappa B, Chemistry, Tumor Necrosis Factor-alpha, RANK Ligand, Imidazoles, Interleukin, General Medicine, Angiotensin II, Rats, Endocrinology, Matrix Metalloproteinase 9, Experimental periodontal disease, RANKL, Cyclooxygenase 2, Myeloperoxidase, Citocines, biology.protein, Matrix Metalloproteinase 2, Tumor necrosis factor alpha, medicine.drug
Abstract

The objective of this study is to investigate the participation of inflammatory and oxidative stress mediators and the effects on the expression of matrix metalloproteinase (MMP)-2, MMP-9, and receptor activator of NF-κB ligand (RANKL)/receptor activator of NF-κB (RANK)/osteoprotegerin (OPG) pathway in the response to treatment with olmesartan, an angiotensin II type 1 receptor blocker. Male Wistar albino rats were randomly divided into five groups of ten rats each: (1) non-ligature with water, (2) ligature with water, (3) ligature with 1 mg/kg olmesartan, (4) ligature with 6 mg/kg olmesartan, and (5) ligature with 10 mg/kg olmesartan. All groups were treated with olmesartan or the vehicle by gavage daily for 10 days. Following the treatment course, the periodontal tissue of the animals was analyzed by histopathology and immunohistochemistry to determine the expression of cyclooxygenase-2 (COX-2), MMP-2, MMP-9, and members of the RANKL/RANK/OPG pathway and by ELISA and spectroscopic assay to determine the levels of interleukin (IL)-1β, IL-10, tumor necrosis factor (TNF)-α, myeloperoxidase (MPO), malonaldehyde (MDA), and glutathione. The concentrations of MPO and MDA were reduced in the group that received 6 mg/kg olmesartan (p

Published
2013

14. Design, synthesis and pharmacological profile of new lead compounds of vasorelaxant drugs

Author

Pazini, Francine, Lião, Luciano Morais, Menegatti, Ricardo, Barreiro, Eliezer de Jesus, Pinto, Angelo da Cunha, Ghedini, Paulo César, Oliveira, Cecília Maria Alves de, and Queiroz Junior, Luiz Henrique Keng

Subjects
Pirazóis, Ressonância magnética nuclear, Tetrazóis, Pyrazoles, Tetrazoles, Heterocycles, Anéis heterocíclicos, Nuclear magnetic resonance, FOTOQUIMICA ORGANICA [QUIMICA ORGANICA]
Abstract

As doenças cardiovasculares são a principal causa de morte no mundo, logo a busca de candidatos a protótipos de fármacos cardiotônicos que sejam mais efetivos, seguros e que apresentem menos efeitos colaterais quando comparados aos já disponíveis na terapêutica, é de fundamental importância. Neste contexto, foram empregados em nosso planejamento os protótipos inibidores de fosfodiesterase 3, milrinona (13) e cilostazol (4), que mostram atividade inotrópica e efeito vasodilatador. Os novos compostos heterociclos 5-(1-fenil-1H-pirazola-4-il)-2H-tetrazolas (20a-20o) foram originalmente desenhados através da estratégia de hibridação molecular a partir destes protótipos. A rota sintética eleita, composta por quatro etapas, para a obtenção dos compostos 5-(1- fenil-1H-pirazola-4-il)-2H-tetrazolas (20a-20o) resultou em rendimentos globais que variaram entre 16 e 73%. Inicialmente ocorreu uma reação de condensação entre as fenilhidrazinas 14a- 14o e 1,1,3,3 tetrametoxipropano, catalisada por ácido clorídrico, com formação dos intermediários 1-fenil-1H-pirazolas (16a-16o). Na sequência, os compostos 16a-16o foram submetidos a uma reação de formilação quimio e regioespecífica na posição 4 do anel pirazola. Os intermediários 1-fenil-1H-pirazola-4-carbaldeído (18a-18o) foram então submetidos a uma reação de condensação com cloridrato de hidroxilamina que desidratou in sito na presença de iodeto de potássio aos intermediários 1-fenil-1H-pirazola-4-carbonitrilas (19a-19o). Ao final, os compostos 19a-19o, através de um processo de cicloadição 1,3 bipolar, reagiram com azida de sódio formando os compostos desejados 20a-20o. A utilização das condições da reação Duff para a formilação de N-fenilpirazóis (1-fenil- 1H-pirazol) (9a-o), se mostrou uma metodologia sintética alternativa às condições clássicas de Vilsmeier-Haack. Todos os compostos sintetizados tiveram suas estruturas químicas elucidadas através das espectroscopias na região do infravermelho e ressonância magnética nuclear de 1H, 13C, HSQC e HMBC. Os compostos 5-[1-(4-fluorfenil)-1H-pirazola-4-il]-2H-tetrazola (20c), 5-[1-(3- fluorfenil)-1H-pirazola-4-il]-2H-tetrazola (20d), 5-[1-(4-clorofenil)-1H-pirazola-4-il]-2Htetrazola (20e), 5-[1-(3-nitrofenil)-1H-pirazola-4-il]-2H-tetrazola (20f) e 5-[1-(3-clorofenil)-1H-pirazola-4-il]-2H-tetrazola (20g), foram avaliados quanto ao seu perfil de relaxamento do músculo liso vascular. A partir deste ensaio preliminar, o composto 5-[1-(3-fluorfenil)-1Hpirazola- 4-il]-2H-tetrazola (20d) foi selecionado para ser avaliado em modelos farmacológicos complementares, uma vez que apresentou melhor perfil de relaxamento dentre esta série de compostos, a fim de investigar seu mecanismo de ação. Nestes ensaios, o composto 20d mostrou uma ação relaxante em artérias isoladas, potencializada pelo endotélio, com participação das vias GCs/GMPc e AC/AMPc e onde os fluxos de K+ e Ca2+ através da membrana e a captação de Ca2+ pelo retículo sarcoplasmático são importantes. Face ao perfil farmacológico promissor do composto 5-[1-(3-fluorfenil)-1H-pirazola-4- il]-2H-tetrazola (20d), o mesmo foi submetido aos ensaios de segurança pré-clínica no modelo in vitro de incorporação do vermelho neutro com culturas de células 3T3 e a toxicidade oral aguda em modelo in vivo. Segundo o protocolo internacional Organization for Economic Cooperation and Development (OECD) 423 o composto 20d foi classificado na classe 4, que mostra que o composto foi bem tolerado na dose de 2000 mg/kg por via oral. Ao término deste trabalho, podemos concluir que a estratégia de planejamento empregada no mesmo foi validada, uma vez que o composto 5-[1-(3-fluorfenil)-1H-pirazola- 4-il]-2H-tetrazola (20d) apresentou um perfil farmacológico vasodilatador com prováveis ações cardioativas. A avaliação farmacológica completa, incluindo experimentos com a enzima fosfodiesterase 3, de todos os compostos sintetizados neste trabalho servirá de guia para se estabelecer a relação estrutura atividade da série, e por sua vez, conduzir as futuras modificações sobre as estruturas químicas dos compostos visando à otimização da atividade cardiotônica. Cardiovascular diseases are the leading cause of death worldwide, so the search for cardiotonic drugs more effective, safer and with lower side effects compared to currently available therapy, is of fundamental importance. Thus, we used in our design the phosphodiesterase 3 inhibitors, milrinone (13) and cilostazol (4), which show positive inotropic activity, relaxation effect and vasodilators. The new heterocyclic compounds (20a-20o) were originally designed by applying molecular hybridization strategy from these lead-compounds. The synthetic route to obtain the compounds 20a-20o resulted in overall yields ranging from 16.2 and 73.4%. During the synthesis, we used the Duff reaction conditions to formylation of N-phenylpyrazoles (1-phenyl-1H-pyrazole) (9a-o), which was an alternative synthetic methodology to classic Vilsmeier-Haack conditions. All the synthesized compounds were characterized by infrared and NMR spectroscopy combining the 1H, 13C, HSQC and HMBC correlation spectra. The compounds 20c, 20d, 20e, 20f and 20g, were evaluated for their relaxation profile of vascular smooth muscle. From this preliminary test, the 20d compound was selected to be further evaluated in pharmacological models, as provided better relaxation among this series of compounds in order to investigate the action mechanism. In these assays, 20d compound showed a relaxing activity in isolated arteries, potentiate by the presence of endothelium, with the participation of routes GCs/GMPc and AC/AMPc and where the flows of K+ and Ca2+through the membrane and the uptake of Ca2+ by the sarcoplasmic reticulum are important. Given the promising pharmacological profile of 20d compound, it was subjected to safety testing in preclinical in vitro model of the neutral red incorporation by cultures of 3T3 cells and acute oral toxicity tests. According to the International Organization for Economic Cooperation and Development (OECD) 423, the 20d compound was classified in 4 class, which shows that the compound was tolerated at a dose of 2000mg/kg orally. At the end of this work, we conclude that the design strategy employed has been validated, as the 20d compound showed a similar pharmacological profile to lead-compounds milrinone (13) and cilostazol (4). The pharmacological evaluation of all synthesized compounds in this work, will serve as a guide to establish the structure activity relationship of the series, and in turn, lead future changes on the chemical structures of the compounds for the activity cardiotonic optimization.

Published
2012

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