Caractérisation des mécanismes moléculaires impliqués dans la prolifération cellulaire induite par la protéine HBZ du rétrovirus HTLV-1 / Deciphering the molecular mechanisms responsible for the cellular proliferation induced by the HBZ oncoprotein of the HTLV-1 retrovirus

Terol, Marie

27 September 2016

Le virus T lymphotropique humain de type 1 (HTLV-1) est l’agent étiologique d’une forme rare et très agressive de leucémie de l’adulte (ATL). Le processus leucémogène a longtemps été attribué à la seule action de l’oncoprotéine Tax. Cependant, une nouvelle protéine virale, appelée HBZ (HTLV-1 bZIP factor), a été découverte en 2002. Elle est codée par le brin complémentaire du génome proviral et transcrite en antisens à partir du LTR3’. HBZ s’est avéré être un acteur clef de la prolifération et de la transformation des cellules T infectées, et donc du développement de l’ATL. La présente étude propose de nouvelles pistes quant aux mécanismes par lesquels HBZ induit la survie et la prolifération cellulaire. Nous avons montré que la protéine HBZ stimule l’expression de la neurotrophine BDNF et que les cellules de patients ATL surexpriment à la fois BDNF et son récepteur TrkB. De plus, ces patients présentent une concentration sérique anormalement élevée de la forme mature de BDNF, suggérant l’existence d’une boucle autocrine/paracrine BDNF/TrkB. L’activité de cette boucle a été confirmée in vitro et promeut la survie des cellules infectées par HTLV-1. D’autre part, nous avons découvert qu’HBZ dérégule l’expression du suppresseur de tumeur JunD dans les cellules T infectées, et induit celle de l’isoforme potentiellement oncogène ΔJunD. La production de ΔJunD résulterait d’une altération des mécanismes d’initiation de la traduction par HBZ. Nos résultats montrent aussi que ΔJunD promeut la prolifération et la transformation cellulaire en l’absence de sérum. Nous proposons donc que son expression pourrait contribuer à l’évolution des cellules T infectées en cellules leucémiques. / The human T-lymphotropic virus type 1 (HTLV-1) is associated with a rare and aggressive form of adult leukemia (ATL). For a long time, leukemogenesis was thought to mainly result from the action of the Tax oncoprotein. However, a new viral protein, called HBZ (HTLV-1 bZIP factor), was discovered in 2002. It is encoded by the minus strand of the proviral genome and transcribed in antisens from the 3’LTR. Since its discovery, HBZ came out as a key player in proliferation and transformation of infected T cells, thus contributing to ATL development. In this study we provide new leads regarding the mechanisms of HBZ-induced cell survival and proliferation. On one hand, we show that HBZ stimulates the expression of the BDNF neurotrophin and that ATL cells from patients overexpress both BDNF and its high-affinity receptor TrkB. Moreover, sera from patients exhibited abnormal levels of the mature form of BDNF, suggesting the existence of a BDNF/TrkB paracrine/autocrine loop. That loop was confirmed to be activated in vitro and to support the survival of HTLV-1-infected cells. On the other hand, we discovered that HBZ deregulates the expression of the JunD tumor suppressor in infected T cells and induces that of the ∆JunD isoform, which is potentially oncogenic. ∆JunD production would result from alteration of the translational initiation by HBZ. Our results also show that ∆JunD induces proliferation and transformation of serum starved cells. Finally, we hypothesize that HBZ-induced expression of ∆JunD may influence infected T cells to turn leukemic.

Htlv-1

Atl

Hbz

BDNF/TrkB

JunD

Htlv-1

Atl

Hbz

BDNF/TrkB

JunD

Role of BDNF in Cardiac Remodeling and Dysfunction in Rats After Myocardial Infarction

Lee, Heow Won

23 September 2019

Myocardial infarction (MI) induced heart failure (HF) is a leading cause of morbidity and mortality over the world. Regular exercise improves quality of life and decreases hospitalization and mortality of patients with HF. In animals, exercise post MI attenuates progressive cardiac remodeling and cardiac dysfunction, and decreases neuronal activity in the paraventricular nucleus (PVN) and rostral ventrolateral medulla (RVLM), which are key brain nuclei contributing to sympathetic hyperactivity post MI. The peripheral and central molecular mechanisms underlying these beneficial effects of exercise are not well understood. We studied one possible mechanism, brain-derived neurotrophic factor (BDNF), an exercise-induced factor, which via binding to its receptor tropomyosin-related kinase B (TrkB) may contribute to improvement of cardiac function post MI. In the brain, the ratio between two isoforms of the TrkB receptor, full-length and truncated forms (TrkB.FL/TrkB.T1) determines the extent of intracellular responses to mature BDNF (mBDNF; an active form of BDNF) and a decrease in this ratio may reflect down-regulation of BDNF-TrkB.FL signaling. Ca2+/calmodulin-dependent kinase II (CaMKII) and protein kinase B (Akt) are intracellular factors of BDNF-TrkB signaling in hippocampal/cortical neurons. Activation of cardiac BDNF-TrkB signaling may increase cardiomyocyte survival and myocardial contractility. In hypertensive rats, the role of BDNF-TrkB signaling in the PVN and RVLM appears opposite with activation of this axis in the PVN increasing, but in the RVLM decreasing sympathetic nerve activity (SNA). However, activation of CaMKII and Akt in the PVN and RVLM both mediate increase in SNA. The specific role of BDNF-TrkB signaling in the PVN and RVLM of rats with HF post MI has not yet been studied. We hypothesized that exercise training post MI enhances BDNF-TrkB signaling pathways in the left ventricle (LV) and RVLM, but inhibits in the PVN, and thereby preserves cardiac structure and function post MI. We evaluated changes in BDNF-TrkB axis and intracellular factors CaMKII and Akt in the non-infarct area of the LV, PVN and RVLM in sedentary and exercising rats with MI. The impact of systemic blockade of BDNF-TrkB signaling was assessed with ANA-12, a selective non-competitive antagonist of TrkB receptors. In the infarct area of the LV, mBDNF protein decreased and TrkB.T1 protein increased. In the non-infarct area, mBDNF tended to be decreased without change in TrkB.T1 expression. The activities of CaMKII and Akt were decreased in the non-infarct area of the LV. In the PVN and RVLM, the TrkB.FL/TrkB.T1 ratio was decreased but without changes in mBDNF and downstream factors except for decrease in Akt activity in the RVLM. Exercise training improved ejection fraction (EF), cardiac index and LV end-diastolic pressure, but only the exercise-induced improvement of EF was blocked by ANA-12. In the non-infarct area of the LV, exercise prevented decreases in mBDNF, CaMKII and Akt, and these effects were prevented by ANA-12. In the PVN, exercise increased mBDNF and decreased Akt activity, whereas in the RVLM, exercise had no effect on mBDNF but decreased CaMKII activity. The exercise-induced increase mBDNF in the PVN and decrease in p-CaMKIIβ expression in the RVLM were prevented by ANA-12. Our findings suggest that down-regulation of BDNF-TrkB signaling post MI is prominent in the LV with decreases in mBDNF protein in the infarct area and intracellular factors CaMKII and Akt in the non-infarct area. Increases in mBDNF, CaMKII and Akt in the LV by exercise may contribute to improvement of EF. In the PVN and RVLM, despite a decrease in the ratio of TrkB.FL/TrkB.T1 in both brain nuclei, only Akt activity decreased in the RVLM post MI. Exercise-induced decreases in activities of CaMKII in the RVLM and Akt in the PVN may both contribute to reduction in sympathetic hyperactivity post MI.

Exercise

Heart failure

BDNF-TrkB signaling

LV

PVN

RVLM

ANA-12

A role for CRH and HPA Activation in the Regulation of Plasticity Signaling, Neuroinflammation and Emotional/Mnesic Behavior Following Global Cerebral Ischemia in Rats

Barra de la Tremblaye, Patricia

January 2016

Depression occurs in about one third of patients with stroke and cardiac arrest. Hyperactivity of the stress system is the most commonly observed neuroendocrine change in major depressive disorder (MDD), which involves elevated levels in the cerebrospinal fluid of corticotropin-releasing hormone (CRH), a key stress neurohormone. Substantial evidence suggests that normalization of the stress system may be a requirement for successful treatment of MDD through region-specific changes in the mesocorticolimbic circuitry. Thus, alteration in the stress system may underlie the emotional and functional impairments observed following brain ischemic events. In addition, recent findings suggest that ischemic brain injury triggers a restorative process, creating a cerebral environment similar to that of early brain development, a period characterized by rapid neuronal growth and neuroplasticity, critical to optimize functional recovery of individuals post stroke. In particular brain-derived neurotrophic factor (BDNF), has been shown to play an important role in the pathophysiology of major depression and cerebral ischemia. However, whether CRH can mediate the expression of BDNF in the reparative process triggered by ischemic injury remains to be characterized. Therefore, the purpose of the current thesis is to characterize the effect of pharmacological blockade of CRH signaling at the onset of a global ischemic stroke, on emotional and cognitive behaviors, alteration in the neuroendocrine stress system, and markers of neuroplasticity including BDNF. To do this, an animal model of global cerebral ischemia with subsequent behavioral testing and postmortem brain analysis was used to determine underlying biochemical and behavioral changes modulated by CRH signaling following brain ischemia. This doctoral work will help elucidate the relationship between CRH and BDNF in the context of cerebral ischemia, and may provide insights for therapies targeting the stress system. These studies address considerations such as: the interplay between stress, neuroplasticity and emotionality, and whether global ischemia can affect mood via changes in the HPA axis response.

Global cerebral ischemia

Corticotropin releasing hormone

BDNF/TrkB

HPA dysregulation

Anxiety

Depression

Sociability

Learning & Memory

Neuroprotection

Neuroinflammation

Participação da via NMDA-NO do córtex pré-frontal medial ventral na modulação das consequências comportamentais do estresse de nado forçado: mecanismos intracelulares / Participation of NMDA-NO pathway from the medial préfrontal córtex on the behavioural consequences of forced swim stress: molecular mechanisms

Pereira, Vitor Silva

17 April 2015

PEREIRA, V.S. Participação da via NMDA-NO do córtex pré-frontal medial ventral na modulação das consequências comportamentais do estresse de nado forçado: mecanismos intracelulares. 2015. 191p. Tese (Doutorado) Faculdade de Medicina de Ribeirão Preto, Universidade de São Paulo, Ribeirão Preto, 2014. A ativação dos receptores glutamatérgicos do tipo NMDA é capaz de desencadear a síntese de óxido nítrico (NO) no SNC. A administração de antagonistas NMDA (p.ex., ketamina) ou de inibidores da síntese de NO (p.ex., 7-NI) produz efeitos do tipo antidepressivo em animais e reforça o potencial dos sistemas glutamatérgico e nitrérgico como alvos terapêuticos para o tratamento da depressão. Trabalhos recentes sugerem o envolvimento de vias intracelulares no controle de mecanismos de plasticidade neural, como a via BDNF-TrkBmTOR, nos efeitos antidepressivos produzidos por antagonistas NMDA. Foi demonstrado, por exemplo, que os efeitos antidepressivos da ketamina dependem da síntese de BDNF e da ativação da mTOR no córtex pré-frontal medial (CPFMv) de ratos. O bloqueio farmacológico do CPFMv ou a administração de antagonista NMDA (LY235959) nessa estrutura também produz efeitos do tipo antidepressivo em animais. Porém, não se sabe se esses efeitos envolvem a via NMDA-NO do CPFMv, assim como não se sabe se o efeito antidepressivo induzido por inibidores da síntese de NO dependeria da via BDNF-TrkB-mTOR do CPFMv. Dessa forma, avaliamos a participação da neurotransmissão glutamatérgica e nitrérgica, bem como a participação da via BDNF-TrkB-mTOR, no CPFMv-pré límbico (PL), na modulação de respostas comportamentais de animais submetidos ao teste do nado forçado (TNF), um teste preditivo de efeito antidepressivo. Em um primeiro grupo de experimentos observou-se que a administração de inibidor da nNOS (NPA), da sGC (ODQ) ou de sequestrador de NO (c-PTIO) no PL de animais submetidos ao TNF promoveu efeito do tipo-antidepressivo, de forma similar ao que foi previamente descrito com a injeção local de LY235959. Posteriormente, os efeitos do LY235959, mas não os do NPA, foram bloqueados pelo tratamento prévio com antagonista dos receptores glutamatérgicos do tipo AMPA (NBQX), sugerindo que as vias NMDA e NO do PL estejam dissociadas na modulação das alterações comportamentais promovidas pelo TNF. A administração de BDNF no PL promoveu efeito tipoantidepressivo, o qual foi bloqueado pelo pré-tratamento com antagonista dos receptores TrkB (K252a) ou com inibidor da mTOR (rapamicina). Os efeitos tipo antidepressivo da administração de LY235959 ou NPA, no PL, não foram alterados na presença de K252a. No entanto, a administração prévia de rapamicina foi capaz de bloquear os efeitos do LY235959, mas não os do NPA, novamente sugerindo mecanismos distintos desencadeados por NMDA e NO no PL. Nossos dados indicam uma interação maior dos efeitos dos antagonistas NMDA com a via BDNF-TrkB-mTOR, enquanto os efeitos dos inibidores da via do NO parecem não modular essa via no PL. O tratamento sistêmico com ketamina (antagonista NMDA) ou 7-NI (inibidor preferencial da nNOS) foi capaz de produzir efeitos do tipo antidepressivo, sendo que esses tratamentos não alteraram a ativação ou expressão dos receptores TrkB e da mTOR, no CPFm de animais estressados ou não estressados. Assim, mais estudos são necessários para esclarecer a interação das neurotransmissões glutamatérgica e nitrérgica com a via BDNFTrkB-mTOR, no CPFMv-PL, no que diz respeito ao efeito antidepressivo em animais estressados, após administração sistêmica. Em conjunto, os dados do presente trabalho suportam o envolvimento da neurotransmissao glutamatérgica e nitrérgica do PL na neurobiologia das respostas comportamentais associadas a neurobiologia da depressão. Porém, a interação entre esses sistemas no PL e os mecanismos envolvidos se mostram consideravelmente complexos. / PEREIRA, V.S. Participation of NMDA-NO pathway from the medial préfrontal córtex on the behavioural consequences of forced swim stress: molecular mechanisms. 2015. 191p. Thesis (Doctoral) School of Medicine of Ribeirão Preto, University of São Paulo, Ribeirão Preto, 2014. The activation of NMDA receptors is capable of increasing nitric oxide (NO) synthesis in the brain. The administration of NMDA antagonists (e.g., ketamine) or nitric oxide synthesis inhibitors (e.g., 7-NI) produce antidepressant-like effects in animals and highlights the potential of glutamatergic and nitrergic systems as therapeutic targets for the treatment of major depression. The involvement of intracellular mechanisms associated to neural plasticity, such as BDNF-TrkBmTOR pathway, has been implicated in the antidepressant-like effects induced by systemic administration of NMDA antagonists. For instance, the antidepressant effects of ketamine are associated with increased BDNF synthesis and mTOR in the medial prefrontal cortex (vMPFC). In addition, injection of an NMDA antagonist (LY235959) into the vMPFC-PL produces antidepressant-like effect in animals. However, it is not yet known if the aforementioned antidepressant-like effects involve the modulation of NO synthesis or the activation of the BDNF-TrkB-mTOR pathway in the vMPFC. Therefore, this work investigated the involvement of glutamatergic and nitrergic neurotransmission of the vMPFC, as well as the participation of local BDNF-TrkBmTOR pathway, in the modulation of behavioral responses of animals submitted to forced swimming test, an animal model predictive of antidepressant effects. The administration of nNOS inhibitor (NPA), sGC inhibitor (ODQ) or NO scavenger (c-PTIO) into the vMPFC-PL produced antidepressant-like effects, similarly to what has been previously described with the local injection of LY235959. The effects of LY235959 were blocked by pretreatment with an antagonist of AMPA receptors (NBQX), but not the NPA effects. Thus suggesting a possible dissociation between NMDA- and NO-induced mechanism in the PL. BDNF administration in the PL induced antidepressant-like effect, which was blocked by prior administration of the TrkB receptor antagonist (K252a) or the mTOR inhibitor (rapamycin). The antidepressant-like effects induced by intra-PL administration of LY235959 and NPA, into vMPFC-PL were not altered in the presence of K252a. However, the prior administration of rapamycin was able to block the effects of LY235959, but not NPA-induced effect. This result further supports the dissociation of the NMDA-NO system in the PL in the modulation of immobility in the FST. Systemic treatment with ketamine (NMDA antagonist) or 7-NI (nNOS inhibitor) produced antidepressant-like effects in the FST, although these treatments did not affect the activation or the expression of TrkB receptors or mTOR in the MPFC of stressed animals. These results further corroborate the involvement of the glutamatergic and nitrergic neurotransmission in the modulation of behavioral consequences of the forced swim stress and highlight that the interaction of these systems with mTOR and trkB in the PL is considerably complex. Altogether, our data supports the possible modulation of BDNF-TrkBmTOR pathway of the PL in the effects induced by NMDA antagonist injection.. However, the effects induced by inhibitors of the NO pathway semms dissociated from an interaction with the aforementioned pathway. Thus, further studies are necessary to clarify the interaction of glutamatergic and nitrergic neurotransmission with BDNF-TrkB-mTOR pathway into vMPFC-PL regarding the neurobiology of stress and depression.

BDNF

BDNF, TrKB

Behavior

Comportamento

Córtex pré-frontal medial ventral

Depressão

Depression

Forced Swim.

Glutamate

Glutamato

mTOR

mTOR Ventral Medial Prefrontal Córtex

Nado forçado.

Nitric oxide

Óxido nítrico

TrkB

Participação da via NMDA-NO do córtex pré-frontal medial ventral na modulação das consequências comportamentais do estresse de nado forçado: mecanismos intracelulares / Participation of NMDA-NO pathway from the medial préfrontal córtex on the behavioural consequences of forced swim stress: molecular mechanisms

Vitor Silva Pereira

17 April 2015

PEREIRA, V.S. Participação da via NMDA-NO do córtex pré-frontal medial ventral na modulação das consequências comportamentais do estresse de nado forçado: mecanismos intracelulares. 2015. 191p. Tese (Doutorado) Faculdade de Medicina de Ribeirão Preto, Universidade de São Paulo, Ribeirão Preto, 2014. A ativação dos receptores glutamatérgicos do tipo NMDA é capaz de desencadear a síntese de óxido nítrico (NO) no SNC. A administração de antagonistas NMDA (p.ex., ketamina) ou de inibidores da síntese de NO (p.ex., 7-NI) produz efeitos do tipo antidepressivo em animais e reforça o potencial dos sistemas glutamatérgico e nitrérgico como alvos terapêuticos para o tratamento da depressão. Trabalhos recentes sugerem o envolvimento de vias intracelulares no controle de mecanismos de plasticidade neural, como a via BDNF-TrkBmTOR, nos efeitos antidepressivos produzidos por antagonistas NMDA. Foi demonstrado, por exemplo, que os efeitos antidepressivos da ketamina dependem da síntese de BDNF e da ativação da mTOR no córtex pré-frontal medial (CPFMv) de ratos. O bloqueio farmacológico do CPFMv ou a administração de antagonista NMDA (LY235959) nessa estrutura também produz efeitos do tipo antidepressivo em animais. Porém, não se sabe se esses efeitos envolvem a via NMDA-NO do CPFMv, assim como não se sabe se o efeito antidepressivo induzido por inibidores da síntese de NO dependeria da via BDNF-TrkB-mTOR do CPFMv. Dessa forma, avaliamos a participação da neurotransmissão glutamatérgica e nitrérgica, bem como a participação da via BDNF-TrkB-mTOR, no CPFMv-pré límbico (PL), na modulação de respostas comportamentais de animais submetidos ao teste do nado forçado (TNF), um teste preditivo de efeito antidepressivo. Em um primeiro grupo de experimentos observou-se que a administração de inibidor da nNOS (NPA), da sGC (ODQ) ou de sequestrador de NO (c-PTIO) no PL de animais submetidos ao TNF promoveu efeito do tipo-antidepressivo, de forma similar ao que foi previamente descrito com a injeção local de LY235959. Posteriormente, os efeitos do LY235959, mas não os do NPA, foram bloqueados pelo tratamento prévio com antagonista dos receptores glutamatérgicos do tipo AMPA (NBQX), sugerindo que as vias NMDA e NO do PL estejam dissociadas na modulação das alterações comportamentais promovidas pelo TNF. A administração de BDNF no PL promoveu efeito tipoantidepressivo, o qual foi bloqueado pelo pré-tratamento com antagonista dos receptores TrkB (K252a) ou com inibidor da mTOR (rapamicina). Os efeitos tipo antidepressivo da administração de LY235959 ou NPA, no PL, não foram alterados na presença de K252a. No entanto, a administração prévia de rapamicina foi capaz de bloquear os efeitos do LY235959, mas não os do NPA, novamente sugerindo mecanismos distintos desencadeados por NMDA e NO no PL. Nossos dados indicam uma interação maior dos efeitos dos antagonistas NMDA com a via BDNF-TrkB-mTOR, enquanto os efeitos dos inibidores da via do NO parecem não modular essa via no PL. O tratamento sistêmico com ketamina (antagonista NMDA) ou 7-NI (inibidor preferencial da nNOS) foi capaz de produzir efeitos do tipo antidepressivo, sendo que esses tratamentos não alteraram a ativação ou expressão dos receptores TrkB e da mTOR, no CPFm de animais estressados ou não estressados. Assim, mais estudos são necessários para esclarecer a interação das neurotransmissões glutamatérgica e nitrérgica com a via BDNFTrkB-mTOR, no CPFMv-PL, no que diz respeito ao efeito antidepressivo em animais estressados, após administração sistêmica. Em conjunto, os dados do presente trabalho suportam o envolvimento da neurotransmissao glutamatérgica e nitrérgica do PL na neurobiologia das respostas comportamentais associadas a neurobiologia da depressão. Porém, a interação entre esses sistemas no PL e os mecanismos envolvidos se mostram consideravelmente complexos. / PEREIRA, V.S. Participation of NMDA-NO pathway from the medial préfrontal córtex on the behavioural consequences of forced swim stress: molecular mechanisms. 2015. 191p. Thesis (Doctoral) School of Medicine of Ribeirão Preto, University of São Paulo, Ribeirão Preto, 2014. The activation of NMDA receptors is capable of increasing nitric oxide (NO) synthesis in the brain. The administration of NMDA antagonists (e.g., ketamine) or nitric oxide synthesis inhibitors (e.g., 7-NI) produce antidepressant-like effects in animals and highlights the potential of glutamatergic and nitrergic systems as therapeutic targets for the treatment of major depression. The involvement of intracellular mechanisms associated to neural plasticity, such as BDNF-TrkBmTOR pathway, has been implicated in the antidepressant-like effects induced by systemic administration of NMDA antagonists. For instance, the antidepressant effects of ketamine are associated with increased BDNF synthesis and mTOR in the medial prefrontal cortex (vMPFC). In addition, injection of an NMDA antagonist (LY235959) into the vMPFC-PL produces antidepressant-like effect in animals. However, it is not yet known if the aforementioned antidepressant-like effects involve the modulation of NO synthesis or the activation of the BDNF-TrkB-mTOR pathway in the vMPFC. Therefore, this work investigated the involvement of glutamatergic and nitrergic neurotransmission of the vMPFC, as well as the participation of local BDNF-TrkBmTOR pathway, in the modulation of behavioral responses of animals submitted to forced swimming test, an animal model predictive of antidepressant effects. The administration of nNOS inhibitor (NPA), sGC inhibitor (ODQ) or NO scavenger (c-PTIO) into the vMPFC-PL produced antidepressant-like effects, similarly to what has been previously described with the local injection of LY235959. The effects of LY235959 were blocked by pretreatment with an antagonist of AMPA receptors (NBQX), but not the NPA effects. Thus suggesting a possible dissociation between NMDA- and NO-induced mechanism in the PL. BDNF administration in the PL induced antidepressant-like effect, which was blocked by prior administration of the TrkB receptor antagonist (K252a) or the mTOR inhibitor (rapamycin). The antidepressant-like effects induced by intra-PL administration of LY235959 and NPA, into vMPFC-PL were not altered in the presence of K252a. However, the prior administration of rapamycin was able to block the effects of LY235959, but not NPA-induced effect. This result further supports the dissociation of the NMDA-NO system in the PL in the modulation of immobility in the FST. Systemic treatment with ketamine (NMDA antagonist) or 7-NI (nNOS inhibitor) produced antidepressant-like effects in the FST, although these treatments did not affect the activation or the expression of TrkB receptors or mTOR in the MPFC of stressed animals. These results further corroborate the involvement of the glutamatergic and nitrergic neurotransmission in the modulation of behavioral consequences of the forced swim stress and highlight that the interaction of these systems with mTOR and trkB in the PL is considerably complex. Altogether, our data supports the possible modulation of BDNF-TrkBmTOR pathway of the PL in the effects induced by NMDA antagonist injection.. However, the effects induced by inhibitors of the NO pathway semms dissociated from an interaction with the aforementioned pathway. Thus, further studies are necessary to clarify the interaction of glutamatergic and nitrergic neurotransmission with BDNF-TrkB-mTOR pathway into vMPFC-PL regarding the neurobiology of stress and depression.

BDNF, TrKB

Comportamento

Córtex pré-frontal medial ventral

Depressão

Glutamato

mTOR

Nado forçado.

Óxido nítrico

BDNF

Behavior

Depression

Forced Swim.

Glutamate

mTOR Ventral Medial Prefrontal Córtex

Nitric oxide

TrkB