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Dive into the research topics where Amanda Galvão-de Almeida is active.

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Featured researches published by Amanda Galvão-de Almeida.


Schizophrenia Research | 2011

Are cavum septum pellucidum abnormalities more common in schizophrenia spectrum disorders? A systematic review and meta-analysis

Clarissa Trzesniak; Irismar Reis de Oliveira; Matthew J. Kempton; Amanda Galvão-de Almeida; Marcos Hortes Nisihara Chagas; Maria Cecília Freitas Ferrari; Alaor Santos Filho; Antonio Waldo Zuardi; Daniel Almeida Prado; Geraldo F. Busatto; P.K. McGuire; Jaime Eduardo Cecílio Hallak; José Alexandre S. Crippa

Magnetic resonance imaging (MRI) studies have reported a variety of brain abnormalities in association with schizophrenia. These include a higher incidence of cavum septum pellucidum (CSP), which is consistent with a neurodevelopmental model for this disorder. In this meta-analytic review, we describe and discuss the main CSP MRI findings in schizophrenia spectrum disorders (SSDs) to date. We adopted as keywords cavum and schizophrenia or psychosis, and the inclusion criteria were articles in English, with samples of SSD patients compared to healthy subjects, which used MRI to assess CSP, without time limit. From 18 potential reports, fifteen were eligible to be part of the current review. These studies included 1054 patients with SSD and 866 healthy volunteers. Six out of 15 studies pointed to a higher prevalence of CSP of any size in SSD patients, while five out of 15 showed that subjects with SSD had a greater occurrence of a large CSP than healthy individuals. However, the meta-analysis demonstrated that only the incidence of a large CSP was significantly higher in SSD relative to healthy comparisons (odds ratio=1.59; 95%CI 1.07-2.38; p=0.02). Overall our results suggest that only a large CSP is associated with SSD while a small CSP may be considered a normal neuroanatomical variation. Our review revealed a large degree of variability in the methods employed across the MRI studies published to date, as well as evidence of publication bias. Studies in large, community-based samples with greater standardization of methods should clarify the true significance of CSP in SSD.


Progress in Neuro-psychopharmacology & Biological Psychiatry | 2011

Adhesio interthalamica alterations in schizophrenia spectrum disorders: A systematic review and meta-analysis.

Clarissa Trzesniak; Matthew J. Kempton; Geraldo F. Busatto; Irismar Reis de Oliveira; Amanda Galvão-de Almeida; Joseph Kambeitz; Maria Cecília Freitas Ferrari; Alaor Santos Filho; Marcos Hortes Nisihara Chagas; Antonio Waldo Zuardi; Jaime Eduardo Cecílio Hallak; P.K. McGuire; José Alexandre S. Crippa

Magnetic resonance imaging (MRI) studies have reported a variety of brain abnormalities in association with schizophrenia. These include a higher prevalence of an absent adhesio interthalamica (AI; also known massa intermedia), a gray matter junction that is present between the two thalami in approximately 80% of healthy subjects. In this meta-analytic review, we describe and discuss the main AI MRI findings in schizophrenia spectrum disorders (SSDs) to date. The MEDLINE and ISI Web of Knowledge databases were searched up to December 2010, for studies that used MRI to assess AI in patients with SSD and controls. From fourteen potential reports, eleven were eligible to be part of the current review. These studies included 822 patients with SSD and 718 healthy volunteers. There was a large degree of variability in the MRI methods they employed. Patients with SSD had a higher prevalence of absent AI than healthy volunteers (odds ratio = 1.98; 95% confidence interval 1.33-2.94; p = 0.0008). This association was evident in both male and female SSD subjects, and there was no evidence that the prevalence was related to age or duration of illness. The significance of the absence of an AI for SSD may be clarified by studies in large, longitudinal community-based samples using standardized methods.


Brain Behavior and Immunity | 2011

Lack of association of indoleamine 2,3-dioxygenase polymorphisms with interferon-alpha-related depression in hepatitis C

Amanda Galvão-de Almeida; Lucas C. Quarantini; Aline S. Sampaio; André Castro Lyra; Carmen Lívia Parise; Raymundo Paraná; Irismar Reis de Oliveira; Karestan C. Koenen; Ângela Miranda-Scippa; Camila Guindalini

BACKGROUND Major depression is a frequent adverse effect of interferon-alpha (IFN-α) therapy. Although the indoleamine 2,3-dioxygenase (IDO) enzyme seems to be involved in the pathophysiology of IFN-α-induced depression, no pharmacogenetic study has investigated whether variation in the IDO gene modifies vulnerability to this adverse effect. METHODS A cross-sectional study assessing 277 hepatitis C patients recruited in two specialized outpatient clinics of Brazil. They were interviewed with the Mini International Neuropsychiatric Interview (MINI) approximately 1 month after the end of IFN-α plus ribavirin therapy. Genomic DNA of individuals was extracted from venous blood. Three IDO single-nucleotide polymorphisms (SNPs) were genotyped (rs3824259; rs10089084 and rs35099072). RESULTS MINI indicated that 21.3% of the sample met criteria for a major depressive episode during the course of IFN-α therapy. No association with the diagnosis of a major depressive episode during the course of IFN-α therapy was observed genotype or allele-wise (p>0.05). Current major depression and/or current anxiety disorder was significantly associated with IFN-α-related depression (p<0.005). However, gender, age, route of infection, result of the antiviral treatment, past history of substance use disorders, depression or any other psychiatric disorder showed no association with IFN-α-related depression (p>0.05). CONCLUSIONS Our results suggest no influence of the variants in the IDO gene and the diagnosis of interferon-α-related depression in the Brazilian population. Interferon-α-related depression may impose persistent psychopathology on at least 15% of the depressed patients even 2 years after antiviral therapy termination. The cross-sectional design is a limitation of our study, predisposing memory bias. Prospective pharmacogenetic studies are warranted to continue investigation of the impact of IDO polymorphisms on the development of IFN-α-induced depression.


Cns Spectrums | 2007

Obsessive-Compulsive Disorder: An Open-Label Pilot Trial of Escitalopram

Amanda Galvão-de Almeida; Lucas C. Quarantini; Cristianne R. Góis; Rogério Santos-Jesus; Ângela Miranda-Scippa; Irismar Reis de Oliveira; Helena da Silva Prado; James F. Leckman; Maria Conceição do Rosário

INTRODUCTION Selective serotonin reuptake inhibitors are considered the most effective and well-established pharmacotherapy for the treatment of obsessive-compulsive disorder (OCD), a chronic and disabling condition. However, approximately 40% of patients do not have a significant improvement, suggesting that new medications are needed. This study was designed to investigate the treatment response to escitalopram in OCD patients. METHODS This open-label study involved 11 adult OCD outpatients diagnosed with the Structured Clinical Interview for Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition Axis I Disorders. Data were collected and the treatment response was assessed by an experienced psychiatrist by using the Yale-Brown Obsessive-Compulsive Scale. Subjects received escitalopram 30 mg/day for 12 weeks starting at 10 mg/day. Dosage adjustments were made within 2 weeks, depending on the tolerability of the patient. RESULTS Six of the 11 patients (54.5%) presented a reduction of at least 40% in the baseline total Yale-Brown Obsessive-Compulsive Scale scores. CONCLUSION Despite the small sample size and the open-label nature of this trial, these data suggest that escitalopram may be a useful option for patients with OCD.


World Journal of Biological Psychiatry | 2010

Is the interferon-α-triggered depressive episode a self-limited kind of depression? Four cases of persistent affective symptoms after antiviral treatment in HCV-infected individuals.

Amanda Galvão-de Almeida; Lucas C. Quarantini; Susana Batista-Neves; André Castro Lyra; Raymundo Paraná; Irismar Reis de Oliveira; Ângela Miranda-Scippa; Camila Guindalini

Abstract Objectives. To discuss relevant aspects in a series of cases in which interferon-α-triggered depressive symptoms persisted up to 4 years after therapy cessation in HCV-infected patients. Methods. Two experienced psychiatrists (AGA and LCQ) identified these four cases in a systematic evaluation program of HCV patients in the Hepatology Unit of the Teaching Hospital at the Federal University of Bahia, Brazil. Lifetime psychiatric diagnoses were confirmed by the Mini International Neuropsychiatric Interview (MINI Plus), and a questionnaire was submitted in order to gather clinical and sociodemographic characteristics. Results. In three out of the four cases identified, major depression diagnosis was reached after more than 12 months of interferon-α therapy interruption and, in one case, depression recurred 6 months after antiviral treatment cessation in a patient on antidepressants. The only case that referred a past history of psychiatric diagnosis reported no offer of mental health care despite the presence of a major depressive episode with psychotic features and suicidal behaviour during the cytokine usage. Conclusions. Interferon-α-triggered depression may remain undiagnosed even in tertiary university hospitals, may persist years after the antiviral therapy cessation, and may recur even in patients on adequate antidepressant treatment.


Revista De Psiquiatria Clinica | 2015

Social support and bipolar disorder

Paula Studart; Severino Bezerra Filho; Ana Beatriz Didier Studart; Amanda Galvão-de Almeida; Ângela Miranda-Scippa

Background Bipolar disorder is a chronic condition that affects the functioning of its carriers in many different ways, even when treated properly. Therefore, it’s also important to identify the psychosocial aspects that could contribute to an improvement of this population’s quality of life.Objective Carry out a literature review on the role of social support in cases of bipolar disorder.Method A research on the following online databases PubMed, Lilacs and SciELO was conducted by using the keywords “social support” or “social networks” and “mood disorders” or “bipolar disorder” or “affective disorder,” with no defined timeline.Results Only 13 studies concerning the topic of social support and BD were found in the search for related articles. Generally speaking, the results show low rates of social support for BD patients.Discussion Despite the growing interest in the overall functioning of patients with bipolar disorder, studies on social support are still rare. Besides, the existing studies on the subject use different methodologies, making it difficult to establish data comparisons.


General Hospital Psychiatry | 2014

Serotonin-1A receptor CC genotype is associated with persistent depression related to interferon-alpha in hepatitis C patients

Amanda Galvão-de Almeida; Lucas C. Quarantini; Amanda Guindalini Tartaglioni; André Castro Lyra; Carmen Lívia Parise; Raymundo Paraná; Irismar Reis de Oliveira; Ângela Miranda-Scippa; Camila Guindalini

OBJECTIVE The aim of this study is to investigate the development of depression during interferon-alpha (IFN-α) therapy and the variations in the expression of the serotonin receptor (5-HTR) and transporter (5-HTT) in hepatitis C patients. METHOD Hepatitis C patients (n=277) were given the Mini International Neuropsychiatric Interview at the end of IFN-α therapy. Three polymorphisms were genotyped: the serotonin transporter repeat length polymorphic region [5-HTT gene-linked polymorphic region (5-HTTLPR)], as well as SNPs rs25531 and rs6295, located within the 5-HTTLPR and the transcriptional control region of the 5-HTR1A gene, respectively. RESULTS The diagnosis of current depression, which was associated with IFN-α-related depression (P<.001), demonstrated a statistically significant association with the CC genotype of the 5-HTR1A gene (odds ratio=5.57, 95% confidence interval=1.61-19.24, P=.007). CONCLUSIONS Persistent depression may represent a more specific type of IFN-α-related psychopathology. Future studies need to investigate the genetic risk factors for vulnerability associated with persistent depression. Limitations, such as the studys cross-sectional design, small sample size and retrospective assessment of IFN-α-induced depression diagnosis, must be taken into account while interpreting the results found in this study.


General Hospital Psychiatry | 2010

Can antidepressants prevent interferon-alpha-induced depression? A review of the literature.

Amanda Galvão-de Almeida; Camila Guindalini; Susana Batista-Neves; Irismar Reis de Oliveira; Ângela Miranda-Scippa; Lucas C. Quarantini


Revista Brasileira de Psiquiatria | 2012

The involvement of the orbitofrontal cortex in psychiatric disorders: an update of neuroimaging findings

Andrea Parolin Jackowski; Gerardo Maria de Araújo Filho; Amanda Galvão-de Almeida; Célia Maria de Araújo; Marilia Alves dos Reis; Fabiana Nery; Ilza Rosa Batista; Ivaldo Silva; Acioly L.T. Lacerda


Revista Brasileira de Psiquiatria | 2009

Transtornos de humor e de ansiedade comórbidos em vítimas de violência com transtorno do estresse pós-traumático

Lucas C. Quarantini; Liana R. Netto; Mônica Andrade-Nascimento; Amanda Galvão-de Almeida; Aline S. Sampaio; Angela Miranda-Scippa; Rodrigo Affonseca Bressan; Karestan C. Koenen

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Camila Guindalini

Federal University of São Paulo

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André Castro Lyra

Federal University of Bahia

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Raymundo Paraná

Federal University of Bahia

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Adriana Cardoso

Federal University of Bahia

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