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1. Moderators of ayahuasca’s biological antidepressant action

Author: Geovan Menezes de Sousa, Vagner Deuel de Oliveira Tavares, Ana Cecília de Menezes Galvão, Raíssa Nóbrega de Almeida, Fernanda Palhano-Fontes, Bruno Lobão-Soares, Fúlvio Aurélio de Morais Freire, Emerson Arcoverde Nunes, João Paulo Maia-de-Oliveira, Daniel Perkins, Jerome Sarris, Dráulio Barros de Araujo, and Nicole Leite Galvão-Coelho
Subjects: psychedelics, cortisol, BDNF, inflammation, depression, Psychiatry, RC435-571
Abstract: IntroductionThe understanding of biological responses to psychedelics with antidepressant potential is imperative. Here we report how a set of acute parameters, namely emotional (depressive symptoms), cognitive (psychedelic experience), and physiological (salivary cortisol), recorded during an ayahuasca dosing session, modulated serum brain-derived neurotrophic factor (BDNF), serum cortisol (SC), serum interleukin 6 (IL-6), plasma C-reactive protein (CRP), and salivary cortisol awakening response (CAR).MethodsResults were analyzed 2 days after the psychedelic intervention (ayahuasca) versus placebo in both patients with treatment-resistant depression and healthy volunteers. These measures were assessed as part of a randomized double-blinded, placebo-controlled trial (n = 72).ResultsResults revealed that larger reductions of depressive symptoms during the dosing session significantly moderated higher levels of SC in patients. Whereas lesser changes in salivary cortisol levels during the ayahuasca intervention were related to higher BDNF levels in patients with a larger clinical response in the reduction in depressive symptoms. No moderator was found for patient’s CAR, IL-6, and CRP responses to ayahuasca and for all biomarker responses to ayahuasca in healthy controls and in the placebo group.DiscussionIn summary, some specific emotional and physiological parameters during experimental ayahuasca session were revealed as critical moderators of the improvement of major depression biomarkers, mainly BDNF and SC two days after ayahuasca intake. These findings contribute to paving the way for future studies investigating the biological antidepressant response to psychedelic therapy.
Published: 2022
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2. Pathophysiology of Major Depression by Clinical Stages

Author: Ana Cecília de Menezes Galvão, Raíssa Nobrega Almeida, Geovan Menezes de Sousa, Mario André Leocadio-Miguel, Fernanda Palhano-Fontes, Dráulio Barros de Araujo, Bruno Lobão-Soares, João Paulo Maia-de-Oliveira, Emerson Arcoverde Nunes, Jaime Eduardo Cecilio Hallak, Felipe Barreto Schuch, Jerome Sarris, and Nicole Leite Galvão-Coelho
Subjects: cortisol, C-reactive protein, brain-derived neurotrophic factor, sleep quality, precision psychiatry, Psychology, BF1-990
Abstract: The comprehension of the pathophysiology of the major depressive disorder (MDD) is essential to the strengthening of precision psychiatry. In order to determine the relationship between the pathophysiology of the MDD and its clinical progression, analyzed by severity of the depressive symptoms and sleep quality, we conducted a study assessing different peripheral molecular biomarkers, including the levels of plasma C-reactive protein (CRP), serum mature brain-derived neurotrophic factor (mBDNF), serum cortisol (SC), and salivary cortisol awakening response (CAR), of patients with MDD (n = 58) and a control group of healthy volunteers (n = 62). Patients with the first episode of MDD (n = 30) had significantly higher levels of CAR and SC than controls (n = 32) and similar levels of mBDNF of controls. Patients with treatment-resistant depression (TRD, n = 28) presented significantly lower levels of SC and CAR, and higher levels of mBDNF and CRP than controls (n = 30). An increased severity of depressive symptoms and worse sleep quality were correlated with levels low of SC and CAR, and with high levels of mBDNF. These results point out a strong relationship between the stages clinical of MDD and changes in a range of relevant biological markers. This can assist in the development of precision psychiatry and future research on the biological tests for depression.
Published: 2021
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3. Potential biomarkers of major depression diagnosis and chronicity.

Author: Ana Cecília de Menezes Galvão, Raíssa Nobrega Almeida, Geovan Menezes de Sousa Júnior, Mário André Leocadio-Miguel, Fernanda Palhano-Fontes, Dráulio Barros de Araujo, Bruno Lobão-Soares, João Paulo Maia-de-Oliveira, Emerson Arcoverde Nunes, Jaime Eduardo Cecilio Hallak, Jerome Sarris, and Nicole Leite Galvão-Coelho
Subjects: Medicine, Science
Abstract: BackgroundMolecular biomarkers are promising tools to be routinely used in clinical psychiatry. Among psychiatric diseases, major depression disorder (MDD) has gotten attention due to its growing prevalence and morbidity.MethodsWe tested some peripheral molecular parameters such as serum mature Brain-Derived Neurotrophic Factor (mBDNF), plasma C-Reactive Protein (CRP), serum cortisol (SC), and the salivary Cortisol Awakening Response (CAR), as well as the Pittsburgh sleep quality inventory (PSQI), as part of a multibiomarker panel for potential use in MDD diagnosis and evaluation of disease's chronicity using regression models, and ROC curve.ResultsFor diagnosis model, two groups were analyzed: patients in the first episode of major depression (MD: n = 30) and a healthy control (CG: n = 32). None of those diagnosis models tested had greater power than Hamilton Depression Rating Scale-6. For MDD chronicity, a group of patients with treatment-resistant major depression (TRD: n = 28) was tested across the MD group. The best chronicity model (p < 0.05) that discriminated between MD and TRD included four parameters, namely PSQI, CAR, SC, and mBDNF (AUC ROC = 0.99), with 96% of sensitivity and 93% of specificity.ConclusionThese results indicate that changes in specific biomarkers (CAR, SC, mBDNF and PSQI) have potential on the evaluation of MDD chronicity, but not for its diagnosis. Therefore, these findings can contribute for further studies aiming the development of a stronger model to be commercially available and used in psychiatry clinical practice.
Published: 2021
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4. Changes in Cortisol but Not in Brain-Derived Neurotrophic Factor Modulate the Association Between Sleep Disturbances and Major Depression

Author: Giuliana Travassos Pires Santiago, Ana Cecília de Menezes Galvão, Raíssa Nóbrega de Almeida, Sergio Arthuro Mota-Rolim, Fernanda Palhano-Fontes, João Paulo Maia-de-Oliveira, Dráulio Barros de Araújo, Bruno Lobão-Soares, and Nicole Leite Galvão-Coelho
Subjects: pittsburgh sleep quality index, brain-derived neurotrophic factor, salivary cortisol awakening response, sleep disturbance, treatment-resistant depression, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract: Sleep disturbance is a symptom consistently found in major depression and is associated with a longer course of illness, reduced response to treatment, increased risk of relapse and recurrence. Chronic insomnia has been associated with changes in cortisol and serum brain-derived neurotrophic factor (BDNF) levels, which in turn are also changed in major depression. Here, we evaluated the relationship between sleep quality, salivary cortisol awakening response (CAR), and serum BDNF levels in patients with sleep disturbance and treatment-resistant major depression (n = 18), and in a control group of healthy subjects with good (n = 21) and poor (n = 18) sleep quality. We observed that the patients had the lowest CAR and sleep duration of all three groups and a higher latency to sleep than the healthy volunteers with a good sleep profile. Besides, low CAR was correlated with more severe depressive symptoms and worse sleep quality. There was no difference in serum BDNF levels between groups with distinct sleep quality. Taken together, our results showed a relationship between changes in CAR and in sleep quality in patients with treatment-resistant depression, which were correlated with the severity of disease, suggesting that cortisol could be a physiological link between sleep disturbance and major depression.
Published: 2020
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5. Modulation of Serum Brain-Derived Neurotrophic Factor by a Single Dose of Ayahuasca: Observation From a Randomized Controlled Trial

Author: Raíssa Nóbrega de Almeida, Ana Cecília de Menezes Galvão, Flávia Santos da Silva, Erick Allan dos Santos Silva, Fernanda Palhano-Fontes, João Paulo Maia-de-Oliveira, Lobão-Soares Barros de Araújo, Bruno Lobão-Soares, and Nicole Leite Galvão-Coelho
Subjects: ayahuasca, antidepressant, BDNF, biomarker, cortisol, depression, Psychology, BF1-990
Abstract: Serotonergic psychedelics are emerging as potential antidepressant therapeutic tools, as suggested in a recent randomized controlled trial with ayahuasca for treatment-resistant depression. Preclinical and clinical studies have suggested that serum brain-derived neurotrophic factor (BDNF) levels increase after treatment with serotoninergic antidepressants, but the exact role of BDNF as a biomarker for diagnostic and treatment of major depression is still poorly understood. Here we investigated serum BDNF levels in healthy controls (N = 45) and patients with treatment-resistant depression (N = 28) before (baseline) and 48 h after (D2) a single dose of ayahuasca or placebo. In our sample, baseline serum BDNF levels did not predict major depression and the clinical characteristics of the patients did not predict their BDNF levels. However, at baseline, serum cortisol was a predictor of serum BDNF levels, where lower levels of serum BDNF were detected in a subgroup of subjects with hypocortisolemia. Moreover, at baseline we found a negative correlation between BDNF and serum cortisol in volunteers with eucortisolemia. After treatment (D2) we observed higher BDNF levels in both patients and controls that ingested ayahuasca (N = 35) when compared to placebo (N = 34). Furthermore, at D2 just patients treated with ayahuasca (N = 14), and not with placebo (N = 14), presented a significant negative correlation between serum BDNF levels and depressive symptoms. This is the first double-blind randomized placebo-controlled clinical trial that explored the modulation of BDNF in response to a psychedelic in patients with depression. The results suggest a potential link between the observed antidepressant effects of ayahuasca and changes in serum BDNF, which contributes to the emerging view of using psychedelics as an antidepressant. This trial is registered at http://clinicaltrials.gov (NCT02914769).
Published: 2019
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6. Nitric oxide plasma/serum levels in patients with schizophrenia: a systematic review and meta-analysis Níveis plasmáticos/séricos do óxido nítrico em pacientes com esquizofrenia: uma revisão sistemática e metanálise

Author: João Paulo Maia-de-Oliveira, Clarissa Trzesniak, Irismar R. Oliveira, Matthew J. Kempton, Tatiana M. N. de Rezende, Sandro Iego, Glen B. Baker, Serdar M. Dursun, João Paulo Machado-de-Sousa, and Jaime E. C. Hallak
Subjects: Óxido nítrico, Esquizofrenia, Psicose, Níveis plasmáticos, Níveis séricos, Metanálise, Revisão sistemática, Nitric Oxide, Schizophrenia, Psychosis, Plasma levels, Serum levels, Meta-analysis, Systematic review, Psychiatry, RC435-571
Abstract: For the last 40 years, schizophrenia has been considered to be the result primarily of a dysfunction in brain dopaminergic pathways. In this review, it is described and discussed findings concerning nitric oxide-mediated neurotransmission in schizophrenia. Studies were searched in PubMed, SciELO, and LILACS using the terms schizophrenia and nitric oxide plasma levels or nitric oxide serum levels, with no time limit. The reference lists of selected articles were also hand-searched for additional articles. From 15 potential reports, 10 were eligible to be included in the review and meta-analysis. These studies included a total of 505 patients with schizophrenia and 339 healthy volunteers. No significant difference was found between patients and healthy controls regarding total nitrite plasma/serum levels (effect size g = 0.285, 95%CI = -0.205 to 0.774, p = 0.254). However, when studies with patients under antipsychotic treatment were examined separately, there was a significant difference between patients and healthy volunteers (effect size g = 0.663, 95%CI = 0.365 to 0.961, p < 0.001), showing that patients under treatment have higher levels of plasma/serum nitric oxide than controls. These results suggest that antipsychotics increase nitric oxide plasma/serum levels and that the nitrergic pathway would be a fertile target for the development of new treatments for patients with schizophrenia.Durante os últimos 40 anos, a esquizofrenia foi considerada, principalmente, como o resultado de disfunções dopaminérgicas no cérebro. Esta revisão descreve e discute algumas descobertas sobre a neurotransmissão mediada pelo óxido nítrico na esquizofrenia. A busca foi feita nas bases PubMed, SciELO e LILACS usando-se os termos schizophrenia e nitric oxide plasma levels ou nitric oxide serum levels, sem limites de tempo. As listas de referências dos artigos selecionados foram examinadas em busca de outras publicações pertinentes. Dentre 15 artigos passíveis de serem incluídos, 10 preenchiam os critérios estabelecidos para a revisão e metanálise. Esses estudos incluíram 505 pacientes com esquizofrenia e 339 voluntários saudáveis. Não foram encontradas diferenças significativas entre pacientes e voluntários saudáveis quanto aos níveis plasmáticos de nitrito total (effect size g = 0,285, IC 95% = -0,205 a 0,774, p = 0,254). No entanto, o exame separado dos estudos envolvendo pacientes em tratamento antipsicótico apresentou diferenças significativas entre pacientes e voluntários saudáveis (effect size g = 0,663, IC 95% = 0,365 to 0,961, p < 0,001), demonstrando que pacientes em tratamento possuem níveis plasmáticos mais altos de óxido nítrico. Esses resultados sugerem que os antipsicóticos podem aumentar os níveis plasmáticos de óxido nítrico e que a via nitrérgica (e sua estimulação) constituiria um alvo propício para o desenvolvimento de novos tratamentos para pacientes com esquizofrenia.
Published: 2012

7. Why we should use long-acting injectable antipsychotics more frequently

Author: João Paulo Maia-de-Oliveira, Rodrigo A. Bressan, Helio Elkis, João Paulo Machado-de-Sousa, and Jaime E.C. Hallak
Subjects: Psychiatry, RC435-571
Published: 2013
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8. Psychophysiological responses to group cognitive-behavioral therapy in depressive patients

Author: João Paulo Maia-de-Oliveira, Bruno Lobão-Soares, Mario André Leocadio-Miguel, Neuciane Gomes da Silva, Geovan Menezes de Sousa, Yves Martins Varela, Nicole Leite Galvão-Coelho, Raíssa Nóbrega de Almeida, Ana Cecília Lopes de Lima, Ana Cecília de Menezes Galvão, and Jaime Eduardo Cecílio Hallak
Subjects: medicine.medical_specialty, medicine.medical_treatment, 05 social sciences, 050109 social psychology, medicine.disease, 050105 experimental psychology, Cognitive behavioral therapy, Internal medicine, Healthy control, medicine, Major depressive disorder, Anxiety, 0501 psychology and cognitive sciences, medicine.symptom, Trial registration, Psychology, General Psychology, Serum cortisol, After treatment, Salivary cortisol
Abstract: Cognitive-Behavioral Therapy (CBT) has a significant adjunctive effect in the treatment of Major Depressive Disorder (MDD), however its use as monotherapy in group-based approaches is less explored. We assessed the responses of distinct psychophysiological domains after a group-based CBT (gCBT, 16 weeks) intervention in drug-free patients with mild-moderate MDD (n = 20; women = 11) and compared them with a healthy control group (n = 25, women = 13). The treatment resulted in 65% of response and 55% of remission rates. Significant reductions in depressive and anxiety symptoms and increase in self-esteem and sleep quality were observed as gCBT responses. Moreover, after treatment, patients regulated their previously deregulated salivary cortisol awakening response and sleep quality toward healthy parameters. These improvements were correlated among themselves and dependent of remission outcome. Remitted patients showed larger improvements than non-remitted for all psychophysiological domains, except for serum cortisol that significantly changed only for no-remitted patients after gCBT but did not reached controls levels. Further, better baseline sleep quality was predictor of remission. The psychophysiological changes found support the use of gCBT as monotherapy treatment for mild-moderate MDD, corroborate the importance of the observation of the patients in theirs whole sociopsychophysiological condition since they are related to remission outcome and then stimulate further studies of validation of clinical protocols that work on all of these psychophysiological domains studied. Trial Registration U1111–1215-4472. Registered 21 August 2018, http://www.ensaiosclinicos.gov.br/rg/RBR-3npbf8/
Published: 2021

9. Author response for 'Psychosis in <scp>NUS1</scp> de novo mutation: New phenotypical presentation'

Author: Pedro Fraiman, João Paulo Maia-de-Oliveira, Clecio Godeiro-Junior, and Manuel Moreira-Neto
Subjects: Genetics, Psychosis, business.industry, medicine, De novo mutation, Presentation (obstetrics), medicine.disease, business, Phenotype
Published: 2020

10. Changes in inflammatory biomarkers are related to the antidepressant effects of Ayahuasca

Author: Daniel Perkins, Ana Cecília de Menezes Galvão, Dráulio Barros de Araújo, Bruno Lobão Soares, Jerome Sarris, Raíssa Nóbrega de Almeida, João Paulo Maia-de-Oliveira, Isaac Campos Braga, Nicole Leite Galvão-Coelho, and Fernanda Palhano-Fontes
Subjects: Adult, Male, Treatment outcome, 03 medical and health sciences, Depressive Disorder, Treatment-Resistant, 0302 clinical medicine, Double-Blind Method, Medicine, Humans, Pharmacology (medical), Pharmacology, Inflammation, Psychiatric Status Rating Scales, Depressive Disorder, Major, Banisteriopsis, biology, Traditional medicine, business.industry, Ayahuasca, medicine.disease, biology.organism_classification, Inflammatory biomarkers, Antidepressive Agents, 030227 psychiatry, Clinical neurology, Psychiatry and Mental health, Treatment Outcome, Case-Control Studies, Psychiatric status rating scales, Antidepressant, Female, Plant Preparations, business, Treatment-resistant depression, 030217 neurology & neurosurgery, Biomarkers
Abstract: Background: Ayahuasca is a traditional Amazon brew and its potential antidepressant properties have recently been explored in scientific settings. We conducted a double-blind placebo-controlled trial of ayahuasca with treatment-resistant depression patients ( n = 28) and healthy controls ( n = 45). Aims: We are evaluating the blood inflammatory biomarkers: C-reactive protein and interleukin 6, as a potential consequence of ayahuasca intake and their correlation with serum cortisol and brain-derived neurotrophic factor levels. Blood samples were collected at pre-treatment and 48 hours after substance ingestion to assess the concentration of inflammatory biomarkers, together with administration of the Montgomery-Åsberg Depression Rating Scale. Results: At pre-treatment, patients showed higher C-reactive protein levels than healthy controls and a significant negative correlation between C-reactive protein and serum cortisol levels was revealed ( rho = –0.40, n = 14). C-reactive protein in those patients was not correlated with Montgomery-Åsberg Depression Rating Scale scores. We observed a significant reduction of C-reactive protein levels across time in both patients and controls treated with ayahuasca, but not with placebo. Patients treated with ayahuasca showed a significant correlation ( rho = + 0.57) between larger reductions of C-reactive protein and lower depressive symptoms at 48 hours after substance ingestion (Montgomery-Åsberg Depression Rating Scale). No significant result with respect to interleukin 6 and brain-derived neurotrophic factor was found. Furthermore, these biomarkers did not predict the antidepressant response or remission rates observed. Conclusions: These findings enhance the understanding of the biological mechanisms behind the observed antidepressant effects of ayahuasca and encourage further clinical trials in adults with depression.
Published: 2020

11. Suicide by jumping from high places in a Brazilian city: regional peculiarities as a determining factor of variation in suicide methods

Author: Gustavo X Fernandes, João Paulo Maia-de-Oliveira, Emerson Arcoverde Nunes, and Amannda Melo de Oliveira Lima
Subjects: Psychiatry, Time Factors, RC435-571, MEDLINE, medicine.disease_cause, Letters to the Editors, Suicide, Psychiatry and Mental health, Suicide methods, Variation (linguistics), Geography, Jumping, Risk Factors, medicine, Humans, Built Environment, Cities, Brazil, Demography
Published: 2019

12. Effects of sodium nitroprusside in the prevention of schizophrenia-like symptoms induced by ketamine – A translational double-blind study

Author: Serdar M. Dursun, Jaime Eduardo Cecílio Hallak, D. A. Prado, Antonio Waldo Zuardi, Ludmyla Kandratavicius, Acioly L.T. Lacerda, João Paulo Machado-de-Sousa, Tatiana M. N. de Rezende, Rodrigo A. Bressan, Glen B. Baker, João Abrão, and João Paulo Maia-de-Oliveira
Subjects: Psychosis, ketamine, lcsh:RC435-571, Placebo, 03 medical and health sciences, 0302 clinical medicine, Bolus (medicine), lcsh:Psychiatry, medicine, SNP, Ketamine, psychosis, sodium nitroprusside, Maintenance dose, business.industry, Nitric oxide, medicine.disease, 030227 psychiatry, schizophrenia, Psychiatry and Mental health, Anesthesia, Sodium nitroprusside, business, 030217 neurology & neurosurgery, medicine.drug, Psychopathology
Abstract: Background: Recent evidence has shown improvements in schizophrenia symptoms after the infusion of sodium nitroprusside (SNP), a nitric oxide (NO) donor. In the rat model of schizophrenia using ketamine injection, pretreatment with SNP seems to prevent behavioral changes associated with positive symptoms for up to one week. Objective: We investigated whether SNP would have preventative effects on psychogenic symptoms induced by ketamine in healthy subjects. Methods: Healthy subjects (N = 38) were assigned to distinct groups that received SNP in different doses (0.15, 0.25, and 0.5 mcg/kg/min). First, participants received an infusion of SNP or placebo over 75 minutes. After 10 minutes, they were injected for 1 minute with a bolus of 0.26 mg/kg of ketamine and a maintenance dose was started 5 minutes later, with 0.25 mg/kg/h of ketamine for 50 minutes. Results: Ketamine-induced psychopathological alterations induced were reduced by SNP, as assessed with the Brief Psychological Rating Scale. Scores in the objective subscale of the Clinician-Administered Dissociative States Scale were also lower in SNP sessions compared to placebo. SNP had protective effects against deterioration in facial emotion and identity recognition tasks induced by ketamine. Discussion: Our findings support the view that SNP has preventative properties against psychotic manifestations.
Published: 2017

13. Psychosis in <scp>NUS1</scp> de novo mutation: New phenotypical presentation

Author: João Paulo Maia-de-Oliveira, Manuel Moreira-Neto, Clecio Godeiro-Junior, and Pedro Fraiman
Subjects: Psychosis, business.industry, media_common.quotation_subject, MEDLINE, De novo mutation, medicine.disease, Bioinformatics, Phenotype, Presentation, Genetics, medicine, business, Genetics (clinical), media_common
Published: 2020

14. Rapid antidepressant effects of the psychedelic ayahuasca in treatment-resistant depression: a randomized placebo-controlled trial

Author: Gabriela de Oliveira Silveira, Antonio A. Silva-Junior, Dráulio Barros de Araújo, Katia C. Andrade, João Carlos Alchieri, Flávia de Lima Osório, Francisco Rr Santos, Bruno Lobão-Soares, Jéssica de Andrade Pessoa, Emerson Arcoverde, Jordi Riba, Nicole Leite Galvão-Coelho, Rafael Faria Sanches, Rafael Miyashiro Nunes dos Santos, João Paulo Maia-de-Oliveira, Heloisa Onias, Dayanna Barreto, Sérgio A. Mota-Rolim, Morgana M. Novaes, Fernanda Palhano-Fontes, Luís Fernando Tófoli, Jaime Eduardo Cecilio Hallak, and Mauricio Yonamine
Subjects: Hallucinogen, Adult, Male, medicine.medical_specialty, Time Factors, HRS, Placebo-controlled study, Placebo, law.invention, 03 medical and health sciences, Depressive Disorder, Treatment-Resistant, 0302 clinical medicine, Randomized controlled trial, randomized controlled trial (RCT), Double-Blind Method, Antidepressive agents, law, Internal medicine, medicine, Humans, Applied Psychology, Depression (differential diagnoses), Psychiatric Status Rating Scales, Banisteriopsis, biology, business.industry, Depression, Ayahuasca, Original Articles, psychedelics, biology.organism_classification, medicine.disease, Antidepressive Agents, 030227 psychiatry, Psychiatry and Mental health, Treatment Outcome, MEQ, depression, Randomized Controlled Trial (RCT), Hallucinogens, Female, Psychedelic, business, Treatment-resistant depression, 030217 neurology & neurosurgery, Phytotherapy
Abstract: BackgroundRecent open-label trials show that psychedelics, such as ayahuasca, hold promise as fast-onset antidepressants in treatment-resistant depression.MethodsTo test the antidepressant effects of ayahuasca, we conducted a parallel-arm, double-blind randomized placebo-controlled trial in 29 patients with treatment-resistant depression. Patients received a single dose of either ayahuasca or placebo. We assessed changes in depression severity with the Montgomery-Åsberg Depression Rating Scale (MADRS) and the Hamilton Depression Rating scale at baseline, and at 1 (D1), 2 (D2), and 7 (D7) days after dosing.ResultsWe observed significant antidepressant effects of ayahuasca when compared with placebo at all-time points. MADRS scores were significantly lower in the ayahuasca group compared with placebo at D1 and D2 (p= 0.04), and at D7 (p< 0.0001). Between-group effect sizes increased from D1 to D7 (D1: Cohen'sd= 0.84; D2: Cohen'sd= 0.84; D7: Cohen'sd= 1.49). Response rates were high for both groups at D1 and D2, and significantly higher in the ayahuasca group at D7 (64%v.27%;p= 0.04). Remission rate showed a trend toward significance at D7 (36%v.7%,p= 0.054).ConclusionsTo our knowledge, this is the first controlled trial to test a psychedelic substance in treatment-resistant depression. Overall, this study brings new evidence supporting the safety and therapeutic value of ayahuasca, dosed within an appropriate setting, to help treat depression. This study is registered athttp://clinicaltrials.gov(NCT02914769).
Published: 2018

15. An Overview of Animal Models Related to Schizophrenia

Author: Ludmyla Kandratavicius, John G. Howland, Serdar M. Dursun, Glen B. Baker, Ian R. Winship, Priscila Alves Balista, Jaime Eduardo Cecílio Hallak, and João Paulo Maia-de-Oliveira
Subjects: 0301 basic medicine, business.industry, Schizophrenia (object-oriented programming), Cognition, Disease, Brain pathologies, behavioral disciplines and activities, 03 medical and health sciences, Psychiatry and Mental health, Preclinical research, Disease Models, Animal, 030104 developmental biology, 0302 clinical medicine, Multiple Models, Endophenotype, mental disorders, MODELOS ANIMAIS DE DOENÇAS, Schizophrenia, Medicine, Animals, In Review Series Articles, business, Neuroscience, 030217 neurology & neurosurgery
Abstract: Schizophrenia is a heterogeneous psychiatric disorder that is poorly treated with current therapies. In this brief review, we provide an update regarding the use of animal models to study schizophrenia in an attempt to understand its aetiology and develop novel therapeutic strategies. Tremendous progress has been made developing and validating rodent models that replicate the aetiologies, brain pathologies, and behavioural abnormalities associated with schizophrenia in humans. Here, models are grouped into 3 categories—developmental, drug induced, and genetic—to reflect the heterogeneous risk factors associated with schizophrenia. Each of these models is associated with varied but overlapping pathophysiology, endophenotypes, behavioural abnormalities, and cognitive impairments. Studying schizophrenia using multiple models will permit an understanding of the core features of the disease, thereby facilitating preclinical research aimed at the development and validation of better pharmacotherapies to alter the progression of schizophrenia or alleviate its debilitating symptoms.
Published: 2018

16. Acute effects of ayahuasca in a juvenile non-human primate model of depression

Author: João Paulo Maia-de-Oliveira, Dráulio Barros de Araújo, Bruno Lobão-Soares, Geovan Menezes de Sousa, Jaime Eduardo Cecílio Hallak, Maria Bernardete Cordeiro de Sousa, Erick A. S. Silva, Vanessa de Paula Soares-Rachetti, Nicole Leite Galvão-Coelho, and Flávia Santos da Silva
Subjects: Male, Primates, Hydrocortisone, lcsh:RC435-571, Translational animal model, Physiology, Context (language use), non-human primate, cortisol, common marmoset, 03 medical and health sciences, Feces, 0302 clinical medicine, psychedelic drugs, lcsh:Psychiatry, FÁRMACOS SINTÉTICOS, medicine, Juvenile, Animals, Humans, Juvenile animal, Depression (differential diagnoses), Depressive Disorder, Major, marmoset, Banisteriopsis, biology, business.industry, Ayahuasca, medicine.disease, biology.organism_classification, Antidepressive Agents, early-age depression, 030227 psychiatry, Psychiatry and Mental health, Disease Models, Animal, Mood disorders, Callitrichinae, Hallucinogens, Antidepressant, Female, Original Article, business, 030217 neurology & neurosurgery
Abstract: Objective: The incidence rate of major depression in adolescents reaches approximately 14%. This disorder is usually recurrent, without remission of symptoms even after pharmacological treatment, and persists throughout adult life. Since the effects of antidepressants take approximately 2 weeks to begin, new pharmacological therapies are under continuous exploration. Recent evidence suggests that psychedelics could produce rapid antidepressant effects. In this study, we evaluated the potential antidepressant effects of ayahuasca in a juvenile non-human primate model of depression. Methods: While living with their families, juvenile marmosets (8 males; 7 females) were observed on alternate days for four weeks during a baseline phase. This was followed by 8 weeks of an induced depressive state protocol, the social isolated context (IC), in which the animals were monitored in the first and last weeks. Subsequently, five males and four females were randomly selected for treatment, first with a single administration of saline vehicle (1.67 mL/300 g of body weight, via gavage), followed by a single dose of ayahuasca (1.67 mL/300 g of body weight, via gavage). Both phases lasted 1 week and the animals were monitored daily. A third week of sampling was called the tardive-pharmacological effects phase. In all phases the marmosets were assessed for behavior, fecal cortisol levels, and body weight. Results: After IC, the animals presented typical hypocortisolemia, but cortisol recovered to baseline levels 24 h after an acute dose of ayahuasca; this recovery was not observed in vehicle-treated animals. Additionally, in males, ayahuasca, but not the vehicle, reduced scratching, a stereotypic behavior, and increased feeding. Ayahuasca treatment also improved body weight to baseline levels in both sexes. The ayahuasca-induced behavioral response had long-term effects (14 days). Thus, in this translational juvenile animal model of depression, ayahuasca presented beneficial effects. Conclusions: These results can contribute to the validation of ayahuasca as an antidepressant drug and encourage new studies on psychedelic drugs as a tool for treating mood disorders, including for adolescents with early-onset depression.
Published: 2018

17. A Single Dose Of Ayahuasca Modulates Salivary Cortisol In Treatment-Resistant Depression

Author: Heloisa Onias, Fúlvio Aurélio de Morais Freire, Bruno Lobão-Soares, Raíssa N. de Almeida, Fernanda Palhano-Fontes, João Paulo Maia-de-Oliveira, Erick Allan dos Santos Silva, Dráulio Barros de Araújo, Emerson Arcoverde, Nicole Leite Galvão-Coelho, and Ana Cecília de Menezes Galvão
Subjects: Mood, business.industry, Physiology, Medicine, Antidepressant, Ingestion, Dosing, business, medicine.disease, Ayahuasca, Placebo, Treatment-resistant depression, Depression (differential diagnoses)
Abstract: Major depression is a highly prevalent mood disorder, affecting about 350 million people, and around 30% of the patients are resistant to currently available antidepressant medications. Recent evidence from a randomized placebo-controlled trial supports the rapid antidepressant effects of the psychedelic ayahuasca in treatment-resistant depression. The aim of this study was to explore the effect of ayahuasca on plasma cortisol and awakening salivary cortisol response, in the same group of treatment-resistant patients and in healthy volunteers. Subjects received a single dose of ayahuasca or placebo, and both plasma and awakening salivary cortisol response were measured at baseline (before dosing) and 48h after the dosing session. Baseline assessment (D0) showed blunted awakening salivary cortisol response and hypocortisolemia in patients (DM), both with respect to healthy controls group (C). Salivary cortisol also was measured during dosing session and we observed a large increased for both C and DM that ingested ayahuasca, than placebo groups. After 48h of the dosing session (D2) with ayahuasca, awakening salivary cortisol response (for both sexes) of treated patients became similar to levels detected in controls. This was not observed in patients that ingested placebo. No changes in plasma cortisol were observed after 48 hours of ayahuasca or placebo ingestion for both groups and sexes. Therefore, these findings point to new evidence of modulation of ayahuasca on salivary cortisol levels, as cortisol acts in regulation of distinct physiological pathways, emotional and cognitive processes related to etiology of depression, this modulation could be an important part of the antidepressant effects observed with ayahuasca. Moreover, this study highlights the importance of psychedelics in the treatment of human mental disorders.
Published: 2018

18. Acute antidepressant effect of ayahuasca in juvenile non-human primate model of depression

Author: Maria Bernardete Cordeiro de Sousa, Bruno Lobão Soares, João Paulo Maia-de-Oliveira, Vanessa de Paula Soares Rachetti, Geovan Menezes de Sousa Júnior, Flávia Santos da Silva, Dráulio Barros de Araújo, Erick Allan dos Santos Silva, and Nicole Leite Galvão-Coelho
Subjects: Drug, biology, business.industry, medicine.drug_class, media_common.quotation_subject, Physiology, Tricyclic antidepressant, Marmoset, Ayahuasca, biology.animal, medicine, Antidepressant, Ingestion, Nortriptyline, business, Depression (differential diagnoses), media_common, medicine.drug
Abstract: The incidence of major depression in adolescents, aged between 15 to 18 years, reaches approximately 14%. Usually, this disorder presents a recurrent way, without remission of symptoms even after several pharmacological treatments, persisting through adult life. Due to the relatively low efficacy of commercially available antidepressant, new pharmacological therapies are under continuous exploration. Recent evidence suggests that classic psychedelics, such as ayahuasca, produce rapid and robust antidepressant effects in treatment-resistant depression patients. In this study, we evaluated the potential of antidepressant effects of ayahuasca in a juvenile model of depression in a non-human primate, common marmoset (Callithrix jacchus). The model induces depressive-like symptoms by chronic social isolation (60 days) and antidepressant effects monitoring included fecal cortisol, body weight, and behavioral parameters. The animals presented hypocortisolemia and the recovery of cortisol to baseline levels started already at 24h after the ingestion of ayahuasca, but not the vehicle. Moreover, in males, ayahuasca, and not the vehicle, reduced the scratching, a stereotypic behavior, and increased the feeding. Ayahuasca also improving body weight to baseline levels in male and female common marmosets. The behavioral response induced by ayahuasca shows long effect, lasting 14 days. Therefore, for this translational animal model of juvenile depression, it could be proposed that ayahuasca treatment presented more notable antidepressant effects than tricyclic antidepressant nortriptyline, investigated by our group, using this same protocol in an anterior study. Ayahuasca produced faster and more durable effect on reversion of physiological changes and depressive-like symptoms. Therefore, the results found for ayahuasca treatment corroborates in the validation of this substance as an effective antidepressant drug and encourages the return of studies with psychedelic drugs in the treatment of humor disorders, including adolescents with early-age depression. Keywords: translational animal model, non-human primate, common marmoset, behaviors, cortisol, early-age depression, psychedelic drugs.
Published: 2018
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19. Antidepressant effects of a single dose of ayahuasca in patients with recurrent depression: a preliminary report

Author: Rafael Faria Sanches, Jordi Riba, Lauro Wichert-Ana, Dráulio Barros de Araújo, Rafael G. dos Santos, João Paulo Maia-de-Oliveira, Flávia de Lima Osório, Lígia Ribeiro Horta Macedo, José Alexandre de Souza Crippa, and Jaime Eduardo Cecílio Hallak
Subjects: Adult, Male, medicine.medical_specialty, Time Factors, lcsh:RC435-571, Dimethyltryptamine, Young Mania Rating Scale, Severity of Illness Index, N,N-Dimethyltryptamine, lcsh:Psychiatry, Brief Psychiatric Rating Scale, medicine, Humans, harmine, Psychiatry, ANTIPSICÓTICOS, Analysis of Variance, Depressive Disorder, dimethyltryptamine, Banisteriopsis, Hamilton Rating Scale for Depression, monoamine oxidase inhibitors, Middle Aged, medicine.disease, Antidepressive Agents, humanities, Psychiatry and Mental health, Mood, Hypomania, Treatment Outcome, Mood disorders, Anti-Anxiety Agents, therapeutic use, Hallucinogens, Female, medicine.symptom, Psychology, Psychedelic agents, Mania, Clinical psychology, Phytotherapy
Abstract: Objectives: Ayahuasca (AYA), a natural psychedelic brew prepared from Amazonian plants and rich in dimethyltryptamine (DMT) and harmine, causes effects of subjective well-being and may therefore have antidepressant actions. This study sought to evaluate the effects of a single dose of AYA in six volunteers with a current depressive episode. Methods: Open-label trial conducted in an inpatient psychiatric unit. Results: Statistically significant reductions of up to 82% in depressive scores were observed between baseline and 1, 7, and 21 days after AYA administration, as measured on the Hamilton Rating Scale for Depression (HAM-D), the Montgomery-A u sberg Depression Rating Scale (MADRS), and the Anxious-Depression subscale of the Brief Psychiatric Rating Scale (BPRS). AYA administration resulted in nonsignificant changes in Young Mania Rating Scale (YMRS) scores and in the thinking disorder subscale of the BPRS, suggesting that AYA does not induce episodes of mania and/or hypomania in patients with mood disorders and that modifications in thought content, which could indicate psychedelic effects, are not essential for mood improvement. Conclusions: These results suggest that AYA has fast-acting anxiolytic and antidepressant effects in patients with a depressive disorder.
Published: 2015

20. Nitroprusside single-dose prevents the psychosis-like behavior induced by ketamine in rats for up to one week

Author: Jaime Eduardo Cecílio Hallak, Bruno Lobão-Soares, Glen B. Baker, Vanessa de Paula Soares, Thais Ramalho, Leslie Teixeira, Serdar M. Dursun, Elaine C. Gavioli, and João Paulo Maia-de-Oliveira
Subjects: Male, Nitroprusside, Psychosis, Time Factors, Rotation, medicine.medical_treatment, Video Recording, Motor Activity, Pharmacology, Open field, Random Allocation, Stereotypy, medicine, Animals, SNP, Nitric Oxide Donors, Ketamine, Rats, Wistar, Antipsychotic, ANTIPSICÓTICOS, Saline, Biological Psychiatry, business.industry, medicine.disease, Disease Models, Animal, Psychiatry and Mental health, Treatment Outcome, Psychotic Disorders, Anesthesia, Sodium nitroprusside, Stereotyped Behavior, medicine.symptom, business, Software, Antipsychotic Agents, medicine.drug
Abstract: Recently, we found a rapid and long-lasting improvement of symptoms in schizophrenic patients on antipsychotics after a single four-hour infusion of sodium nitroprusside (SNP), a nitric oxide (NO) donor with a short half-life. This improvement persisted for up to 4 weeks. Because these patients remained on antipsychotics after infusion of SNP was finished, the question arises about whether this improvement was due to SNP itself. We have now investigated whether SNP, alone, can produce preventive antipsychotic effects in rats treated with ketamine (KET). 56 adult rats divided into 7 groups were infused with SNP 4 mg/kg, KET 25 mg/kg, or saline as follows: group1 — saline, group2 — SNP, group3 — KET, group4 — KET 12 h after SNP, group5 — KET 1 day after SNP, group6 — KET 2 days after SNP, and group7 — KET 1 week after SNP. The animals were filmed in an open field arena for 30 min and the videos were later analyzed by ANY-Maze software to measure activity and stereotypy. SNP significantly prevented the emergence of hyperactivity induced by KET when it was administered for up to 1 week before KET, and prevented the emergence of stereotypies when it was administered for up to 1 day before KET. These findings in rats, which have an even faster metabolic rate than humans, suggest that the long-lasting effects observed in our clinical trial with SNP in humans could have been due to SNP itself, and indicate for the first time that SNP may present preventive antipsychotic effects.
Published: 2015

21. A randomized placebo-controlled trial on the antidepressant effects of the psychedelic ayahuasca in treatment-resistant depression

Author: Oliveira Silveira Gd, Jaime Eduardo Cecílio Hallak, Jordi Riba, Bruno Lobão-Soares, João Paulo Maia-de-Oliveira, Morgana M. Novaes, Sérgio A. Mota-Rolim, Mauricio Yonamine, Dráulio Barros de Araújo, Arnóbio Antônio da Silva-Júnior, Flávia de Lima Osório, Emerson Arcoverde, Fernanda Palhano-Fontes, João Carlos Alchieri, Francisco Rr Santos, Heloisa Onias, dos Santos Rg, Katia C. Andrade, Luís Fernando Tófoli, Dayanna Barreto, Rafael Faria Sanches, Jéssica de Andrade Pessoa, and Nicole Leite Galvão-Coelho
Subjects: medicine.medical_specialty, business.industry, Placebo-controlled study, Ayahuasca, medicine.disease, Placebo, law.invention, Clinical trial, Randomized controlled trial, law, Internal medicine, Medicine, Antidepressant, business, Treatment-resistant depression, Depression (differential diagnoses)
Abstract: Recent open label trials show that psychedelics, such as ayahuasca, hold promise as fast-onset antidepressants in treatment-resistant depression. In order to further test the antidepressant effects of ayahuasca, we conducted a parallel-arm, double-blind randomized placebo-controlled trial in 29 patients with treatment-resistant depression. Patients received a single dose of either ayahuasca or placebo. Changes in depression severity were assessed with the Montgomery–Åsberg Depression Rating Scale (MADRS) and the Hamilton Depression Rating scale (HAM-D). Assessments were made at baseline, and at one (D1), two (D2) and seven (D7) days after dosing. We observed significant antidepressant effects of ayahuasca when compared to placebo at all timepoints. MADRS scores were significantly lower in the ayahuasca group compared to placebo (at D1 and D2: p=0.04; and at D7: p
Published: 2017
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22. Letter to the Editor: Sodium nitroprusside for schizophrenia: could methodological variables account for the different results obtained?

Author: João Paulo Maia-de-Oliveira, Glen B. Baker, Jaime Eduardo Cecílio Hallak, and Serdar M. Dursun
Subjects: Nitroprusside, medicine.medical_specialty, Letter to the editor, Schizophrenia (object-oriented programming), 030227 psychiatry, 03 medical and health sciences, Psychiatry and Mental health, 0302 clinical medicine, medicine, Schizophrenia, Humans, Sodium nitroprusside, Psychology, Psychiatry, 030217 neurology & neurosurgery, Applied Psychology, medicine.drug, Antipsychotic Agents
Published: 2016

23. Sodium Nitroprusside Treatment of Clozapine-Refractory Schizophrenia

Author: Paulo Silva Belmonte-de-Abreu, João Paulo Maia-de-Oliveira, Glen B Baker, Rodrigo A. Bressan, S.M. Dursun, Jaime Eduardo Cecílio Hallak, and Carolina Tosetto Cachoeira
Subjects: Olanzapine, business.industry, Sodium, chemistry.chemical_element, Pharmacology, medicine.disease, Psychiatry and Mental health, Pharmacotherapy, Refractory, chemistry, Schizophrenia, Medicine, Pharmacology (medical), Sodium nitroprusside, business, ANTIPSICÓTICOS, Clozapine, medicine.drug
Published: 2014

24. Novel Targets for Development of Drugs for Treating Schizophrenia: Focus on Glycine, D-Serine and Nitric Oxide

Author: Serdar M. Dursun, João Paulo Maia-de-Oliveira, Glen B. Baker, Kamaldeep S. Dhami, Marnie MacKay, Kathryn G. Todd, and Jaime Eduardo Cecílio Hallak
Subjects: business.industry, medicine.medical_treatment, Pharmacology, Bioinformatics, medicine.disease, 030227 psychiatry, Nitric oxide, Serine, 03 medical and health sciences, Psychiatry and Mental health, chemistry.chemical_compound, 0302 clinical medicine, Neurochemical, Pharmacotherapy, chemistry, Dopamine, Schizophrenia, Glycine, Medicine, Pharmacology (medical), business, Antipsychotic, 030217 neurology & neurosurgery, medicine.drug
Abstract: For many years the focus of neurochemical and pharmacological studies on schizophrenia was on dopamine, and that work yielded a great deal of information about the possible etiology of this debilitating disorder and contributed significantly to the development of antipsychotic drugs. However, it has become increasingly apparent that other neurotransmitters and neuromodulators must also play an important role, and in recent years there has been considerable interest in these other compounds and the systems related to them in the search for developing drugs that are more effective and have fewer side effects than the antipsychotics currently available. This review deals with three of those neurochemicals, namely glycine, D-serine and nitric oxide, and shows how an increased knowledge of them may be important in the future diagnosis and/or pharmacotherapy of schizophrenia.
Published: 2013

25. Nitric Oxide's Involvement in the Spectrum of Psychotic Disorders

Author: João Paulo Maia-de-Oliveira, Emerson Arcoverde Nunes, Jaime Eduardo Cecílio Hallak, João Paulo Machado-de-Sousa, Serdar M. Dursun, and Ludmyla Kandratavicius
Subjects: Psychosis, medicine.medical_specialty, Schizoaffective disorder, Arginine, Nitric Oxide, Biochemistry, Sildenafil Citrate, Nitric oxide, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Drug Discovery, medicine, Humans, Schizophreniform disorder, Psychiatry, Pharmacology, Clinical Trials as Topic, biology, Delusional disorder, business.industry, Organic Chemistry, Brief psychotic disorder, Brain, Phosphodiesterase 5 Inhibitors, medicine.disease, 030227 psychiatry, Nitric oxide synthase, chemistry, Psychotic Disorders, Schizophrenia, biology.protein, Molecular Medicine, Nitric Oxide Synthase, business, 030217 neurology & neurosurgery, Antipsychotic Agents
Abstract: Background: Recent findings suggest that dopaminergic abnormalities found in psychotic disorders may be secondary to nitric oxide dysfunctions. Nitric oxide seems to influence glutamatergic and dopaminergic neurotransmission, both of which have been associated with psychosis. Objective: To search and review published works which examined the influence of nitric oxide in psychotic disorders subjects. Method: The research was executed in the on-line collections of Pubmed and ISI Web of Science. The key aspects utilized were “Psychotic Disorders AND Nitric Oxide”, “Psychosis AND Nitric Oxide”,“Schizotypal Personality Disorder AND Nitric Oxide”, “Delusional Disorder AND Nitric Oxide”, “Brief Psychotic Disorder AND Nitric Oxide”, “Schizophreniform Disorder AND Nitric Oxide”, “Schizoaffective Disorder AND Nitric Oxide”, and “Schizophrenia AND Nitric Oxide”. Empirical works utilizing human subjects, published in the last 10 years, in English language were included. Results: Initially, the search yielded a total of 95 studies. Then, 39 were elected according to the inclusion requirements. The selected articles were divided into five groups: biochemical studies (n=15; 38.5%), genetic studies (n=11; 28.2%), postmortem studies (n=6; 15.4%), clinical trials (n=6; 15.4%), and case reports (n=1; 2.5%). The studies evaluated only schizophrenic or schizoaffective disorder subjects. The great majority of them found evidence of nitric oxide dysfunctions in psychosis. Conclusion: The results of the review strengthen the idea that nitric oxide has a key participation in psychotic disorders and deserves deeper investigation as a target for future pharmacological intervention.
Published: 2016

26. Role of methylene blue in trauma neuroprotection and neuropsychiatric diseases

Author: Vitor Tumas, Ludmyla Kandratavicius, Jaime Eduardo Cecílio Hallak, Mário Márcio Vasconcelos Batista-Filho, Paulo Roberto Barbosa Evora, João Paulo Maia-de-Oliveira, Benedicto O. Colli, and Emerson Arcoverde Nunes
Subjects: 0301 basic medicine, Pharmacology, PubMed, business.industry, Brain Neoplasms, General Neuroscience, Mental Disorders, Central nervous system, FÁRMACOS (SISTEMA NERVOSO CENTRAL), Neuroprotection, Methylene Blue, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Neuroprotective Agents, Web of knowledge, medicine, Animals, Humans, business, Neuroscience, 030217 neurology & neurosurgery
Abstract: The prevalence of central nervous system trauma, neurodegenerative and psychiatric diseases has significantly increased in recent years. Most of these diseases show multifactorial causes and several progression mechanisms. The search for a medication which positively interferes in these mechanisms and thereby changes the course of these diseases is of great scientific interest. The aim of the present review is to assess current literature on the possible role of methylene blue (MB) in the central nervous system due to the increasing number of citations in spite of the few articles available on the subject which suggest growing interest in the protective effects of MB on the central nervous system. Searches were performed on PubMed and Thomson Reuters Web of Knowledge. Therefore, we provide an overview of existing articles concerning: 1) MB actions; 2) MB neuroprotection and cardiac arrest; 3) MB neuroprotection and degenerative brain diseases; 4) MB neuroprotection and psychiatric diseases. PubMed was chosen because it holds the highest number of articles on the subject, Thomson Reuters was chosen due to its functionality which evaluates citations through analytic graphs. We conclude that MB has a beneficial effect and acts through many mechanisms and pathways of the central nervous system, being a potential alternative for the treatment of many neurodegenerative and psychiatric diseases.
Published: 2016

27. Antidepressant Effects of a Single Dose of Ayahuasca in Patients With Recurrent Depression: A SPECT Study

Author: Jordi Riba, Rafael G. dos Santos, José Alexandre de Souza Crippa, Lígia Ribeiro Horta Macedo, João Paulo Maia-de-Oliveira, Rafael Faria Sanches, L. Wichert-Ana, Jaime Eduardo Cecílio Hallak, Flávia de Lima Osório, and Dráulio Barros de Araújo
Subjects: Hallucinogen, Adult, Male, medicine.medical_specialty, Time Factors, Dimethyltryptamine, Administration, Oral, Young Mania Rating Scale, 03 medical and health sciences, 0302 clinical medicine, Rating scale, Recurrence, Brief Psychiatric Rating Scale, medicine, Humans, Pharmacology (medical), harmine, Psychiatry, ANTIPSICÓTICOS, Psychiatric Status Rating Scales, Tomography, Emission-Computed, Single-Photon, Depressive Disorder, Major, dimethyltryptamine, Banisteriopsis, Hamilton Rating Scale for Depression, Brain, monoamine oxidase inhibitors, Middle Aged, Ayahuasca, Antidepressive Agents, 030227 psychiatry, Psychiatry and Mental health, Treatment Outcome, Anesthesia, Vomiting, Hallucinogens, Female, Plant Preparations, medicine.symptom, Psychology, 030217 neurology & neurosurgery, ayahuasca
Abstract: Ayahuasca is an Amazonian botanical hallucinogenic brew which contains dimethyltryptamine, a 5-HT2A receptor agonist, and harmine, a monoamine-oxidase A inhibitor. Our group recently reported that ayahuasca administration was associated with fast-acting antidepressive effects in 6 depressive patients. The objective of the present work was to assess the antidepressive potentials of ayahuasca in a bigger sample and to investigate its effects on regional cerebral blood flow. In an open-label trial conducted in an inpatient psychiatric unit, 17 patients with recurrent depression received an oral dose of ayahuasca (2.2 mL/kg) and were evaluated with the Hamilton Rating Scale for Depression, the Montgomery-angstrom sberg Depression Rating Scale, the Brief Psychiatric Rating Scale, the Young Mania Rating Scale, and the Clinician Administered Dissociative States Scale during acute ayahuasca effects and 1, 7, 14, and 21 days after drug intake. Blood perfusion was assessed eight hours after drug administration by means of single photon emission tomography. Ayahuasca administration was associated with increased psychoactivity (Clinician Administered Dissociative States Scale) and significant score decreases in depression-related scales (Hamilton Rating Scale for Depression, Montgomery-angstrom sberg Depression Rating Scale, Brief Psychiatric Rating Scale) from 80 minutes to day 21. Increased blood perfusion in the left nucleus accumbens, right insula and left subgenual area, brain regions implicated in the regulation of mood and emotions, were observed after ayahuasca intake. Ayahuasca was well tolerated. Vomiting was the only adverse effect recorded, being reported by 47% of the volunteers. Our results suggest that ayahuasca may have fast-acting and sustained antidepressive properties. These results should be replicated in randomized, double-blind, placebo-controlled trials.
Published: 2015

28. Mood Disorder Due to a General Medical Condition with Manic Features

Author: J. E. Cecílio Hallak, Silvio Luiz Morais, José Alexandre de Souza Crippa, João Paulo Maia de Oliveira, B. O. Colli, D. Araújo, and Carlos Gilberto Carlotti
Subjects: medicine.medical_specialty, Psychiatric Disease, business.industry, lcsh:R, Neurocysticercosis, Alternative medicine, lcsh:Medicine, Case Report, General Medicine, medicine.disease, Hydrocephalus, Mood, Medicine, business, Psychiatry
Abstract: This case report describes a patient with manic and psychotic symptoms who had a history of neurocysticercosis and presented with an episode of hypertensive hydrocephalus in 2003. Despite her history, she was initially treated for primary psychiatric disease.
Published: 2009

29. Role of Nitric Oxide in Patients with Schizophrenia- a Systematic Review of the Literature

Author: Antonio Waldo Zuardi, João Paulo Maia de Oliveira, and Jaime Eduardo Cecílio Hallak
Subjects: Psychiatry and Mental health, chemistry.chemical_compound, chemistry, Schizophrenia (object-oriented programming), Brain maturation, Etiology, In patient, Neurotransmission, Psychology, Neuroscience, Nitric oxide
Abstract: In spite of numerous studies focused on schizophrenia, its etiology remain unknown. If we bear in mind that schizophrenia is a progressive syndrome where genetic and environmental components contribute, with impairment in the brain maturation as a result, it is conceivable that research seeking to unveil its etiology should focus on dysfunctions in systems responsible for the control of brain neurodevelopment. Recent scientific evidence has pointed to a possible role for the NO (nitric oxide) in schizophrenia. NO is a gas with unique chemistry and influences the release of neurotransmitters, learning, memory and neurodevelopment. This review tried to focus on researches that examined alterations in NOmediated neurotransmission in patients with schizophrenia. The search was performed in Pubmed, Scielo, and Lilacs, using the keywords Schizophrenia and Nitric Oxide. The search on Pubmed yielded 138 matches, from which 40 were selected. No studies were found in the others databases. In summary, we note that there are studies supporting apparently contradictory results: some of them suggesting a increase of the NO-mediated neurotransmission, and another part supporting a decrease. We discuss these findings, and our overall impression is that the better designed studies found evidence pointing to a disruption in NO-mediated neurotransmission in schizophrenia.
Published: 2008

30. Cognition in at-risk mental states for psychosis

Author: Jaime Eduardo Cecílio Hallak, João Paulo Machado-de-Sousa, Andre Luiz Damiao de Paula, João Paulo Maia-de-Oliveira, and Rodrigo A. Bressan
Subjects: Psychosis, medicine.medical_specialty, Cognitive Neuroscience, Psychological intervention, Early detection, Cognition, medicine.disease, Behavioral Neuroscience, Neuropsychology and Physiological Psychology, Psychotic Disorders, Social cognition, Schizophrenia, Generalization (learning), medicine, Disease Progression, Humans, Cognitive Assessment System, SINAIS E SINTOMAS, Psychiatry, Psychology, Cognition Disorders, Clinical psychology
Abstract: Rationale The devastating nature of schizophrenia and treatment limitations have triggered a search for early detection methods to enable interventions to be implemented as soon as the first signs and symptoms appear. In this effort, several studies have investigated the cognitive functions in individuals regarded as being in at-risk mental states (ARMS) for psychosis. Objective Our aim was to make a systematic review of the literature regarding basic and social cognition in individuals in ARMS following the guidelines of the PRISMA statement. Results In general, the results of the 49 articles included in the review show that individuals in ARMS have pervasive cognitive deficits that seem to be greater in individuals who later convert to psychosis. Conclusions Cognitive impairment can be detected in individuals considered to be in ARMS according to current classifications and may serve as a risk marker for psychotic conversion; however, the lack of standardized criteria to define ARMS and of homogeneous cognitive assessment methods hamper the generalization of findings from different studies.
Published: 2015

31. The effects of sodium nitroprusside treatment on cognitive deficits in schizophrenia. [Carta]: a pilot study

Author: Paulo Belmonte-de-Abreu, Jaime Eduardo Cecílio Hallak, João Abrão, Paulo Roberto Barbosa Evora, José Alexandre de Souza Crippa, Glen B. Baker, Serdar M. Dursun, Antonio Waldo Zuardi, and João Paulo Maia-de-Oliveira
Subjects: Male, Nitroprusside, medicine.medical_specialty, MEDLINE, Pilot Projects, law.invention, Executive Function, Text mining, Randomized controlled trial, Double-Blind Method, law, Schizophrenic Psychology, Medicine, Humans, Pharmacology (medical), Nitric Oxide Donors, Psychiatry, business.industry, ESQUIZOFRENIA, Cognition, medicine.disease, Psychiatry and Mental health, Treatment Outcome, Schizophrenia, Stroop Test, Female, Sodium nitroprusside, business, Cognition Disorders, medicine.drug, Stroop effect
Published: 2015

32. Effects of nitric oxide-related compounds in the acute ketamine animal model of schizophrenia

Author: João Paulo Maia-de-Oliveira, Daniele Cristina Wolf, Serdar M. Dursun, Jaime Eduardo Cecílio Hallak, Ludmyla Kandratavicius, Cristiano Chaves, Francisco Silveira Guimarães, Priscila Alves Balista, Alfredo José Rodrigues, João Abrão, Paulo Roberto Barbosa Evora, Glen B. Baker, and João Pereira Leite
Subjects: Male, Nitroprusside, Motor Activity, Pharmacology, Glyceryl trinitrate, Open field, Nitric oxide, Nitroglycerin, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Animal model, Dietary Sucrose, medicine, Animals, SNP, Nitric Oxide Donors, Ketamine, Rats, Wistar, Sodium nitroprusside, Methylene blue, business.industry, General Neuroscience, Therapeutic effect, Therapeutic treatment, Taste Perception, Recognition, Psychology, Ketamine model, medicine.disease, Disease Models, Animal, Treatment Outcome, chemistry, Schizophrenia, MODELOS ANIMAIS, Acute Disease, Exploratory Behavior, Schizophrenic Psychology, Cognition Disorders, business, Neuroscience, Research Article, Preventive treatment, Antipsychotic Agents, medicine.drug
Abstract: Background Better treatments for schizophrenia are urgently needed. The therapeutic use of the nitric oxide (NO)-donor sodium nitroprusside (SNP) in patients with schizophrenia has shown promising results. The role of NO in schizophrenia is still unclear, and NO modulation is unexplored in ketamine (KET) animal models to date. In the present study, we compared the behavioral effects of pre- and post-treatment with SNP, glyceryl trinitrate (GTN), and methylene blue (MB) in the acute KET animal model of schizophrenia. The present study was designed to test whether acute SNP, GTN, and MB treatment taken after (therapeutic effect) or before (preventive effect) a single KET injection would influence the behavior of rats in the sucrose preference test, object recognition task and open field. Results The results showed that KET induced cognitive deficits and hyperlocomotion. Long- term memory improvement was seen with the therapeutic GTN and SNP treatment, but not with the preventive one. MB pretreatment resulted in long-term memory recovery. GTN pre-, but not post-treatment, tended to increase vertical and horizontal activity in the KET model. Therapeutic and preventive SNP treatment consistently decreased KET-induced hyperlocomotion. Conclusion NO donors – especially SNP – are promising new pharmacological candidates in the treatment of schizophrenia. In addition, we showed that the potential impact of NO-related compounds on KET-induced behavioral changes may depend on the temporal window of drug administration.
Published: 2015

33. Psychotic syndrome secondary to meningioma treated with a low dose of olanzapine. [Carta]

Author: Jaime Eduardo Cecílio Hallak, João Paulo Maia-de-Oliveira, João Paulo Machado-de-Sousa, Lízie Emanuelle Eulálio Brasileiro, and Carlos E. Correia
Subjects: Olanzapine, Meningioma, Psychiatry and Mental health, lcsh:RC435-571, business.industry, lcsh:Psychiatry, Anesthesia, Low dose, medicine, TRANSTORNOS PSICÓTICOS, medicine.disease, business, medicine.drug
Published: 2015

34. Sodium nitroprusside, a nitric oxide donor for novel treatment of schizophrenia, may also modulate dopaminergic systems

Author: Serdar M. Dursun, Bruno Lobão-Soares, Glen B. Baker, Jaime Eduardo Cecílio Hallak, and João Paulo Maia-de-Oliveira
Subjects: Nitroprusside, business.industry, Dopamine, Dopaminergic, Pharmacology, medicine.disease, Synaptic Transmission, Nitric oxide, Psychiatry and Mental health, chemistry.chemical_compound, Treatment Outcome, chemistry, Schizophrenia, Medicine, Humans, Drug Therapy, Combination, Nitric Oxide Donors, Sodium nitroprusside, business, Biological Psychiatry, medicine.drug, Antipsychotic Agents
Abstract: “Schizophrenia is arguably the worst disease affecting mankind, even AIDS not excepted”. Since this statement in 1988 (Editors, 1988), schizophrenia still remains a major challenge to medicine, with up to 60% of patients not responding adequately to treatment despite the relatively large arsenal of antipsychotics currently available. By modulating the nitric oxide (NO) pathway, a new paradigm for schizophrenia treatment apparently involving modulation of nitric oxide (NO) has been proposed (Oliveira et al., 2011).
Published: 2014

35. Functional neuroimaging of minocycline's effect in a patient with schizophrenia

Author: João Paulo Maia-de-Oliveira, José Alexandre de Souza Crippa, Antonio Waldo Zuardi, Kathryn G. Todd, Glen B. Baker, Serdar M. Dursun, Emerson Nobuyuki Itikawa, C. Marque, Cristiano Chaves, Lauro Wichert-Ana, and Jaime Eduardo Cecílio Hallak
Subjects: Pharmacology, Functional imaging, Psychosis, Functional neuroimaging, Schizophrenia, medicine, Minocycline, Psychology, medicine.disease, Neuroscience, Biological Psychiatry, medicine.drug
Published: 2010

36. A False Case of Clozapine-Resistant Schizophrenia

Author: João Paulo Maia-de-Oliveira, Jaime Eduardo Cecílio Hallak, Joel Porfirio Pinto, V. Alexandre, Silvio Luiz Morais, Cristiano Chaves, Antonio Waldo Zuardi, José Alexandre de Souza Crippa, A.C. Sakamoto, and João Paulo Machado-de-Sousa
Subjects: Psychosis, Pediatrics, medicine.medical_specialty, business.industry, Refractory period, lcsh:R, lcsh:Medicine, Case Report, General Medicine, Antipsychotic treatment, medicine.disease, Epilepsy, Refractory, Schizophrenia, mental disorders, medicine, business, Psychiatry, Clozapine, medicine.drug
Abstract: One of the subjects that most concerns physicians is treatment-resistance. About 30%–60% of schizophrenia patients do not respond adequately to antipsychotic treatment and are known as refractory schizophrenia patients. Clozapine has been the drug of choice in such cases. However, approximately 30% of them do not respond to clozapine either. Here, we describe a patient with an initial diagnosis of refractory schizophrenia who had a history of dramatic aggressiveness. However, in this case, “refractoriness” was a wrong diagnosis. A case of psychosis secondary to epilepsy had been treated as schizophrenia for almost 20 years. Reports like this one are important because they remind us of how a thorough investigation can lead to the correct diagnosis and improve the patient's prognosis.
Published: 2010

37. Rapid improvement of acute schizophrenia symptoms after intravenous sodium nitroprusside: a randomized, double-blind, placebo-controlled trial

Author: Paulo Roberto Barbosa Evora, José Alexandre de Souza Crippa, Paulo Belmonte-de-Abreu, João Abrão, Serdar M. Dursun, Antonio Waldo Zuardi, Jaime Eduardo Cecílio Hallak, João Paulo Maia-de-Oliveira, and Glen B. Baker
Subjects: Adult, Male, Nitroprusside, medicine.medical_treatment, Placebo-controlled study, Placebo, PLACEBOS, Placebos, Double-Blind Method, Brief Psychiatric Rating Scale, medicine, Humans, Antipsychotic, Positive and Negative Syndrome Scale, business.industry, medicine.disease, Psychiatry and Mental health, Schizophrenia, Anesthesia, Administration, Intravenous, Female, Schizophrenic Psychology, Sodium nitroprusside, business, medicine.drug, Diagnosis of schizophrenia, Antipsychotic Agents
Abstract: Importance The treatment of schizophrenia remains a challenge, and the currently available antipsychotic drugs are slow acting and produce a number of adverse effects. Objective To examine the effectiveness and safety of a single intravenous administration of sodium nitroprusside (0.5 μg/kg/min for 4 hours) on the positive, negative, anxiety, and depressive symptoms in patients with schizophrenia. Design Single-center, randomized, double-blind, placebo-controlled trial performed from March 9, 2007, to March 12, 2009. Setting University teaching hospital in Sao Paulo, Brazil. Participants Twenty inpatients aged 19 to 40 years with a diagnosis of schizophrenia who were in the first 5 years of the disease who are taking antipsychotics. Intervention Sodium nitroprusside administration. Main Outcome Measures The 18-item Brief Psychiatric Rating Scale and the negative subscale of the Positive and Negative Syndrome Scale. Results After the infusion of sodium nitroprusside, a rapid (within 4 hours) improvement of symptoms was observed. The placebo and experimental groups had significant differences in the 18-item Brief Psychiatric Rating Scale total score and subscale scores, which persisted for 4 weeks after infusion. Conclusions The results clearly show a therapeutic effect of sodium nitroprusside. If this drug is approved for routine clinical use in patients with schizophrenia, this discovery will be an important advance in the pharmacologic treatment of this devastating disorder. Trial Registration clinicaltrials.gov Identifier:NCT01548612
Published: 2013

38. Níveis plasmáticos/séricos do óxido nítrico em pacientes com esquizofrenia: uma revisão sistemática e metanálise

Author: Irismar Reis de Oliveira, Serdar M. Dursun, Jaime Eduardo Cecílio Hallak, Tatiana M. N. de Rezende, Clarissa Trzesniak, Sandro Iêgo, João Paulo Machado-de-Sousa, João Paulo Maia-de-Oliveira, Matthew J. Kempton, and Glen B. Baker
Subjects: medicine.medical_specialty, Psychosis, Psicose, Esquizofrenia, Empirical Research, Nitric Oxide, Gastroenterology, Nitric oxide, Metanálise, chemistry.chemical_compound, Plasma levels, Internal medicine, medicine, Humans, In patient, Serum levels, Nitrite, Níveis plasmáticos, medicine.disease, Surgery, Psychiatry and Mental health, Meta-analysis, medicine.anatomical_structure, chemistry, Níveis séricos, Revisão sistemática, Schizophrenia, Dopaminergic pathways, Data Interpretation, Statistical, Systematic review, Psychology, PESQUISA BIBLIOGRÁFICA (MÉTODOS), Óxido nítrico, Antipsychotic Agents
Abstract: For the last 40 years, schizophrenia has been considered to be the result primarily of a dysfunction in brain dopaminergic pathways. In this review, it is described and discussed findings concerning nitric oxide-mediated neurotransmission in schizophrenia. Studies were searched in PubMed, SciELO, and LILACS using the terms schizophrenia and nitric oxide plasma levels or nitric oxide serum levels, with no time limit. The reference lists of selected articles were also hand-searched for additional articles. From 15 potential reports, 10 were eligible to be included in the review and meta-analysis. These studies included a total of 505 patients with schizophrenia and 339 healthy volunteers. No significant difference was found between patients and healthy controls regarding total nitrite plasma/serum levels (effect size g = 0.285, 95%CI = -0.205 to 0.774, p = 0.254). However, when studies with patients under antipsychotic treatment were examined separately, there was a significant difference between patients and healthy volunteers (effect size g = 0.663, 95%CI = 0.365 to 0.961, p < 0.001), showing that patients under treatment have higher levels of plasma/serum nitric oxide than controls. These results suggest that antipsychotics increase nitric oxide plasma/serum levels and that the nitrergic pathway would be a fertile target for the development of new treatments for patients with schizophrenia. Durante os últimos 40 anos, a esquizofrenia foi considerada, principalmente, como o resultado de disfunções dopaminérgicas no cérebro. Esta revisão descreve e discute algumas descobertas sobre a neurotransmissão mediada pelo óxido nítrico na esquizofrenia. A busca foi feita nas bases PubMed, SciELO e LILACS usando-se os termos schizophrenia e nitric oxide plasma levels ou nitric oxide serum levels, sem limites de tempo. As listas de referências dos artigos selecionados foram examinadas em busca de outras publicações pertinentes. Dentre 15 artigos passíveis de serem incluídos, 10 preenchiam os critérios estabelecidos para a revisão e metanálise. Esses estudos incluíram 505 pacientes com esquizofrenia e 339 voluntários saudáveis. Não foram encontradas diferenças significativas entre pacientes e voluntários saudáveis quanto aos níveis plasmáticos de nitrito total (effect size g = 0,285, IC 95% = -0,205 a 0,774, p = 0,254). No entanto, o exame separado dos estudos envolvendo pacientes em tratamento antipsicótico apresentou diferenças significativas entre pacientes e voluntários saudáveis (effect size g = 0,663, IC 95% = 0,365 to 0,961, p < 0,001), demonstrando que pacientes em tratamento possuem níveis plasmáticos mais altos de óxido nítrico. Esses resultados sugerem que os antipsicóticos podem aumentar os níveis plasmáticos de óxido nítrico e que a via nitrérgica (e sua estimulação) constituiria um alvo propício para o desenvolvimento de novos tratamentos para pacientes com esquizofrenia.
Published: 2012
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39. THE USE OF SODIUM NITROPRUSSIDE FOR THE TREATMENT OF SCHIZOPHRENIA

Author: Paulo Roberto Barbosa Evora, Antonio Waldo Zuardi, Jaime Eduardo Cecílio Hallak, João Abrão, José Alexandre de Souza Crippa, João Paulo Maia de Oliveira, Paulo Abreu, Glen B. Baker, and Serdar M. Dursun
Subjects: Psychiatry and Mental health, business.industry, Schizophrenia (object-oriented programming), Medicine, Sodium nitroprusside, Pharmacology, business, Biological Psychiatry, medicine.drug
Published: 2014

40. Targeting the NMDA receptor-nitric oxide-cyclic GMP pathway to develop non-dopaminergic antipsychotic medications for schizophrenia A via receptor NMDA-óxido nítrico-GMP cíclico como alvo para o desenvolvimento de medicações antipsicóticas não-dopaminérgicas para a esquizofrenia

Author: João Paulo Maia de Oliveira, Bruno Lobão, João Paulo Machado-de-Sousa, Glen B. Baker, Serdar Dursun, and Jaime E. C. Hallak
Subjects: lcsh:RC435-571, lcsh:Psychiatry
Published: 2011

41. Targeting the NMDA receptor-nitric oxide-cyclic GMP pathway to develop non-dopaminergic antipsychotic medications for schizophrenia

Author: Bruno Lobão, Jaime Eduardo Cecílio Hallak, Serdar M. Dursun, Glen B. Baker, João Paulo Maia de Oliveira, and João Paulo Machado-de-Sousa
Subjects: medicine.medical_treatment, Population, Nitric Oxide, Receptors, N-Methyl-D-Aspartate, Dopamine, medicine, Humans, education, Antipsychotic, Cyclic GMP, education.field_of_study, Dopaminergic, Glutamate receptor, medicine.disease, Psychiatry and Mental health, medicine.anatomical_structure, Dopaminergic pathways, Schizophrenia, Anesthesia, NMDA receptor, Psychology, Neuroscience, Antipsychotic Agents, medicine.drug
Abstract: Schizophrenia is a devastating disorder that occurs in about 1% of the population worldwide. For over 30 years, it has been considered to be the result of dysfunctional brain dopaminergic pathways. However, dopaminergic antipsychotic drugs have proven effective for only some of the symptoms found in schizophrenia patients. Recent evidence suggests that dopaminergic abnormalities may be secondary to dysfunctions in multi-neurotransmitter systems modulating dopamine. One of the key neurotransmitters thought to be involved in schizophrenia is glutamate, and there is strong support for the involvement of a hypoactivity of N-methyl-D-aspartate (NMDA) glutamate receptors in the pathogenesis of schizophrenia. However, research with NMDA receptor agonists for the treatment of schizophrenia has produced inconsistent results, which may be due to the development of rapid tolerance to these compounds secondary to down-regulation of NMDA receptors. Perhaps the development of drugs that act on targets downstream NMDA receptors, such as nitric oxide (NO), could avoid the problem of the down-regulation of these receptors.
Published: 2011

42. Minocycline and psychoneuroimmunology in schizophrenia

Author: Jaime Eduardo Cecílio Hallak, Glen B. Baker, Antonio Waldo Zuardi, José Alexandre de Souza Crippa, C. Marque, Kathryn G. Todd, Serdar M. Dursun, Emerson Nobuyuki Itikawa, Lauro Wichert-Ana, João Paulo Maia-de-Oliveira, and Cristiano Chaves
Subjects: Pharmacology, Psychosis, medicine.medical_specialty, Psychotherapist, Schizophrenia, medicine, Minocycline, medicine.disease, Psychiatry, Psychology, Biological Psychiatry, medicine.drug, Psychoneuroimmunology
Published: 2010

43. Vortioxetine-induced manic mood switch in patient with previously unknown bipolar disorder

Author: João Paulo Maia de Oliveira, Gonçalo Sobreira, and Sofia Brissos
Subjects: Vortioxetine, medicine.medical_specialty, business.industry, lcsh:RC435-571, Trazodone, Manic Mood, medicine.disease, Letters to the Editors, 030227 psychiatry, 03 medical and health sciences, Psychiatry and Mental health, 0302 clinical medicine, Mood disorders, lcsh:Psychiatry, Psychiatric status rating scales, medicine, In patient, Bipolar disorder, business, Psychiatry, Serotonin Uptake Inhibitors, 030217 neurology & neurosurgery, medicine.drug

44. Potencialização do tratamento antipsicótico convencional da esquizofrenia com administração repetida de nitroprussiato de sódio

Author: Juliana Mayumi Ushirohira, João Paulo Machado de Sousa, João Abrão, João Paulo Maia de Oliveira, and Antonio Waldo Zuardi
Abstract: A busca pelo entendimento da etiofisiopatogênese da esquizofrenia permanece desafiadora e tratamentos convencionais com medicações antipsicóticas que agem principalmente através da modulação da neurotransmissão dopaminérgica mostramse insuficientes, vistos os elevados índices de refratariedade e superrefratariedade nesta população. Estudos recentes apontam resultados promissores de moduladores do sistema glutamatérgico com ação em receptores NMDA, como o nitroprussiato de sódio (NPS), um doador de óxido nítrico, capaz de reduzir sintomas positivos, negativos e cognitivos do transtorno. O objetivo do presente estudo foi estudar os efeitos da administração repetida de NPS sobre a sintomatologia de pacientes com esquizofrenia. Recrutados 17 pacientes portadores de esquizofrenia acompanhados no Hospital das Clínicas da Faculdade de Medicina de Ribeirão Preto - USP, em idade entre 18-45 anos, submetidos ao protocolo experimental com delineamento cruzado, duplo-cego, randomizado e controlado por placebo. Cada participante recebeu oito infusões intravenosas, sendo destas, quatro de NPS (0,5 ?g/kg/min por 4 horas/sessão) e quatro de placebo, em intervalo de 15 dias entre as sessões. A avaliação dos sintomas positivos, negativos e cognitivos foi feita através dos seguintes instrumentos: Escala de Avaliação das Síndromes Positiva e Negativa para Esquizofrenia (PANSS), Escala de Avaliação Psiquiátrica Breve (BPRS), Escala de Impressão Clínica Geral - Esquizofrenia (CGI-SCH), Stroop Color Word Test (SCWT), N-back, Teste de Fluência Verbal (FAS). Para avaliação de efeitos colaterais das medicações foi usada a Escala de Avaliação de Efeitos Colaterais (UKU). A análise dos dados demográficos e clínicos da amostra foi realizada através de estatística descritiva. As análises estatísticas foram feitas com o programa Statistical Package for the Social Sciences versão 17.0. Para avaliar o efeito do NPS nos escores BPRS, PANSS, SCWT, N-back e FAS, os dados foram submetidos a análise de variância de medidas repetidas para modelos de estudo crossover. Análises independentes para sessões de nitroprussiato de sódio e placebo foram realizadas quando houve significância estatística, seguidas de teste t de Student, que também foi empregado para avaliações pareadas entre dados do ínicio e final das sessões. Para análise da CGI-SCH, foi utilizado o teste de Friedman para medidas não-paramétricas. O nível de significância adotado foi de p
Published: 2019

45. Modelo animal de epilepsia e psicose comórbida: aspectos neuropatológicos, corportamentais e modulação pelo tratamento com nitroprussiato de sódio

Author: Priscila Alves Balista, Jaime Eduardo Cecilio Hallak, Ludmyla Kandratavicius, Acioly Luiz Tavares de Lacerda, João Pereira Leite, and João Paulo Maia de Oliveira
Abstract: Introdução: A esquizofrenia é um dos principais transtornos mentais e promove distúrbios comportamentais e cognitivos. Apesar do grande impacto social, pouco se conhece sobre a patofisiologia e etiologia da esquizofrenia. Pacientes com desordens psicóticas têm aumentado risco de desenvolver epilepsia, e pacientes com epilepsia do lobo temporal tem alta frequência de psicoses. A utilização de modelos experimentais animais de esquizofrenia e epilepsia pode ajudar a entender a neurobiologia dessas doenças e ter papel importante no desenvolvimento de novas estratégias terapêuticas. As interações complexas das crises epilépticas e quadros psicóticos tem sido aos poucos desvendadas. O óxido nítrico (NO) é um importante modulador da neurotransmissão e doadores de NO como o nitroprussiato de sódio (NPS) tem efeitos promissores em pacientes com esquizofrenia. Em modelos animais de epilepsia, NO pode ter efeito pró ou anticonvulsivante, sugerindo que o uso de NPS em pacientes com epilepsia e psicose pode não ser tão simples. Objetivos: Desenvolver um modelo animal de epilepsia e psicose comórbida, e compará-lo do ponto de vista comportamental e neuropatológico com modelos animais puros de epilepsia e esquizofrenia. Além disso, verificar a possível modulação desencadeada pelo tratamento com NPS nos modelos citados. Metodologia: Ratos Wistar machos (260-300g) foram divididos em grupos controle (SAL+SAL), epilepsia puro (PILO+SAL), esquizofrenia (SAL+QUET), epilepsia e psicose comórbida (PILO+QUET) e suas versões tratadas com NPS (SAL+SAL+NPS, PILO+SAL+NPS, SAL+QUET+NPS e PILO+QUET+NPS). Esses animais foram avaliados em diferentes aspectos comportamentais (campo aberto, teste de inibição pré- pulso, memória de reconhecimento de objeto e memória de trabalho), e filmados ao longo de 71 dias para o monitoramento de crises epilépticas espontâneas recorrentes. Também foram avaliadas a perda neuronal e a expressão de nNOS em diferentes regiões cerebrais. Resultados: NPS reduziu a frequência de crises nos animais com epilepsia e psicose comórbida quando comparados a animais não tratados. NPS também teve efeito ansiolítico no modelo animal de epilepsia com e sem psicose, e diminuiu os correlatos comportamentais de sintomas positivos dos animais no modelo de psicose e no de epilepsia + psicose, além de reverter o prejuízo no filtro sensório motor nos animais que receberam pilocarpina e quetamina. No reconhecimento de objeto o modelo de epilepsia e epilepsia+psicose o tratamento com NPS não interferiu no desempenho de memória de curto prazo, porém NPS melhorou a memória de longo prazo no modelo de psicose. NPS preservou regiões como o córtex entorrinal e subiculum nos animais epilépticos, mas a camada granular e córtex pré-límbico revelaram perda significativa nos animais controles. Alta expressão de nNOS em diferentes regiões cerebrais foram visualizadas nos animais com epilepsia, com destaque para aqueles que receberam tratamento com NPS. Conclusão: O tratamento com NPS foi efetivo na amenização de sintomas correlatos comportamentais de psicose no modelo puro de esquizofrenia e no comórbido VIII com epilepsia. Além disso, não exacerbou crises e contribuiu para diminuição delas nos animais do modelo de epilepsia e psicose, que apresentou grandes similaridades com o que é encontrado em casos clínicos. Nossos resultados sugerem que o uso do NPS pode ter resultados na melhoria dos sintomas da psicose interictal humana, assim como já observado para a esquizofrenia. Introdution: Schizophrenia is a major mental disorder that affects 1% of young adults and has a great impact on quality of life, behavior, and cognition. Despite the high social burden, little is known about the pathophysiology and etiology of schizophrenia. Patients with psychotic disorders have increased risk of developing epilepsy, and patients with temporal lobe epilepsy have a high frequency of psychoses. The use of experimental animal models of epilepsy and schizophrenia may help to better understand the neurobiology of these diseases and play an important role in the development of potential new therapeutic strategies. The complex interactions of seizures and psychotic symptoms are being unveiled. Nitric oxide (NO) is an important modulator of neurotransmission and NO donors such as sodium nitroprusside (SNP) have shown promising effects in schizophrenic patients. In animal models of epilepsy, NO may exert pro- or anticonvulsant effects, suggesting that the use of SNP in patients with epilepsy and psychosis may not be so straightforward. Objectives: To develop an animal model of epilepsy and comorbid psychosis, and compare it from the behavioral and neuropathological point of view with pure animal models of epilepsy and schizophrenia. It was hoped, to verify the possible modulation triggered by the treatment with SNP. Metodology: Males Wistar rats weighing 260-300g were divided in controls group (SAL+SAL), pure epilepsy (PILO+SAL), schizophrenia (SAL+QUET), comorbid psychosis (PILO+KET) and their versions treated with SNP (SAL+SAL+SNP, PILO+SAL+SNP, SAL+KET+SNP and PILO+KET+SNP). These animals were evaluated in a variety of behavioral tests (open field, prepulse inhibition startle reflex, object recognition and working memory), and were filmed over 71 days to monitor spontaneous recurrent seizures. We also evaluated neuronal loss and nNOS expression in different brain regions. Results: SNP reduced seizure frequency in animals with epilepsy and psychosis when compared to those not treated with SNP. SNP also showed anxiolytic effects in the animal model of epilepsy with or without psychosis, decreased behavioral correlates of positive symptoms in the animal model of epilepsy + psychosis, and prevented sensorimotor gating deficits in epilepsy + psychosis IX model, The object recognition test showed that in epilepsy and epilepsy + psychosis models the treatment with SNP did not interfere with short-term memory performance, but SNP improved long-term memory in the psychosis model. SNP preserved brain regions like entorhinal cortex and subiculum in epileptic animals, but the granular layer and prelimbic cortex revealed significant loss in controls animals. High expression of NOS in same brain regions was observed in the animal model of epilepsy, especially in the animals receiving SNP. Conclusion: Treatment with SNP was effective in ameliorating symptoms of behavioral correlates of psychosis in the pure model of schizophrenia and the model comorbid with epilepsy. Moreover, SNP did not exacerbate seizures and reduced seizure frequency in the animal model of epilepsy + psychosis, which showed striking similarities to clinical cases. Our results suggest that the use of SNP could ameliorate symptoms of human interictal psychosis, such as those observed in schizophrenia.
Published: 2018

46. Double-blind, placebo-controlled trial of the effects of sodium nitroprusside on P300 and MMN auditory evoked potentials in schizophrenia

Author: Juliana Silva de Almeida, João Paulo Machado de Sousa, João Paulo Maia de Oliveira, and Antonio Waldo Zuardi
Abstract: INTRODUÇÃO: A esquizofrenia é um transtorno que se caracteriza pela desorganização de diversos processos mentais, dentre os quais a cognição. Pacientes com esquizofrenia apresentam alterações na amplitude e latência dos potenciais evocados P300 e MMN. A maioria das drogas antipsicóticas atuais têm pouco efeito sobre os sintomas negativos e prejuízos cognitivos dos pacientes, por isso, pesquisadores têm buscado alternativas farmacológicas que possam agir sobre os prejuízos cognitivos e sintomas negativos. Pesquisas recentes demonstraram que o nitroprussiato de sódio (NPS) é capaz de atenuar algumas das manifestações do transtorno que não respondem adequadamente aos tratamentos hoje disponíveis. OBJETIVO: Investigar os efeitos da infusão de NPS sobre a sintomatologia e os potenciais evocados auditivos MMN e P300 em pacientes com esquizofrenia em um ensaio duplo-cego controlado por placebo. MÉTODO: Foram avaliados 12 pacientes com idade entre 25 e 54 anos em tratamento antipsicótico acompanhados no Hospital das Clínicas da Faculdade de Medicina de Ribeirão Preto. Cada paciente participou de duas sessões experimentais, uma com infusão de NPS e outra com placebo. Escalas psiquiátricas (BPRS e PANSS) foram aplicadas imediatamente antes da infusão de NPS ou soro glicosado, a cada hora durante a infusão e imediatamente após a realização dos exames de P300 e MMN, realizados após o fim da infusão. RESULTADOS: A infusão de NPS foi associada a um aumento significativo da amplitude do potencial evocado MMN e a uma redução nos escores das escalas de sintomas psiquiátricos BPRS e PANSS em comparação com o placebo. CONCLUSÃO: A infusão de NPS foi associada à melhora dos sintomas de esquizofrenia conforme medidos pela BPRS e PANSS e a um aumento da amplitude do potencial evocado MMN. Não houve efeitos da administração do NPS sobre o potencial evocado P300. INTRODUCTION: Schizophrenia is a mental disorder characterized by disorganization of several mental processes including cognition. Schizophrenia patients present alterations in the amplitude and latency of auditory evoked potentials P300 and MMN. Most current antipsychotics have little or no effect on the negative symptoms or cognitive impairment in schizophrenia, which led researchers to search for pharmacological alternatives that may counteract these manifestations. Recent evidence suggests that sodium nitroprusside (SNP) is able to ameliorate some of the manifestations associated with schizohrenia that do not respond adequately to currently available treatments. OBJECTIVE: To investigate the effects of SNP on schizophrenia symptoms and on the evoked potentials P300 and MMN in a double-blind, placebocontrolled trial. METHODS: The trial involved 12 patients aged 25-54 years in antipsychotic treatment followed up at the Ribeirã Preto Medical School University Hospital. Each patient attended two experimental sessions, one for the infusion of SNP and another for the infusion of placebo. The Brief Psychiatric Rating Scale (BPRS) and the Positive and Negative Syndromes Scale (PANSS) were completed immediately before the infusion, every consecutive hour, and immediately after the P300 and MMN tests, performed after the end of the infusion. RESULTS: The infusion of SNP was associated with a significant increase in the amplitude of MMN and with a reduction in the psychopathology scores of the BPRS and PANSS compared to placebo. CONCLUSION: The administration of SNP was associated with an improvement in schizophrenia symptoms as measured with the BPRS and PANSS and with an increase in the amplitude of the evoked potential MMN. There were no effects of SNP on the evoled potential P300.
Published: 2017

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