Can a horse learn while under the influence of a tranquilizer (Acepromazine maleate)

Griffith, Samantha C., McCall, Cynthia Ann.

January 2006

Thesis(M.S.)--Auburn University, 2006. / Abstract. Vita. Includes bibliographic references.

Untersuchung der einstufigen Gasphasenhydrierung von Dimethylmaleat zur Herstellung von g-Butyrolacton, 1,4-Butandiol und Tetrahydrofuran

Ohlinger, Christoph.

January 2005

Universiẗat, Diss., 2005--Karlsruhe.

Pharmacokinetic and Bioequivalence Evaluation of Two Formulations of 100 mg Trimebutine Maleate (Recutin™ and Polybutin™) in Healthy Male Volunteers Using the LC-MS/MS Method

Jhee, Ok Hwa, Lee, Yun Sik, Shaw, Leslie M., Jeon, Yong Cheol, Lee, Min Ho, Lee, Seung Hoon, Kang, Ju Seop

01 January 2007

Background: Trimebutine maleate is a prokinetic agent that acts directly on the smooth muscle of the GI tract. A bioequivalence (BE) study of 2 oral formulations of 100 mg trimebutine maleate (TMB) was carried out in 24 healthy male Korean volunteers according to a crossover-randomized design. Methods: Subjects were given a single dose of 2 100 mg tablets of each formulation. The test and reference formulations were Recutin™ (Hutax Co., South Korea) and Polybutin™ (Samil Co., South Korea), respectively. Each set of tablets was administered with 240 ml of water to subjects after 10 h overnight fasting on 2 treatment days separated by a 1 week washout period. After dosing, serial blood samples were collected for a period of 36 h. Plasma was analyzed for the main metabolite of TMB, N-monodesmethyl trimebutine (nor-TMB), by a validated LC with MS/MS detection capacity for nor-TMB in the range 5-1500 ng/ml, with a lower limit of quantification (LLOQ) of 5 ng/ml. Several pharmacokinetic (PK) parameters (including AUCt, AUCinfinity, Cmax, Tmax, T1/2, and Ke) were determined from the plasma concentrations of nor-TMB of both formulations. AUCt, AUCinfinity, and Cmax were tested for BE after log-transformation of the data. Results: No significant difference was found based on ANOVA; 90% confidence intervals (98.98%112.03% for AUCt; 98.60%-113.20% for AUCinfinity; 90.85%-107.87% for Cmax) for the test and reference were found within KFDA acceptance range of 80-125%. Conclusions: Based on these statistical inferences, it was concluded that Recutin™ is bioequivalent to Polybutin™ and can be used interchangeably in a clinical setting.

bioequivalence test

N-monodesmethyl trimebutine

pharmacokinetics

trimebutine maleate

Perioperative Administration of Topical Dorzolamide Hydrochloride/Timolol Maleate Reduces Postoperative Ocular Hypertension in Dogs Undergoing Cataract Surgery

Matusow, Rachel Brodman

15 May 2015

Development of cataracts is a relatively frequent ocular disease of the dog and cataract extraction via phacoemulsification (PE) is commonly performed by veterinary ophthalmologists. Postoperative ocular hypertension (POH) describes the elevation of pressures within the eye during the acute postoperative period and can result in vision loss and poor surgical outcome. Relatively little is known about risk factors or efficacy of prophylactic treatment for POH, and current clinical practice with regard to pressure monitoring and medication administration are highly variable. The literature on POH prophylaxis in humans indicates that improved efficacy may be achieved with a multi-dose approach and that dorzolamide hydrochloride/timolol maleate (DHTM) may be more efficacious than other pressure lowering medications. The canine literature on POH prophylaxis is limited and DHTM has not yet been evaluated despite common use in the clinical setting. Our objectives, therefore, were to investigate risk factors for POH and to test the hypothesis that perioperative topical ophthalmic dorzolamide hydrochloride 2%/timolol maleate 0.5% (DHTM) reduces the prevalence and/or severity of postoperative ocular hypertension (POH) in dogs undergoing cataract extraction by phacoemulsification (PE). We employed a randomized double-masked placebo-controlled study and enrolled 103 dogs (180 eyes) presenting for unilateral or bilateral PE. Select historical, signalment, ophthalmic examination, and surgical data was collected. Dogs were treated with DHTM or Blink Contacts (BC) placebo at 14- and 2-h preoperatively and at conclusion of surgical closure. Intraocular pressures were assessed by rebound tonometry at 2, 4, 6, and 8 hours after surgery and at 8 am the following morning. POH was defined as IOP>25 mmHg and intervention consisted of latanoprost 0.005% if IOP rose to 26 mmHg - 45 mmHg or surgeon treatment of choice if >45 mmHg. Our investigation of risk factors yielded a statistically significant association only with surgeon and surgical time, which were also associated with one another. DHTM significantly reduced the prevalence of POH in comparison with BC (26% versus 49% of eyes, OR=0.36; 34% versus 62% of dogs, OR=0.32). There was also a trend toward reduction of POH severity in DHTM-treated eyes (POH value 37.17±10.47 mmHg with BC, 32.67±6.39 mmHg with DHTM). DHTM-treated eyes that developed POH were significantly more likely to respond favorably (1 hour post-treatment IOP <25 mmHg) to treatment with latanoprost than those in the BC group (76% versus 51%, OR=3.87). We conclude that multi-dose perioperative administration of DHTM may be recommended in dogs undergoing PE to reduce the risk of POH and improve responsiveness of POH to treatment with latanoprost. / Master of Science

Cataracts

Phacoemulsification

Dog

Postoperative Ocular Hypertension

Evaluation des différentes approches pour l'estimation de l'incertitude des mesures analytiques

Marini Djang'Eing'A, Roland

19 April 2006

=RESUME= Trois approches différentes ont été comparées pour lestimation de lincertitude de mesure, à savoir celles basées sur des études inter-laboratoire, sur la robustesse et sur la validation. Pour ce faire, deux techniques analytiques séparatives, la chromatographie liquide haute performance (CLHP) et lélectrophorèse capillaire (EC), ont été utilisées pour la détermination de lénantiomère R-timolol dans des échantillons de maléate de S-timolol. Loptimisation de la méthode de CLHP a été effectuée sur une phase chirale à base de cellulose modifiée selon une approche multivariée. En ce qui concerne lEC, une séparation chirale convenable a été obtenue en milieu non aqueux en utilisant de lheptakis(2,3-di-O-méthyl-6-O-sulfo)-β-cyclodextrine comme sélecteur chiral en combinaison avec le camphosulfonate. Les deux méthodes ont été validées pour lusage prédéfini en appliquant la stratégie du profil dexactitude, ce qui a permis également destimer lincertitude de mesure. Par la suite, un test de robustesse a été effectué pour les deux méthodes. Linfluence des paramètres opératoires a été évaluée en considérant non seulement les réponses qualitatives mais surtout les réponses quantitatives. Les résultats de ces dernières (teneurs en R-timolol) ont servi à lestimation de lincertitude de mesure, selon le guide ISO 5725-2. Ce même guide a été utilisé pour évaluer la reproductibilité des résultats obtenus lors des études inter-laboratoire menées avec les deux méthodes. Lincertitude estimée à partir de la reproductibilité, a été trouvée dépendante de la concentration, comme observé également lors des études de validation et de robustesse. Il apparaît que lincertitude obtenue en robustesse prédit très bien celle obtenue en inter-laboratoire et constitue donc une alternative intéressante à cette dernière. Par contre, lincertitude associée à la validation est quant à elle différente de celle des autres approches. Cependant, elle reste parfaitement valable pour autant que le protocole de validation soit en accord avec la routine et que la méthode ne quitte pas le laboratoire qui la validée. Lors de la comparaison des deux méthodes, lincertitude obtenue en CLHP a été trouvée plus faible que celle obtenue en EC. =SUMMARY= Three different approaches (inter-laboratory, robustness and validation) have been applied to the estimation of uncertainty and compared. For that purpose, two analytical separation techniques, namely high performance chromatography liquid (HPLC) and capillary electrophoresis (CE), have been used for the determination of R-timolol enantiomer in S-timolol maleate samples. The optimisation of the HPLC method was carried out on a chiral stationary phase containing modified cellulose, by applying a multivariate approach. Concerning the CE method, a suitable chiral separation was obtained in a nonaqueous medium using heptakis(2,3-di-O-méthyl-6-O-sulfo)-β-cyclodextrin as chiral selector in combination with camphorsulfonate. The two methods were validated for the intended use by applying the strategy of the accuracy profile, which could be used additionally to estimate the uncertainty of measurement. Then, a robustness test was performed for the two methods. The influence of the operating parameters was assessed considering not only the qualitative responses but mainly the quantitative ones (the R-timolol content). The latter were used to estimate the uncertainty of measurement according to the ISO 5725-2 guide. The same guide was applied to evaluate the reproducibility of results obtained in inter-laboratory studies carried out with the two methods. The uncertainty was found to be concentration dependent, as also observed in validation and in robustness studies. The uncertainty obtained by robustness studies predicts well that obtained in inter-laboratory studies and can be proposed as an alternative to the latter. On the other hand, the estimation of uncertainty obtained with the validation studies leads to lower values than those obtained with the two other approaches but is still acceptable as long as the analytical method is used in a single laboratory. When comparing the two analytical methods, the uncertainty obtained in LC was found to be lower than that obtained in CE.

chiral separation/separation chirale

HPLC/CLHP

timolol maleate/maleate de timolol

validation/validation

CE/EC

robustness/robustesse

uncertainty/incertitude.

Fabrication of polymeric microfluidic devices via photocurable liquid monomers

Haraldsson, Klas Tommy

January 2005

Microfluidic devices have long been considered an ideal tool for rapid and inexpensive chemical analysis and reactions in areas ranging from point-of-care health to national security applications. However, fabricating microfluidic devices is time consuming, difficult and above all expensive. In commercial applications many thousand units need to be sold before the development costs are recovered. The problem is compounded since most microfluidic devices do not have generalized architectures which means that each end use requires a specialized design. The microfluidics marketplace can therefore be seen as being composed of 1000’s of niche markets. To address development costs, there is clearly a need for a versatile technology that can be used for many different applications and that enables rapid testing and optimization of new designs. This work describes such a technology: Contact Liquid Photolithographic Polymerization (CLiPP). The thesis consists of two parts: polymerization kinetics and the fabrication of polymeric microfluidic devices via CLiPP. The photopolymerization kinetics is evaluated for a number of monomer types, and the results are used to assess their suitability in the CLiPP process. Vinyl ether/maleate photoinitiated copolymerization is examined in detail. It is shown that the polymerization kinetics is dramatically influenced by the availability of easily abstractable hydrogens The presence of α-hydrogens adjacent to the vinyl ether functional group reduces the polymerization rate and the dependence of the polymerization rate as a function of initiation rate. Also, photoinitiated acrylate and methacrylate polymerization kinetics are presented. The kinetics results in these three monomer types are used to explain the different patterning properties of the monomer functionalities used in the CLiPP process, in which acrylates show enhanced patterning properties compared to methacrylates. The polymerization kinetics is studied with traditional tools and methods: photo Differential Scanning Calorimetry (photo-DSC), photo Fourier Transform Real Time Infrared Spectroscopy (photo-RTIR), and photo Real Time Electron Paramagnetic Spectroscopy (ESR). The microfluidic fabrication is performed via both in-house fabricated and commercially available CLiPP-specific hardware. The patterning qualities of the structures are evaluated via Scanning Electron Microscopy (SEM) and Optical Microscopy. The finished devices are used in their intended environment and evaluated in suitable manners to assess their utility. In this thesis, the development and design of specialized CLiPP fabrication machines, fabrication techniques and resulting microfluidic device features are presented anddiscussed. It is shown that the CLiPP scheme enables features such as 3 dimensional (3D) capabilities for minimized device footprints, a very large number of polymeric materials for optimized device components as well as facile integration of prefabricated components. Also, covalent layer adhesion and permanent surface modifications via living radical processes are demonstrated. These capabilities are exemplified in a number of examples that range from a 3D fluidic channel maze with separated fluidic streams and a device with independently moveable parts to a device constructed from multiple polymeric materials and devices with permanently modified surfaces, Also, batch processing capabilities are shown through fabrication of 400 identical undercut microstructures. Rapid and inexpensive design evaluations, multiple materials capabilities and the ability to seamlessly incorporate prefabricated microstructures of the CLiPP process strongly encourages continued method development. The future work that remains to be addressed is divided into two parts. First, to enable novel research devices, new polymer materials with enhanced mechanical and surface properties must be developed. Also, integration of prefabricated microstructures such as sensors and actuators has to be incorporated in a reproducible and rational manner. Secondly, to enable device mass fabrication, new automated equipment is to be developed in order to utilize the full batch processing potential of CLiPP. / QC 20101019

Photopolymerization

radical photopolymerization

polymerization kinetics

photoinitiation

vinyl ether

maleate

vinyloxy

Polymer chemistry

Polymerkemi

Fabrication of polymeric microfluidic devices via photocurable liquid monomers

Haraldsson, Klas Tommy

January 2005

<p>Microfluidic devices have long been considered an ideal tool for rapid and inexpensive chemical analysis and reactions in areas ranging from point-of-care health to national security applications. However, fabricating microfluidic devices is time consuming, difficult and above all expensive. In commercial applications many thousand units need to be sold before the development costs are recovered. The problem is compounded since most microfluidic devices do not have generalized architectures which means that each end use requires a specialized design. The microfluidics marketplace can therefore be seen as being composed of 1000’s of niche markets.</p><p>To address development costs, there is clearly a need for a versatile technology that can be used for many different applications and that enables rapid testing and optimization of new designs. This work describes such a technology: Contact Liquid Photolithographic Polymerization (CLiPP).</p><p>The thesis consists of two parts: polymerization kinetics and the fabrication of polymeric microfluidic devices via CLiPP.</p><p>The photopolymerization kinetics is evaluated for a number of monomer types, and the results are used to assess their suitability in the CLiPP process. Vinyl ether/maleate photoinitiated copolymerization is examined in detail. It is shown that the polymerization kinetics is dramatically influenced by the availability of easily abstractable hydrogens The presence of α-hydrogens adjacent to the vinyl ether functional group reduces the polymerization rate and the dependence of the polymerization rate as a function of initiation rate. Also, photoinitiated acrylate and methacrylate polymerization kinetics are presented. The kinetics results in these three monomer types are used to explain the different patterning properties of the monomer functionalities used in the CLiPP process, in which acrylates show enhanced patterning properties compared to methacrylates. The polymerization kinetics is studied with traditional tools and methods: photo Differential Scanning Calorimetry (photo-DSC), photo Fourier Transform Real Time Infrared Spectroscopy (photo-RTIR), and photo Real Time Electron Paramagnetic Spectroscopy (ESR).</p><p>The microfluidic fabrication is performed via both in-house fabricated and commercially available CLiPP-specific hardware. The patterning qualities of the structures are evaluated via Scanning Electron Microscopy (SEM) and Optical Microscopy. The finished devices are used in their intended environment and evaluated in suitable manners to assess their utility.</p><p>In this thesis, the development and design of specialized CLiPP fabrication machines, fabrication techniques and resulting microfluidic device features are presented anddiscussed. It is shown that the CLiPP scheme enables features such as 3 dimensional (3D) capabilities for minimized device footprints, a very large number of polymeric materials for optimized device components as well as facile integration of prefabricated components. Also, covalent layer adhesion and permanent surface modifications via living radical processes are demonstrated. These capabilities are exemplified in a number of examples that range from a 3D fluidic channel maze with separated fluidic streams and a device with independently moveable parts to a device constructed from multiple polymeric materials and devices with permanently modified surfaces, Also, batch processing capabilities are shown through fabrication of 400 identical undercut microstructures.</p><p>Rapid and inexpensive design evaluations, multiple materials capabilities and the ability to seamlessly incorporate prefabricated microstructures of the CLiPP process strongly encourages continued method development. The future work that remains to be addressed is divided into two parts. First, to enable novel research devices, new polymer materials with enhanced mechanical and surface properties must be developed. Also, integration of prefabricated microstructures such as sensors and actuators has to be incorporated in a reproducible and rational manner. Secondly, to enable device mass fabrication, new automated equipment is to be developed in order to utilize the full batch processing potential of CLiPP.</p>

Photopolymerization

radical photopolymerization

polymerization kinetics

photoinitiation

vinyl ether

maleate

vinyloxy

Polymer chemistry

Polymerkemi

Role of Cu(I) complexes in the electrochemical reduction of glycinate and maleate Cu(II) complexes / Cu(I) kompleksų vaidmuo glicinatinių ir maleatinių Cu(II) kompleksų elektrocheminės redukcijos PROCESUOSE

Uljanionok, Julija

04 February 2010

A comparative investigation of electrochemical characteristics of two complex systems, viz. Cu|Cu(II), glycine and Cu|Cu(II), maleic acid, was carried out. The equations were obtained for quantitative description of pH-metric and spectrophotometric data, which were used for determination of equilibrium characteristics in Cu(II)-maleic acid solutions. Thermodynamic analysis shows that deep changes are possible in this system resulting in 90 % transform of Cu(II) into Cu(I). The rates of Cu corrosion and Cu2O formation are estimated to be of the same order (nmol cm-2 s-1). Regularities of formal electrochemical kinetics, which account for the mass transport of chemically interacting particles and for step-wise charge transfer process, are suitable for interpretation of voltammetric data of the Cu|Cu(II), glycine system. Kinetic parameters Cu(II) glycinate complex depend on the nature of the supporting electrolyte: the exchange current density decreases and the cathodic charge transfer coefficient increases in the sequence: Li+ - Na+ - K+ - Cs+. To enhance the Cu(I) generation in maleic acid system, the pre-electrolysis procedure was applied. It was found that its effect depends on solution pH. Applied theoretical model describes satisfactorily the steady-state voltammetric characteristics of Cu|Cu(II), maleic acid system, but some contradictory results were obtained in the case of time-dependent processes. Theoretical and experimental problems to be solved are discussed. / Atliktas palyginamasis dviejų kompleksinių sistemų - Cu|Cu(II), glicinas ir Cu|Cu(II), maleino rūgštis - elektrocheminių charakteristikų tyrimas. Nustatytos maleino rūgšties tirpalų pusiausvyrinės charakteristikos. Kiekybiniam titravimo kreivių aprašymui išvestos lygtys, kuriose įvertinti medžiagų bei krūvių balansai bei atsižvelgta į praskiedimo efektus. Jų taikymas pH-metrinių duomenų analizei davė tokias maleato anijonų protonizacijos konstantų reikšmes: log = 6,05, log = 7,48. Nustatyta, kad tirpaluose su 0,3 M K2SO4 priedu protonizuotų ligando formų stabilumas sumažėja (log = 5,75, log = 7,30). Cu(II) maleatinių kompleksų stabilumui nustatyti panaudotas spektrofotometrijos metodas ir pasiūlyta duomenų analizės procedūra. Ji remiasi kiekybiniu absorbcijos spektrų aprašymu, taikant lygtis, išplaukiančias iš valdomo harmoninio osciliatoriaus teorijos. Išanalizavus įvairių sudėčių tirpalų absorbcijos maksimumo dydžius, prieita išvados, kad rūgščiose terpėse vyrauja monoligandinis kompleksas, kurio koncentracinė stabilumo konstanta log b1 = 2,2. Atlikta sistemos Cu|Cu(II), maleino rūgštis pusiausvyrų termodinaminė analizė. Nustatyta, kad esant metalinio vario ir tirpalų sąlyčiui, sistemoje galimi gilūs virsmai, kurių metu iki 90 % Cu(II) transformuojasi į Cu(I). Teorines išvadas patvirtina eksperimentiniai duomenys, gauti spektrofotometrijos ir elektrocheminės kvarco kristalo mikrogravimetrijos metodais. Įvertinti Cu korozijos bei fazinių Cu2O sluoksnių susidarymo... [toliau žr. visą tekstą]

Chemistry

Cu (I) complexes

Glycinate

Maleate Cu (II) Complexes

Cu(I) Kompekslai

Maleatiniai

Glicinatiniai Cu(II) kompleksai

Aplicação da técnica de eletroforese capilar para verificação e comparação da homogeneidade de dosagem em medicamentos industriais e magistrais

Aleixo, Fernanda Caroline

January 2016

Orientador: Prof. Dr. Alexandre Zatkovskis Carvalho / Dissertação (mestrado) - Universidade Federal do ABC. Programa de Pós-Graduação em Ciência e Tecnologia/Química, 2016. / No Brasil, onde a desigualdade social é evidente, nem todos os cidadãos têm acesso aos mesmos medicamentos. No entanto, algumas práticas como a distribuição de medicamentos pelo SUS, quebra de patentes, produção de genéricos e aviamento de medicamentos permitem que a população mais carente seja atendida em suas necessidades terapêuticas. Para que essas vantagens sejam efetivamente reais, deve-se garantir que a eficácia terapêutica dos medicamentos mais acessíveis seja similar à dos medicamentos de referência. Neste trabalho a técnica de eletroforese capilar foi utilizada para a comparação da qualidade de medicamentos. Desta forma, este trabalho constitui também um serviço público à população ao verificar comparativamente a qualidade de medicamentos de referência, genéricos, similares e magistrais utilizados para o tratamento de hipertensão, principalmente verificando a uniformidade de dosagem. A formulação escolhida para este estudo foi a associação de maleato de enalapril e hidroclorotiazida. Foram estudadas amostras do laboratório de referência, um genérico e um similar, na forma farmacêutica de comprimidos para administração via oral, além de duas formulações obtidas em farmácias magistrais, na forma farmacêutica de cápsulas. A identificação dos analitos foi realizada através da obtenção de espectros de absorção molecular. A exatidão do método de análise por eletroforese capilar de zona foi comprovada através de testes de recuperação realizados para todos os laboratórios analisados. A faixa aceita de teor de princípio ativo permitido pela farmacopeia brasileira é de 90 a 110% do valor declarado no rótulo do medicamento, condição satisfeita por todas as formulações testadas. Os testes de uniformidade de peso e dosagem das unidades de cada lote demonstraram que tanto os laboratórios industriais como os magistrais satisfazem os requerimentos da farmacopeia brasileira considerando 30 dias de tratamento, mesmo com grandes diferenças de preço ao consumidor. / Since social differences are remarkable in Brazil, not all citizens have access to the same drugs. However, some health-related policies such as drug distribution by SUS, early patent break, generic manufacture and compounding pharmacies allows less wealth population to access their health treatment. To make these advantages real the therapeutic efficacy of those inexpensive formulations must be assured, as are the reference drugs. In this work the capillary electrophoresis technique was used to compare the quality of medicines. This way, this work also offers a public service to the population due to its comparative study of the quality of anti-hypertensive reference medicine, generics, similar and formulations from compounding pharmacies, accessing principally dose uniformity. Oral pills of the association of enalapril maleate and hydrochlorothiazide were chosen for this study, including a reference drug (patent owner), one generic formulation and one similar formulation. Capsules from two compounding pharmacies were also analyzed. Brazilian Pharmacopoeia preconizes drug approved if active substance assay is between 90 to 110% of label. Weight and dosage uniformity tests of each batch showed that both industrial laboratories as compounding satisfy the requirements of Brazilian Pharmacopoeia given 30 days of treatment, even with large differences in price to the consumer.

ELETROFORESE CAPILAR

MALEATO DE ENALAPRIL

HIDROCLOROTIAZIDA

CAPILLARY ELECTROPHORESIS

ENALAPRIL MALEATE

HYDROCHLOROTHIAZIDE

Memória do medo condicionado ao contexto : alterações por inibição da síntese proteica ou por bloqueio de receptores de glutamato do tipo NMDA no hipocampo / Retrieval of the aversive memory : impairments by protein synthesis inhibition or blockade of NMDA glutamatergic receptor in the hippocampus

Sperandeo, Maria Luiza Antunes, 1949-

28 August 2013

Orientador: Elenice Aparecida de Moraes Ferrari / Tese (doutorado) - Universidade Estadual de Campinas, Instituto de Biologia / Made available in DSpace on 2018-08-23T21:27:10Z (GMT). No. of bitstreams: 1 Sperandeo_MariaLuizaAntunes_D.pdf: 3058745 bytes, checksum: 13c43e27d3d229473548efb9ae77c620 (MD5) Previous issue date: 2013 / Resumo: O estudo do condicionamento clássico aversivo contribuiu para caracterizar as fases da formação da memória (aquisição, consolidação, reconsolidação, persistência e extinção) e os mecanismos de plasticidade neuronal subjacentes. Entre estes, a ativação de receptores glutamatérgicos NMDA, de transcrição gênica e síntese proteica parecem fundamentais. O fator neurotrófico derivado de cérebro (BDNF) e o gene de expressão imediata (IEG) zenk são ativados no hipocampo de mamíferos durante a reconsolidação e a extinção. Este estudo investigou os efeitos da inibição da síntese proteica e do bloqueio dos receptores NMDA no hipocampo de pombos na reconsolidação e extinção da memória de medo contextual. No Experimento 1, pombos foram condicionados, testados ao contexto (reativação), submetidos à infusão intra-hipocampo de salina (SAL-PR), de anisomicina (ANI-PR) ou de MK-801 (MK-PR) após o teste (pós-reativação; PR), e retestados 2 dias depois (Rt 2d). No Experimento 2, três grupos tiveram um segundo reteste, 9 dias após a infusão (Rt 9d), enquanto que outros três grupos não passaram pelo teste (sem reativação- SR). O treino (20 min) teve três pareamentos som-choque. No teste e no Rt 2d houve exposição ao contexto do condicionamento por 5 min e no reteste Rt 9d, por 30 min. Nos dois experimentos, todos os grupos apresentaram alta ocorrência de congelamento (CONG) nas sessões de treino e de teste, mas no Rt 2d os grupos ANI-PR e MK-PR mostraram uma redução significativa de CONG (p < 0,05). Os grupos SR exibiram alta ocorrência de CONG tanto no Rt 2d, quanto no início do Rt 9d (p > 0,05). No Rt 9d o grupo MK-PR não teve recuperação espontânea de CONG, sugerindo prejuízo irreversível provocado pelo MK-801 na memória de medo contextual. Os grupos, SAL-PR, SAL-SR, ANI-PR, ANI-SR e MK-SR mostraram diminuição gradual de CONG durante a sessão de Rt 9d, evidenciando a extinção. Análises com Western blotting após o Rt 9d indicaram que o conteúdo de BDNF-maduro no hipocampo dos pombos SAL-PR foi significativamente maior em comparação aos demais grupos (p < 0,05), mas não foram observadas diferenças entre os grupos para o Zenk (p > 0,05). Isso sugere a participação do BDNF hipocampal na reconsolidação e na extinção da memória de medo contextual em pombos. Assim, a inibição da síntese proteica e o bloqueio dos receptores NMDA no hipocampo de pombos, após o teste ao contexto, prejudicaram a reconsolidação da memória de medo condicionado ao contexto. Além disso, os prejuízos observados foram dependentes da reativação da memória durante o teste / Abstract: The study of classical aversive conditioning has contributed to the characterization of different phases in memory formation (acquisition, consolidation, reconsolidation, extinction and persistence) and the underlying mechanisms of neuronal plasticity. Among these, the activation of NMDA glutamate receptors, gene transcription and protein synthesis are pointed as essentials. The brain-derived neurotrophic factor (BDNF) and immediate expression gene (IEG) zenk are activated in the hippocampus of mammals during reconsolidation and extinction. This study investigated the effects of protein synthesis inhibition and blockade of NMDA receptors in the hippocampus of pigeons on reconsolidation and extinction of contextual fear memory. In Experiment 1, pigeons were conditioned, tested in the context (reactivation), received intra-hippocampus infusion of saline (SAL-PR), anisomycin (ANI-PR) or MK-801 (MK-PR) after the test (post-reactivation, PR), and had a retest two days later (Rt 2d). Experiment 2, had a retest 9 days after intra-hippocampus infusion (Rt 9d) for three PR groups, and other three groups that were not tested 24h after training served as control for reactivation (no reactivation-NR). Three tone-shock pairings were presented during training (20 min). Pigeons were exposed to the context during 5 min in the test and Rt 2d sessions and during 30 min in Rt 9d. In both experiments, the occurrence of freezing (FRZ) was high in training and testing sessions for all the groups, but ANI-PR and MK-PR pigeons showed a significant decrease in FRZ during the Rt 2d (p < 0.05). The NR groups exhibited high occurrence of FRZ both in the Rt 2d and in the beginning of Rt 9d (p > 0.05). MK-PR pigeons had no spontaneous recovery of FRZ, suggesting irreversible impairment caused by MK-801 in contextual fear memory. The groups, SAL-PR, SAL-NR, ANI-PR, ANI-NR and MK-NR showed a gradual decrease in FRZ during the Rt 9d session, evidencing extinction. Western Blotting analysis indicated that the content of mature BDNF in the hippocampus of SAL-PR group after Rt 9d session was higher than that seen for the other groups (p < 0.05), but no between-group differences for Zenk were observed (p > 0.05). This suggests the involvement of hippocampal BDNF in reconsolidation and extinction of contextual fear memory in pigeons. The present data show that inhibition of protein synthesis and blockade of NMDA receptors in the hippocampus of pigeons, after the testing session to context, impaired reconsolidation of contextual fear conditioning memory and affected the process of extinction. Furthermore, the impairments were dependent on the reactivation of fear memory during the test / Doutorado / Fisiologia / Doutor em Biologia Funcional e Molecular

Condicionamento clássico

Memória

Inibidores da síntese de proteínas

Maleato de dizocilpina

Hipocampo

Pombo

Conditioning, classical

Memory

Protein synthesis inhibitors

Dizocilpine maleate

Hippocampus

Pigeon