Mechanismen Isoprenalin-induzierter Extrakontraktionen im humanen Vorhofmyokard / Mechanisms of isoprenaline-induced extra contractions in human atrial myocardium

Schottky, Dörte

31 July 2012

No description available.

610 Medizin, Gesundheit

MED 411 Kardiologie

Medicine

Ryanodinrezeptor

PKA

CaMKII

Arrhythmie

β-adrenerge Stimulation

Vorhofmyokard

ryanodine receptor

PKA

CaMKII

arrhythmia

β-adrenergic stimulation

atrial myocardium

44.85 Kardiologie

Angiologie

Le rôle des récepteurs aux cannabinoïdes CB1 et CB2 dans le guidage axonal

Argaw, Anteneh

12 1900

Au cours du développement, les axones des cellules ganglionnaires de la rétine (CGRs) voyagent sur de longues distances pour établir des connexions avec leurs cellules cibles. La navigation des cônes de croissance est guidée par différentes molécules chimiotropiques présentes dans leur environnement. Les endocannabinoïdes (eCB) sont d’importants neuromodulateurs qui régulent de manière rétrograde la fonction de nombreuses synapses du cerveau. Ils agissent principalement par le biais de leurs récepteurs liés à une protéine Gi/o CB1 (CB1R) et CB2 (CB2R). La présence des eCBs durant le stade fœtal et la période postnatale suggère leur implication dans des événements régulant le développement du système nerveux. Cette thèse confirme l’expression des récepteurs aux cannabinoïdes CB1 et CB2 ainsi que l’enzyme dégradant les eCBs lors du développement embryonnaire et perinatal des CGRs et de la voie rétinothalamique in vivo. La manipulation pharmacologique de l’activité de CB1R et CB2R réorganise la morphologie du cône de croissance des CGRs et des neurones corticaux in vitro. De plus, la stimulation locale avec un agoniste de CB1R ou de CB2R modifie le comportement du cône de croissance entraînant sa répulsion. CB1R et CB2R modulent par le biais de la voie de signalisation AMPc/PKA, la mobilisation de DCC à la membrane plasmique. Par ailleurs, les résultats de cette recherche démontrent également l’implication de CB1R et CB2R dans la ségrégation des projections ipsi- et controlatérales et le développement de la voie rétinothalamique. / Following differentiation, retinal ganglion cell (RGC) axons, tipped at their distal end by the growth cone (GC), navigate through relatively long distances in a highly directed manner in order to establish functional synapses with thalamic and superior colliculus (SC) neurons. This is achieved with the help of extracellular guidance molecules which steer RGC axon growth by regulating GC morphology by means of attractive and/or repulsive mechanisms. In the adult brain, endocannabinoids (eCBs) exert an important neuromodulatory function by acting as retrograde messengers to regulate the function of many synapses. Endocannabinoids act mainly via their Gi/o protein coupled receptors CB1 (CB1R) and CB2 (CB2R). Due to their presence at the fetal and early postnatal periods, it has been proposed that eCBs and their receptors might be involved in several developmental events, such as cell proliferation and migration, axon guidance and synaptogenesis. We observed that during early postnatal development, components of the eCB system are expressed along the visual pathway (the optic chiasm, the lateral geniculate nucleus and the SC). To assess the implication of the eCB system, in vitro, embryonic retinal explant and primary neuron cultures were treated with pharmacological agonists and inverse agonists of CB1R and CB2R. These experiments demonstrated that these cannabinoid receptors modify the GC’s morphology. Most importantly, CB1R and CB2R act through the cAMP/PKA pathway to modulate the presence of DCC at the plasma membrane. In vivo, CB1R and CB2R play a major role and the absence of either one of them induces a decrease in eye-specific segregation of retinal projections. These results show an implication of CB1R and CB2R during RGC growth and retinothalamic development.

Cône de croissance

guidage axonal

récepteurs aux cannabinoïdes

CGR

DCC

PKA

AMPc

Growth cone

axon guidance

cannabinoid receptors

RGC

DCC

PKA

cAMP

Régulation de la migration des cellules cancéreuses coliques HCT-116 par la sous-unité α1D et du canal SK3 par la voie AMPc-PKA / Regulaiton of the migration of the HCT-116 colonic cancer cells by the alpha1D subunit and the SK3 channel via the cAMP-PKA pathway

Fourbon, Yann

06 October 2017

De plus en plus d'études désignent les canaux K+ et Ca2+ comme de nouvelles cibles très prometteuses pour des thérapies anticancéreuses. Parmi ces canaux, les canaux SK3 et CaV1.3 ont été identifiés comme des régulateurs de la migration des cellules cancéreuses. Lors de mes travaux de thèse, nous avons découvert une nouvelle voie de signalisation montrant que la protéine αlD du canal CaVl.3 est impliquée dans la régulation de l'homéostasie Ca2+ ainsi que dans la migration cellulaire, par un mécanisme indépendant de sa fonction canonique. En parallèle nous avons identifié des résidus sérines du canal SK3 qui sont importants dans la régulation négative du canal SK3 par l'activation de la voie AMPc-PKA. Ces résultats suggèrent également que l'Ohmline, un éther-lipide de synthèse, inhibiteur du canal SK3, ne réduit pas l' activité du canal SK3 en favorisant sa phosphorylation suite à l'activation de la voie AMPc-PKA. / Many studies show that K+ and Ca2+ channels are promising new targets for anticancer therapies. Among these channels, SK3 and Ca V 1.3 ion channels have been identified as regulators of cancer cell migration. Here, we have discovered a new signalization pathway showing that the αlD protein of the CaV1 .3 channel is involved in the regulation of Ca2+ homeostasis and in cell migration by a mechanism independent of its canonical function. In parallel, we have identified serine residues of SK3 channel that are important in the negative regulation of the SK3 channel by activation of the cAMP-PKA pathway. These results also suggest that Ohmline, a synthetic ether-lipid, and inhibitor of SK3 channel, does not reduce the activity of SK3 channel by promoting its phosphorylation following the activation of the cAMP-PKA pathway.

"αlD"

CaV1.3

SK3

Ca2+

AMPc

PKA

HCT-116

Migration

"αlD"

CaV1.3

SK3

Ca2+

AMPc

PKA

HCT-116

Migration

Protéine kinase AMP cyclique dépendante et cycle de Plasmodium falciparum / CAMP-dependent protein kinase and plasmodium falciparum life cycle

Wurtz, Nathalie

12 July 2010

L'aggravation actuelle du risque lié au paludisme résulte du développement du phénomène de résistance de souches de Plasmodium falciparum aux molécules antipaludiques. Une telle situation et l’absence de vaccin efficace nécessitent le développement de nouvelles stratégies antiparasitaires. Jusqu’à présent, les mécanismes moléculaires qui contrôlent le cycle parasitaire sont méconnus. Chez la plupart des eucaryotes, les protéine kinases sont impliquées dans des fonctions cellulaires essentielleset constituent une cible privilégiée pour la conception de nouveaux médicaments. Dans cecadre, nous nous sommes intéressés à la voie de transduction de l’AMP cyclique et en particulier à la sous-unité catalytique de la protéine kinase AMPc dépendante (PfPKAc)dont le rôle essentiel reste mal défini chez P. falciparum. Deux approches complémentaires ont été choisies pour étudier cette kinase :1) au niveau biochimique par le clonage, l’expression, la purification et la caractérisation enzymatique de la PfPKAc. L’objectif était d’obtenir une enzyme active in vitro de façon à pourvoir mesurer les constantes enzymatiques de la PfPKAc et conduire les premiers essais d’inhibitions.2) au niveau cellulaire en analysant les conséquences de l’inhibition par des ARN interférents spécifiques des transcrits de la PfPKAc. Le développement parasitaire mais également le transcriptome global ont été étudiés de manière à préciser les voies métaboliques liées à cette kinase plasmodiale.L’ensemble de ces études précise la compréhension de la voie de transduction de l’AMP cyclique et de la PfPKA qui pourrait conduire au développement de nouvelles voies thérapeutiques. / Nowadays, the increase of risks associated with malaria results from the development of resistance of Plasmodium falciparum strains to antimalarial drugs. This situation and the lack of an effective vaccine require the development of new antimalarial strategies. Untilnow, molecular mechanisms controlling the life cycle of malaria parasites, are still poorly understood. In most eukaryotes, protein kinases are implicated in essential cellular functions and represent attractive targets for the development of new drugs. In this context, we focused on the signaling pathway implicating cAMP and particularly the catalytic subunit of cAMP-dependent protein kinase (PfPKAc), whose function is still unclear in P. falciparum. Two complementary strategies were chosen to study this kinase:1) at the biochemical level by the cloning, expression, purification and enzymatic characterization of the PfPKAc. The objective was to obtain an in vitro active PfPKAc to evaluate the kinetic constants of PfPKAc and to conduct the first inhibition studies.2) at the cellular level by studying the consequences of PfPKAc transcripts inhibition byspecific interfering RNAs. The parasite growth but also the overall transcriptome werestudied to specify the metabolic pathways associated with this plasmodial protein kinase.All of these studies improve the understanding of cAMP transduction pathway and PfPKA,which could allow the development of new therapeutic approaches.

Plasmodium falciparum

Protéines kinases

Pka

Caractérisation biochimique

ARN Interférence

Puces à ADN

Voies métaboliques

Plasmodium falciparum

Protein kinases

Pka

Biochimical characterization

Rna interference

Microarray

Metabolic pathways

Inibidores de fosfodiesterases e o controle de processos proteolíticos na atrofia muscular induzida pelo diabetes mellitus / Phosphodiesterase inhibitor and the control of proteolitical processes in muscular atrophy induced by diabetes mellitus

Arcaro Filho, Carlos Alberto [UNESP]

27 April 2018

Submitted by Carlos Alberto Arcaro Filho (carlos_arcaro@hotmail.com) on 2018-07-13T23:08:25Z No. of bitstreams: 1 Tese Final - Carlos Alberto Arcaro Filho.pdf: 7378512 bytes, checksum: cb295c066a7be41be3508e2daf64d24f (MD5) / Approved for entry into archive by Maria Irani Coito null (irani@fcfar.unesp.br) on 2018-07-16T13:17:13Z (GMT) No. of bitstreams: 1 arcarofilho_ca_dr_arafcf_int.pdf: 7378512 bytes, checksum: cb295c066a7be41be3508e2daf64d24f (MD5) / Made available in DSpace on 2018-07-16T13:17:14Z (GMT). No. of bitstreams: 1 arcarofilho_ca_dr_arafcf_int.pdf: 7378512 bytes, checksum: cb295c066a7be41be3508e2daf64d24f (MD5) Previous issue date: 2018-04-27 / Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP) / Considerando os avanços no conhecimento acerca dos mecanismos que controlam o metabolismo de proteínas na musculatura esquelética que permitiram a busca por novas opções para o tratamento das atrofias musculares, o presente estudo teve como objetivo a compreensão do potencial antiproteolítico de inibidores de fosfodiesterase, PDE (pentoxifilina, inibidor não-seletivo de PDE; rolipram, inibidor seletivo de PDE4) em músculos esqueléticos de ratos submetidos à atrofia muscular devido à insuficiência insulínica (diabetes mellitus experimental), com ênfase na elucidação da participação de componentes da sinalização do AMP cíclico (AMPc) nesta resposta. Ratos normais e diabéticos (60 mg/kg de estreptozotocina, administração intravenosa) foram tratados com salina (NS e DS) ou com 2 mg/kg de rolipram (NROL e DROL), ou com 25 mg/kg de pentoxifilina (NPTX e DPTX) durante 3 dias, por via intraperitoneal. Após três dias de tratamento, músculos soleus e extensor digitorum longus (EDL) foram removidos, pesados, congelados e processados para diversas análises: (i) conteúdo de AMPc (ensaio imunoenzimático); (ii) atividades das proteases proteassoma, calpaínas e caspase-3 (uso de substratos específicos fluorigênicos); (iii) níveis proteicos e/ou níveis de fosforilação de componentes das vias proteolíticas, efetores intracelulares sinalizatórios e fatores de transcrição (Western blotting); (iv) determinação dos níveis séricos de insulina e citocinas pró-inflamatórias. Foram realizados experimentos ex-vivo, para verificar a ação direta dos fármacos no controle da proteólise muscular e ativação de efetores intracelulares, via incubações dos músculos na presença de rolipram ou de agonistas de EPAC (Exchange protein directly activated by cAMP) e de PKA (proteína quinase dependente de AMPc), proteínas efetoras ativadas pelo AMPc. Também foram realizados experimentos no Laboratório do Prof. Dr. Marco Sandri, no Venetian Institute of Molecular Medicine, Padova, Itália, para a avaliação do papel de PDE4D no controle do processo autofágico-lisossomal em músculos esqueléticos de camundongos jejuados. Os tratamentos de animais diabéticos com rolipram (DROL) ou com pentoxifilina (DPTX) promoveram uma redução nas atividades do proteassoma e calpaínas em soleus e EDL, bem como nos níveis de componentes-chave do sistema proteolítico ubiquitina-proteassoma (MuRF-1, atrogin-1, conjugados poliubiquitinados), e aumento nos níveis de calpastatina (inibidor das calpaínas). Interesante ressaltar que o grupo DROL apresentou redução na atividade e níveis proteicos de caspase-3, em ambos os músculos, enquanto que o grupo DPTX apenas em músculos EDL. Contribuindo com a redução observada na atividade de caspase-3, houve uma redução nos níveis de Bax (proteína pró-apoptótica) e aumento nos níveis de Bcl-2 (proteína anti-apoptótica) em ambos os músculos de animais DROL. Animais diabéticos tratados com salina (DS) apresentaram aumento nas atividades das três proteases, bem como nos níveis de componentes participantes destes processos proteolíticos. Animais normais e diabéticos tratados com salina (NS e DS) apresentaram níveis de AMPc basais e semelhantes entre si, tanto em soleus quanto em EDL, enquanto que os tratamentos de ratos normais e diabéticos com pentoxifilina (NPTX e DPTX) ou rolipram (NROL e DROL) promoveram aumentos de AMPc, em ambos os músculos. Um dos mecanismos que podem estar envolvidos na inibição da proteólise muscular após aumentos nas concentrações de AMPc envolve a proteína EPAC, responsável por integrar a sinalização do AMPc e a sinalização insulínica via ativação da quinase AKT. Animais diabéticos tratados com pentoxifilina ou com rolipram apresentaram aumento nos níveis proteicos de EPAC 1 e na fosforilação de AKT, quando comparados ao grupo DS. Observamos também um aumento na fosforilação inibitória de fatores de transcrição FoxO 1 e 3a em ambos os músculos de animais DROL. Podemos sugerir que parte das ações de rolipram que culminaram em ativação de AKT e inibição de FoxO na musculatura esquelética possam estar associadas aos aumentos observados nos níveis circulantes de insulina em animais DROL. Investigamos, apenas nos animais tratados com rolipram, a possibilidade de participação da proteína PKA no controle da proteólise muscular. Em animais DROL houve ativação da PKA, verificada tanto pelo aumento na fosforilação de substratos de PKA, bem como do fator de transcrição CREB, em soleus e EDL. Vale destacar que animais DS apresentaram níveis reduzidos de p-CREB e de substratos fosforilados por PKA em soleus e EDL. Animais diabéticos tratados com os inibidores de PDE apresentaram uma diminuição de citocinas pró-inflamatórias séricas (TNF-, PTX e ROL; IL-1, ROL) e aumento nos níveis de insulina sérica (ROL) em relação aos animais DS. Nos estudos ex vivo, as incubações de músculos soleus e EDL com rolipram levaram a uma redução da proteólise total, bem como aumento na fosforilação de substratos de PKA e de AKT. Músculos soleus e EDL incubados com agonistas de EPAC apresentaram aumento na fosforilação de AKT, enquanto que a incubação com agonista de PKA promoveu aumento na fosforilação dos substratos de PKA (em ambos os músculos) e aumento na fosforilação de AKT (apenas em EDL), quando comparados aos músculos incubados na ausência do fármaco. Nos estudos para compreensão do papel de PDE4D no controle do processo autofágico-lisossomal, observou-se que o silenciamento gênico da PDE4D em músculos tibialis anterior promoveu uma preservação da massa muscular e da área da fibra em animais jejuados, quando comparados ao músculo controle. Músculos flexor digitorium brevis, silenciados para PDE4D, apresentaram diminuição na expressão de proteínas-chave do processo autofágico-lisossomal, tais como LC3 e p62. Estes resultados evidenciam os mecanismos que podem estar envolvidos na ação direta de inibidores de PDE no controle do metabolismo proteico muscular esquelético, via ativação de duas vias dependentes de AMPc: (i) a via PKA/CREB, que pode participar do controle da transcrição de Bcl-2 e calpastatina, bem como na inativação direta de caspases, inibindo assim os processos proteolíticos dependentes de caspase-3 e calpaínas, (ii) a via EPAC/AKT, via fosforilação e inibição de FoxO 1 e 3A, regulando a expressão dos atrogenes (MuRF-1 e atrogin-1) e promovendo uma diminuição na atividade do sistema ubiquitina-proteassoma. Além disso, o tratamento com inibidores de PDE diminuem o processo inflamatório e aumentam os níveis circulantes de insulina, ações que podem contribuir para os efeitos antiproteolíticos. Evidências iniciais também sugerem que PDE4D participa no controle do sistema autofágico-lisossomal na musculatura esquelética. Todos estes resultados indicam que PDE participam no controle de processos proteolíticos, portanto inibidores de PDE emergem como uma opção interessante na ativação da sinalização do AMPc na musculatura esquelética, com vistas à utilização futura no tratamento de quadros de perda de massa muscular durante situações de atrofia. / Considering the advances in the knowledge of the mechanisms controlling the protein metabolism in skeletal muscles that allowed the discover of new options for the treatment of muscle atrophies, the present study aimed to understand the antiproteolytic potential of phosphodiesterase (PDE) inhibitors (pentoxifylline, a non-selective PDE inhibitor; rolipram, a selective PDE 4 inhibitor), in skeletal muscles of rats submitted to muscle atrophy due to insulin insufficiency (experimental diabetes mellitus), with emphasis on the elucidation of the participation of cyclic AMP (cAMP) signaling components. Normal and diabetic rats (60 mg/kg streptozotocin, intravenous administration) were treated intraperitoneally with saline (NS and DS) or with 2 mg/kg rolipram (NROL and DROL) or with 25 mg/kg pentoxifylline (NPTX and DPTX) for 3 days. After three days of treatments, soleus and extensor digitorum longus (EDL) muscles were removed, weighed, frozen and processed for several analyzes: (i) cAMP content; (ii) activities of proteasome, calpain and caspase-3 (use of specific fluorigenic substrates); (iii) protein levels and/or phosphorylation levels of components of proteolytic pathways, intracellular signaling effectors and transcription factors (Western blotting); (iv) determination of serum insulin and proinflammatory cytokines levels. Ex vivo experiments were performed to verify the direct action of the drugs in the control of muscle proteolysis and activation of intracellular effectors, via muscle incubations in the presence of rolipram or agonists of EPAC (Exchange protein directly activated by cAMP) and PKA (cAMP-dependent protein kinase), intracellular effectors activated by cAMP. Experiments were also carried out in the Laboratory of Prof. Dr. Marco Sandri at the Venetian Institute of Molecular Medicine, Padova, Italy, for the evaluation of the role of PDE4D in controlling the autophagic-lysosomal process in skeletal muscles of starved mice. Treatments of diabetic animals with rolipram (DROL) or pentoxifylline (DPTX) promoted a reduction in the activities of proteasome and calpain in soleus and EDL, as well as reduced the levels of key components of the ubiquitin-proteasome system (MuRF-1, atrogin-1, polyubiquitinated conjugates), and increased the levels of calpastatin (calpain inhibitor). Interestingly, DROL rats showed a reduction in the activity and in the protein levels of caspase-3 in both muscles, whereas DPTX rat had reductions only in EDL muscles. Contributing to the reduction in caspase-3 activity, it was observed a reduction in the content of Bax (pro-apoptotic protein) and an increase of Bcl-2 (anti-apoptotic protein) in both muscles of DROL rats. Diabetic animals treated with saline (DS) showed an increase in the activities of the three proteases, as well as increases in the levels of components belonging to these proteolytic processes. Normal and diabetic animals treated with saline (NS and DS) had basal and similar levels of cAMP in both soleus and EDL, whereas the treatments of normal and diabetic rats with pentoxifylline (NPTX and DPTX) or with rolipram (NROL and DROL) promoted increases in cAMP in both muscles. One of the mechanisms that may be involved in the muscle proteolysis inhibition after increases in cAMP involves the EPAC protein, responsible for integrating the cAMP and the insulin signaling pathways via AKT activation. Diabetic animals treated with pentoxifylline or with rolipram showed an increase in the protein levels of EPAC 1 and in the phosphorylation of AKT, when compared with the DS group. We also observed an increase in the phosphorylation (inhibitory) of FoxO 1 and 3a in both muscles of DROL rats. It can be suggested that part of the rolipram actions causing AKT activation and FoxO inhibition in skeletal muscles may be associated with the increases in the circulating levels of insulin observed in DROL animals. It was investigated, only in animals treated with rolipram, the possible involvement of PKA in the control of muscle proteolysis. DROL rats had activation of PKA, verified both by the increase in the phosphorylation of PKA substrates, as well as in the phophorylation of the transcription factor CREB, in soleus and EDL. DS rats had decreased levels of p-CREB and of the PKA substrates, in soleus and EDL. Diabetic animals treated with PDE inhibitors showed a decrease in serum proinflammatory cytokines (TNF-, PTX and ROL; IL-1, ROL) when compared with DS. In ex vivo studies, incubations of soleus and EDL with rolipram caused a reduction of the total proteolysis as well as an increase in the phosphorylation of PKA substrates and and of AKT. Soleus and EDL muscles incubated with EPAC agonist showed increased in the AKT phosphorylation, whereas incubation with PKA agonist promoted an increase in the phosphorylation of PKA substrates (in both muscles) and and increase in the AKT phosphorylation (EDL), when compared with muscles incubated in the absence of the drugs. In studies to understand the role of PDE4D in the control of the autophagic-lysosomal process, it was observed that the PDE4D gene silencing in anterior tibialis muscles caused a preservation of the muscle mass and fiber area in fasted animals when compared with control muscle. Flexor digitorium brevis muscles, silenced for PDE4D, showed a decreased expression of key proteins of the autophagic-lysosomal process, such as LC3 and p62. These results suggested the mechanisms that may be involved in the direct action of PDE inhibitors in the control of skeletal muscle protein metabolism, through activation of two cAMP-dependent pathways: (i) the PKA/CREB pathway, which may participate in transcriptional control of Bcl-2 and calpastatin, as well as causing direct inactivation of caspases, thus inhibiting the proteolytic processes dependent on caspase-3 and calpains, (ii) the EPAC/AKT pathway, via phosphorylation and inhibition of FoxO 1 and 3a factors, regulating the expression of atrogenes (MuRF-1 and atrogin-1) and promoting a decrease in activity of ubiquitin-proteasome system. Treatments with PDE inhibitors also decreased the inflammatory process and increased the circulating linsulin levels, which may be contributing to the antiproteolytic responses. Initial evidence also suggests that PDE4D participates in the control of the autophagy-lysosomal system in skeletal muscles. All these results indicate that PDE participate in the control of proteolytic processes, therefore PDE inhibitors emerge as an interesting option to activate the cAMP signaling in the skeletal muscles, which may be used in the future in treatments muscle mass loss during atrophy situations. / FAPESP: Processo 2013/18861-2 / FAPESP: Processo 2014/12202-0 / FAPESP: Processo 2017/02348-5

Atrofia muscular

Fosfodiesterase do tipo 4

Rolipram

Pentoxifilina

AMP cíclico

PKA

EPAC

AKT

Diabetes mellitus

Muscle atrophy

Phosphodiesterase type 4

Rolipram

Pentoxifylline

Cyclic AMP

PKA

EPAC

AKT

diabetes mellitus

Aspectos Comportamentais e Moleculares da Sensibilização Cruzada entre Estresse e Cocaina. / Behavioral and molecular aspects of the cross-sensitization between stress and cocaine

Ana Paula Natalini de Araujo

10 August 2001

Vários estudos clínicos demonstram que existem fatores adicionais ao efeito reforçador primário das drogas que determinam por que alguns indivíduos permanecem usuários ocasionais, enquanto outros progridem para a farmacodependência. Evidências clínicas apontam o estresse como uma variável importante na iniciação, manutenção e recaída ao uso da cocaína ou morfina. Em roedores, a cocaína induz a sensibilização comportamental que se caracteriza pelo aumento progressivo da atividade motora no decorrer do seu uso prolongado. Esse fenômeno é um dos eventos que emergem no decurso temporal das adaptações que levam à farmacodependência. Recentemente foi sugerido que a sensibilização é a gênese do uso compulsivo de drogas. Muitos estudos revelam que o estresse induz a sensibilização comportamental cruzada com os psicostimulantes. O objetivo desse trabalho foi avaliar a sensibilização cruzada entre o estresse e a cocaína, bem como os mecanismos neurais subjacentes. Para tanto foram avaliados as concentrações plasmáticas da corticosterona, a atividade locomotora basal e a induzida por cocaína, e a atividade da PKA nos animais expostos aos estresses agudo ou crônico, previsível ou imprevisível. A exposição ao estresse crônico previsível (EP) aumentou a atividade locomotora basal e a induzida por cocaína. A exposição ao EP aumentou as concentrações basais da corticosterona mas não alterou a atividade da PKA no núcleo acumbens e no corpo estriado. Assim, podemos concluir que a exposição a EP induziu sensibilização comportamental cruzada à cocaína, sendo que esse efeito não se correlacionou com as alterações na atividade da PKA. / A potential etiologic factor in substance abuse is stress, and it is possible that chronic exposure to stressful life’s events is related to the development of drug dependence and relapse. Behavioral sensitization is defined as an augmentation of a response to a drug during repeated drug exposure. Behavioral sensitization has been shown to occur to the locomotor and reinforcing effects of cocaine, amphetamine and other drugs of abuse. It has been suggested that sensitization is the genesis of compulsive drug use. Converging evidence suggests that exposure to stress induces behavioral sensitization to psychostimulant drugs. The present study investigates behavioral and molecular aspects of the cross-sensitization between stress and cocaine. We evaluated the basal and cocaine-induced locomotor activity, corticosterone plasma levels and protein kinase cAMP-dependent (PKA) activity in animals exposed to acute or chronic predictable and unpredictable stress. Increased basal and cocaine-induced locomotor activity was observed in animals exposed to chronic predictable stress. Chronic predictable stress increased basal corticosterone levels but did not change protein kinase A activity in both accumbens and striatum. In conclusion, predictable stress produced sensitization to locomotor effects of cocaine but this effect did not correlate with changes in PKA activity.

Cocaína

Estresse

Sensibilização comportamental

5. Corticosterone

Behavioral sensitization

Cocaine

Protein kinase. cAMP-dependent (PKA)

Stress

Adsorção de 5 fluorouracil e 5 clorouracil sobre HOPG : um estudo da importância do estado de protonação via microscopia de varredura por tunelamento

Passos, Renata Almeida

30 June 2011

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / This work explored the adsorption of organic molecules to achieve change on surfaces. In this context it was proposed, the adsorption of organic molecules of halogenated derivatives of uracil, 5 Fluorouracil and 5 Chlorouracil, in monocrystalline substrate of HOPG (highly oriented pyrolytic graphite), sizzling was the technique used for construction of self-assembled monolayers (SAM). The atomic resolution of the STM (Scanning Tunneling Microscope) images of HOPG substrate prove its hexagonal structure and that their interatomic distance is 0.246 nm. While in the molecular resolution images of 5 Fluorouracil and of 5 Chlorouracil adsorbed on the HOPG substrate, is presented evidence that after in the adsorption some changes occur in the intermolecular distances in the structures and the positioning of these molecular films formed on the substrate because the molecular films behaved in a horizontal position and were stabilized laterally by hydrogen bonds when they are protonated, but when we performed the same procedure of adsorption for these organic molecules, only varying the pH of the environment, the change caused the deprotonation of the molecules, thus allowing one to simulate electrochemical environment and being able to extract information about the pKa of adsorbates using UV-Vis spectroscopy, and was also observed that these deprotonated molecular films behaved in a vertical position on the substrate. / Neste trabalho foi explorada a adsorção de moléculas orgânicas para realizar modificação em superfícies. Neste contexto foi proposta a adsorção das moléculas orgânicas de derivados halogenados do uracil, o 5 Fluorouracil e o 5 Clorouracil no, substrato monocristalino do HOPG (Grafite Pirolítico Altamente Orientado do inglês, Highly Oriented Pyrolitic Graphite), sendo usada a técnica de sizzling para construção de monocamadas automontadas (SAM Self-Assembled Monolayers). As imagens de STM (Scanning Tunneling Microscopy) de resolução atômica do substrato de HOPG comprovam sua estrutura hexagonal e sua distância interatômica que é de 0,246 nm. Já nas imagens de resolução molecular do 5 Fluorouracil e do 5 Clorouracil adsorvido no substrato do HOPG, são apresentadas evidências de que após a adsorção ocorrem mudanças nas distâncias intermoleculares, nas estruturas e no posicionamento desses filmes moleculares formados no substrato, pois os filmes moleculares se comportaram em um posicionamento horizontal e são estabilizados lateralmente por ligações de hidrogênio quando estão protonadas, mas quando foi realizado o mesmo procedimento de adsorção para essas moléculas orgânicas, só que variando o pH do meio, esta variação provocou a deprotonação das moléculas, assim permitindo simular um ambiente eletroquímico e sendo possível extrair informação sobre o pKa dos adsorbatos usando a espectroscopia UV-Vis, e foi observado também que estes filmes moleculares deprotonados se comportaram em um posicionamento vertical no substrato.

5 Fluorouracil

5 Clorouracil

STM

Deprotonação

PKa

UV-Vis

5 Fluorouracil

5 Chlorouracil

STM

Deprotonation

PKa

UV-Vis

Análise da expressão e das interações da subunidade catalítica da PKA do fungo patogênico Paracoccidioides ssp. / Analysis of the expression and interactions of the catalytic subunit of PKA in pathogenic fungus Paracoccidioides ssp.

Teixeira, Mirian Vieira

10 March 2016

Submitted by Luciana Ferreira (lucgeral@gmail.com) on 2016-08-04T11:29:03Z No. of bitstreams: 2 Dissertação - Mirian Vieira Teixeira - 2016.pdf: 1440228 bytes, checksum: a429eb9e9ac048fbcc06d59fca852c03 (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) / Approved for entry into archive by Luciana Ferreira (lucgeral@gmail.com) on 2016-08-04T11:30:39Z (GMT) No. of bitstreams: 2 Dissertação - Mirian Vieira Teixeira - 2016.pdf: 1440228 bytes, checksum: a429eb9e9ac048fbcc06d59fca852c03 (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) / Made available in DSpace on 2016-08-04T11:30:40Z (GMT). No. of bitstreams: 2 Dissertação - Mirian Vieira Teixeira - 2016.pdf: 1440228 bytes, checksum: a429eb9e9ac048fbcc06d59fca852c03 (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Previous issue date: 2016-03-10 / Conselho Nacional de Pesquisa e Desenvolvimento Científico e Tecnológico - CNPq / Fundação de Amparo à Pesquisa do Estado de Goiás - FAPEG / The Paracoccidioides genus comprises a complex of pathogenic fungi that are the etiologic agents of paracoccidioidomycosis (PCM), the most prevalent systemic mycosis in Latin America. The infection begins after inhalation of fungal propagules, which reach the epithelium of the alveoli where the transition from the mycelial to the pathogenic yeast form. Host elevated temperature triggers the morphological switch, which is necessary for fungal pathogenicity. The cAMP/protein kinase A (PKA) signaling pathway has been shown to be important in controlling morphological changes and the pathogenicity of several pathogenic fungi. Evidence also highlights the importance of the cAMP/PKA pathway in the morphological transition of Paracoccidioides. PKA is the major effector of this signaling pathway. The protein is an inactive tetramer composed of regulatory subunit, encoded by the BCY1 gene; and catalytic subunit, encoded by the TPK2 gene. Upon binding of cAMP to the regulatory subunits, the catalytic subunits dissociate and become active. Activated PKA subsequently phosphorylates protein kinases, transcription factors, and other substrates to control several biological processes. In this study, we evaluated the expression and interactions of Tpk2 protein Paracoccididioides spp. The Tpk2 is present in mycelium decreased during the initial stages of transition phases, and increases again at the end of differentiation, with maximal levels in yeast. We analyzed the interactions of recombinant Tpk2p with Paracoccidioides proteins using pull-down assays followed by MS analysis. Two interacting proteins were identified: the heat shock protein 90 (Hsp90) and a conserved hypothetical protein with a MFS domain. Hsp90 is involved in the regulation of morphogenesis, development and virulence in several thermal dimorphic fungi. These data are important for understanding the mechanisms that trigger the transition phases in Paracoccidioides. / O gênero Paracoccidioides compreende um complexo de fungos patogênicos, que são os agentes etiológicos da paracoccidioidomicose (PCM), a micose sistêmica mais prevalente na América Latina. A infecção inicia-se com a inalação de propágulos do fungo, que atingem o epitélio dos alvéolos pulmonares, onde ocorre à transição da forma de micélio para a forma patogênica, de levedura. Há evidências de que a temperatura seja o principal fator responsável pela diferenciação celular desses fungos, e sua patogenicidade é frequentemente associada com a transição dimórfica. A via de sinalização cAMP/ proteína quinase A (PKA) controla alterações morfológicas e de virulência/patogenicidade em várias espécies de fungos patogênicos humanos. Evidências apontam também para a importância da via cAMP/PKA em Paracoccidioides spp. A PKA é o principal efetor desta via de sinalização. A proteína na forma inativa é um tetrâmero composto de subunidade regulatória, codificada pelo gene BCY1; e subunidade catalítica, codificada pelo gene TPK2. Após a ligação de cAMP às subunidades regulatórias, as subunidades catalíticas dissociam-se e tornam-se ativas. Ativada a PKA fosforila proteína-quinases, fatores de transcrição, e outros substratos para controlar diversos processos biológicos. Neste estudo, avaliamos a expressão e as interações da proteína Tpk2 de Paracoccididioides spp. A Tpk2 está presente em micélio, diminui nos estágios iniciais da transição de fases e volta a aumentar no final da diferenciação, apresentando níveis máximos na levedura. Foram analisadas as interações de Tpk2p recombinante com proteínas de Paracoccidioides utilizando ensaios de pull-down, seguido por análise de MS. Foram identificadas duas proteínas que interagem: a proteína de choque térmico 90 (Hsp90) e uma proteína hipotética conservada com um domínio MFS. Hsp90 está envolvido na regulação da morfogênese, desenvolvimento e virulência em vários fungos dimórficos térmicos. Estes dados são importantes para entendimento dos mecanismos que disparam a transição de fases em Paracoccidioides spp.

Paracoccidioides

Transição dimórfica

Via cAMP/PKA

Ensaios de pull down

Paracoccidioides

Dimorphic transition

cAMP/PKA pathway

Pull-down assays

GENETICA::GENETICA HUMANA E MEDICA

Rôle des récompenses dans la sélection et l'utilisation de différentes formes de mémoire : interactions entre l'hippocampe et le striatum / Role of drug and food rewards in the selection and use of different forms of memory : interactions between the striatum and the hippocampus

Baudonnat, Mathieu

02 December 2011

Il existe différents types de mémoire chez l’homme et l’animal. Chez les mammifères, on distingue principalement une mémoire relationnelle/spatiale reposant sur l’hippocampe et le cortex préfrontal, et une mémoire procédurale/indicée dépendante du striatum. Lors de nouveaux apprentissages, ces systèmes interagissent de manière coopérative et/ou compétitive en fonction de la nature de la tâche. S’il est connu que les émotions négatives et le niveau d’entraînement modulent ces interactions, peu de travaux ont étudié le rôle des récompenses dans la sélection et l’utilisation de ces deux formes principales de mémoire. Nous avons utilisé deux versions du test de discrimination spatiale dans un labyrinthe en Y afin de d’évaluer la mémoire spatiale d’une part, et la mémoire procédurale d’autre part. Nos résultats montrent que la stimulation pharmacologique du système de récompense par auto-injection de morphine au niveau de l’aire tegmentale ventrale (ATV), perturbe de manière spécifique l’apprentissage spatial reposant sur le fonctionnement hippocampo-préfrontal Ce déficit spatial s’accompagne d’une forte réduction de l’activité du facteur de transcription CREB (cAMP Response Element Binding) au sein de ce réseau. Au contraire, l’apprentissage indicé est préservé et l’activation de CREB est potentialisée par l’utilisation d’une récompense pharmacologique (injections de morphine). Nous mettons en évidence que la suractivation de la voie PKA/CREB, dans le striatum dorsal, est la cause de l’interférence observée lors de la formation de la mémoire spatiale. De plus, la stimulation répétée du système de récompense par la drogue lors de l’acquisition d’une stratégie indicée entraîne une persistance de l’activité réverbérante de la voie PKA/CREB dans le striatum dorsal. Cette persistance peut être révélée par l’utilisation préférentielle d’une stratégie indicée dans une nouvelle tâche ambigüe, le test de compétition en piscine de Morris. L’ensemble de ce travail éclaire, grâce aux effets différentiels de récompenses sensorielles et pharmacologiques sur l’apprentissage, la compréhension des interactions dynamiques entre les systèmes de mémoire. De plus, il suggère que l’hyperassociativité persistante consécutive à l’usage de drogue est à l’origine de déficits de type déclaratifs qui pourraient jouer un rôle clé dans l’installation d’un comportement addictif. / There are different forms of memory proceeded in human’s and animal’s brain. At least two major systems can be defined. A spatial/declarative form of memory relies on the hippocampus and prefrontal cortex, and secondly, a more rigid, procedural/cued type of memory supported by striatal circuitry. Learning requires cooperative and/or competitive interactions between memory systems, depending on the nature of the task. It is well established that negative emotions and training modulate these interactions. However, little is known about the role of rewards on the selection and formation of these forms of memory.Using two versions (spatial or cue) of a Y-maze discrimination task, we show that drug reward, but not food reward, disrupts spatial learning while sparing the cued task. The spatial memory deficit relies on an decrease of CREB (cAMP Response Element Binding) activity within the hippocampus and the prefrontal cortex. Inhibition of the PKA/CREB signalling pathway restored spatial learning, suggesting that striatal overactivation of this pathway is responsible for the spatial memory deficit. The cued learning strategy elicits a strong CREB activitiy within the dorsal striatum which is further increased by morphine injections. We propose that drug-induced activation of the DA reward system induces abnormal reverberating activity of the PKA/CREB signalling pathway within the dorsal striatum, eventually leading to a preferential use of a striatum-dependent strategy during a new ambiguous learning task, the water maze competition task.In conclusion, our results points to a key role of rewards in the modulation of learning systems. Furthermore, we provide evidence that drug-induced striatal hyperactivity may underlie the declarative memory deficit reported here. This mechanism could represent an important early step toward the development of addictive behaviors by promoting conditioning to the detriment more flexible forms of memory.

Mémoire

Addiction

Récompense

Aire tegmentale ventrale

Hippocampe

Striatum

Morphine

CREB

PKA

Dopamine

Memory

Addiction

Reward

Dopamine

Ventral tegmental area

Hippocampus

Striatum

Morphine

CREB

PKA

AMPc et prise alimentaire sous le contrôle des récepteurs 5-HT4 de la sérotonine dans le noyau accumbens / cAMP and food intake under control of the 5-HT4 serotonin receptors in the nucleus accumbens

Pratlong, Maud

22 April 2014

L'anorexie mentale est une maladie mortelle liée à une privation volontaire d'aliments en dépit d'un besoin énergétique. La compréhension des causes biologiques des anomalies alimentaires requiert un niveau d'analyse simplifié. Ainsi l'utilisation de modèles animaux a permis d'identifier l'une des premières cibles thérapeutiques potentielles de l'anorexie : le récepteur 5-HT4 de la sérotonine (R5-HT4). La stimulation des R5-HT4 dans le noyau accumbens (NAc) active la voie de signalisation AMPc/PKA/CART et inhibe la faim, alors que l'inhibition de son activité constitutive par un agoniste inverse spécifique inhibe cette voie et provoque une hyperphagie. La transfection d'un R5-HT4 muté (R5-HT4ASSL), insensible à la sérotonine et dont l'activité constitutive est plus forte que celle du récepteur natif, dans le NAc chez la souris sauvage ou privée des R5-HT4, réduit la motivation à consommer des aliments, en activant la voie AMPc/PKA/CART de façon indépendante de la sérotonine. Ces résultats constituent un des rares cas connus d'implication de l'activité constitutive d'un récepteur couplé à une protéine G dans une fonction physiologique, la prise alimentaire. Dans ce contexte, nous décrivons un nouveau facteur de régulation du taux d'AMPc sous le contrôle des R5-HT4 dans le NAc : le complexe « A-kinase anchoring protein/Protein kinase A » (AKAP/PKA). La liaison de la PKA à l'AKAP inhibe l'augmentation du taux d'AMPc et d'ARNm codant le peptide CART, induite par la stimulation pharmacologique des R5-HT4, dans le NAc. Cet effet s'accompagne d'une diminution de la prise alimentaire. Ce rétrocontrôle négatif du complexe AKAP/PKA sur l'activité des R5-HT4 permet de diminuer le taux d'AMPc dans le NAc et de réguler la prise alimentaire. Ces résultats suggèrent qu'une trop forte activité constitutive des R5-HT4 induit une augmentation anormale d'AMPc dans le NAc qui peut conduire à des anomalies alimentaires comme l'anorexie mentale. Nous avons ainsi identifié un mécanisme moléculaire capable de réguler l'activité des R5-HT4 et qui pourrait servir de cible pour le traitement de l'anorexie. / Anorexia nervosa is a deadly mental disease related to a voluntary deprivation of food despite an energy requirement. Understanding of the biological causes of food anomalies requires a level of simplified analysis. And the use of animal models has previously allowed us to identify one of the first potential therapeutic targets of anorexia : serotonin 4 receptors (5-HT4Rs). Stimulation of 5-HT4Rs in the nucleus accumbens (Nac) activates the cAMP/PKA/CART signaling pathway and inhibits hunger, while the inhibition of its constitutive activity by a specific inverse agonist inhibits this pathway and causes hyperphagia. Transfection of a mutated 5-HT4R (5-HT4RASSL) insensitive to serotonin and whose constitutive activity is stronger that the native receptor, in the NAc in mice, reduces motivation for consuming food while activating the cAMP/PKA/CART pathway independently of serotonin. These results are one of the few known cases of involvement of the constitutive activity of G protein coupled receptor to a physiological function, the intake of food.In this context, we describe a new factor regulating cAMP levels under the control of 5-HT4Rs in the NAc: the A-kinase anchoring protein/Protein kinase A (AKAP/PKA) complex. The binding of PKA to AKAPs inhibits the increase in cAMP levels and mRNA encoding the peptide CART induced by pharmacological stimulation of 5-HT4Rs, in Nac. This effect is accompanied by a decrease in food intake The negative feedback of AKAP/PKA complex on the activity of 5-HT4Rs reduces the cAMP levels in the NAc and controls food intake.These results suggest that a too strong constitutive activity of 5-HT4Rs induces cAMP abnormal increase in the Nac and leads to eating abnormalities such as anorexia nervosa. We identified a molecular mechanism that regulates the activity of 5-HT4Rs and could serve as a target for the treatment of anorexia.

Récepteurs 5-HT4

AMPc

Activité constitutive

Noyau accumbens

Prise alimentaire

Akap/pka

Récepteurs 5-HT4

Camp

Constitutive activity

Nucleus accumbens

Food intake

Akap/pka