Examination of the Skills of Cognitive Therapy for Depression: Evaluating Specificity and Prediction of Differential Response in Cognitive and Behavioral Treatments

Hollars, Shannon N.

13 August 2015

No description available.

Psychology

Psychotherapy

Behavioral Sciences

Clinical Psychology

Cognitive Therapy

Depression

Major Depressive Disorder

Cognitive and Behavioral Interventions

Cognitive Therapy

Cognitive Therapy Skills

Cognitive and Behavioral Change

A New Role for Vitamin D Binding Protein in Bipolar Disorder

Petrov, Brawnie Rebecca

03 August 2017

No description available.

Nutrition

vitamin D binding protein

bipolar disorder

major depressive disorder

inflammation

DBP-MAF

macrophage activating factor

inflammation

western blot

glycosylation

actin

immunoprecipitation

bait

Clinical Course of Children with a Depressive Spectrum Disorder and Transient Manic Symptoms

Nadkarni-DeAngelis, Radha Bhaskar

26 June 2009

No description available.

Psychology

depression

mania

hypomania

irritability

children

conversion

bipolar disorder

depressive disorder

aggression

medication

dysthymia

major depressive disorder

risk factors

family history

family environment

clinical presentation

C-GAS

ADHD

Evidence Synthesis, Practice Guidelines and Real-World Prescriptions of New Generation Antidepressants in the Treatment of Major Depressive Disorder: A Meta-epidemiological Study / 大うつ病に対する第2世代抗うつ薬に関するエビデンス統合と診療ガイドラインと実際の処方の比較研究

Luo, Yan

23 March 2022

京都大学 / 新制・課程博士 / 博士(医学) / 甲第23756号 / 医博第4802号 / 新制||医||1056(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 中山 健夫, 教授 村井 俊哉, 教授 小杉 眞司 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

Evidence-based medicine

Network meta-analysis

Clinical practice guideline

Major depression

Antidepressant

Evidence evolution

Confidence in the evidence

Shiny

Visualization

Major depressive disorder

Trend

Suboptima dose

490

EMOTIONAL MEMORY IN PREGNANT WOMEN AT RISK FOR POSTPARTUM DEPRESSION

Williams, Marissa

10 1900

<p>Thank you to all who were involved in this research including Drs. Benicio Frey,<br />Sue Becker, Margaret McKinnon, Luciano Minuzzi, and Lauren Cudney and Marg Coote. I would like to express my very great appreciation to the midwives at Community Midwives of Hamilton for enabling me to visit the clinic and recruit their pregnant clients. Finally, I would like to thank Lorenda Williams, John Williams, and Eric Johnson for their continued support.</p> / <p>Postpartum depression (PPD) is a serious disorder associated with debilitating effects on mothers and their infants. A previous history of depression appears to be the strongest risk factor for PPD. Previous studies showed that individuals with history of depression accurately recall more negative compared to positive content. The objective of this study was to compare emotional memory for negative and positive images between pregnant women with previous depressive episodes and pregnant women with no lifetime depression. This is the first study to investigate emotional memory in pregnant women with or without previous history of Major Depressive Disorder (MDD). A total of 77<br />participants between the ages of 18 - 44 (mean age: 27.3  6.2yo) completed the study (14 pregnant women with previous depressive episodes, 30 pregnant women with no lifetime depression, 13 non-pregnant women with previous depressive episodes, and 20 non-pregnant healthy). Participants took part in an emotional encoding task consisting of positive, negative, and neutral images from the International Affective Picture System (IAPS) where they were asked to rate these images based on perceived emotional intensity. Participants returned a week later for a surprise incidental recognition memory task. A multivariate general linear model revealed a significant main effect of group (F(1,71)= 8.04, p=.01). Women with history of MDD demonstrated poorer memory performance than women with no history for negative images, but the two groups did not<br />differ on memory for positive images. This suggests that having a history of depression selectively impaired the memory recognition of negative images.</p> / Master of Science (MSc)

Emotional Memory

Cognition

Pregnancy

Postpartum Depression

Major Depressive Disorder

Hormones

Cognitive Neuroscience

Cognitive Psychology

Maternal and Child Health

Mental Disorders

Women's Health

Cognitive Neuroscience

Predictors of Major Depressive Disorder following Intensive Care of Chronically Critically Ill Patients

Wintermann, Gloria-Beatrice, Rosendahl, Jenny, Weidner, Kerstin, Strauß, Bernhard, Petrowski, Katja

13 December 2018

Objective. Major depressive disorder (MDD) is a common condition following treatment in the Intensive Care Unit (ICU). Long-term data on MDD in chronically critically ill (CCI) patients are scarce. Hence, the primary aim of the present study was to investigate the frequency and predictors of MDD after intensive care of CCI patients. Materials and Methods. In a prospective cohort study, patients with long-term mechanical ventilation requirements () were assessed with respect to a diagnosis of MDD, using the Structured Clinical Interview for DSM-IV, three and six months after the transfer from acute ICU to post-acute ICU. Sociodemographic, psychological, and clinical risk factors with values ≤ 0.1 were identified in a univariate logistic regression analysis and entered in a multivariable logistic regression model. A mediator analysis was run using the bootstrapping method, testing the mediating effect of perceived helplessness during the ICU stay, between the recalled traumatic experience from the ICU and a post-ICU MDD. Results. 17.6% () of the patients showed a full- or subsyndromal MDD. Perceived helplessness, recalled experiences of a traumatic event from the ICU, symptoms of acute stress disorder, and the diagnosis of posttraumatic stress disorder (PTSD) after ICU could be identified as significant predictors of MDD. In a mediator analysis, perceived helplessness could be proved as a mediator. Conclusions. Every fifth CCI patient suffers from MDD up to six months after being discharged from ICU. Particularly, perceived helplessness during the ICU stay seems to mainly affect the long-term evolvement of MDD. CCI patients with symptoms of acute stress disorder/PTSD should also be screened for MDD.

info:eu-repo/classification/ddc/610

ddc:610

Patterns of symptoms in major depressive disorder and genetics of the disorder using low-pass sequencing data

Li, Yihan

January 2013

My thesis aims at identifying both genetic and environmental causes of major depressive disorder (MDD), using a large case-control study: 6,000 Chinese women with recurrent MDD and 6,000 controls. One of the major challenges for conducting genetic research on MDD is disease heterogeneity. The first question addressed is how different MDD is from highly comorbid anxiety disorders. I examine how anxiety disorders predict clinical features of depression and the degree of heterogeneity in their predictive pattern. The second question addressed is whether clinically defined MDD is a single disorder, or whether it consists of multiple subtypes. Results are then compared with and interpreted in the context of Western studies. Furthermore, latent class analysis and factor analysis results are also used in association analysis to explore more genetically homogeneous subtypes. Genetic data were derived using a novel strategy, low pass whole genome sequence analysis. Using genotypes imputed from the sequence data, I show that a cluster of single nucleotide polymorphisms (SNPs) is significantly associated with a binary disease phenotype including only cases with = 4 episodes of MDD, suggesting that recurrence might be an indication of genetic predisposition. The third issue examined is the contribution of rare variants to disease susceptibility. Again using sparse sequence data, I identified exonic sequence variants and performed gene-based analysis by comparing the number of variants between cases and controls in every gene. Furthermore I performed gene enrichment test by combining P values of SNP association tests at different minor allele frequency ranges. Overall, I did not find convincing evidence that rare variants aggregately contribute to disease susceptibility. However, the gene-based analysis resulted in an unexpected finding: cases have an excess of variants in all thirteen-protein coding mitochondrial genes, which was due to copy number differences in the mitochondrial genome. Both human phenotypic data as well as mice experimental data show that the increase in the mitochondrial copy number in cases is due to chronic stress.

616.85

Dépression majeure et douleur : deux problématique liées, mais à quel point?

Fortin-Fournier, Simon

03 1900

La dépression majeure et les douleurs chroniques sont deux problématiques distinctes, mais liées par une comorbidité élevée et un effet néfaste sur la qualité de vie des individus atteints. Ce mémoire est consacré aux liens qui les unissent et présente deux études. L’étude 1 évalue l’impact de la déplétion aiguë du tryptophane sur les mécanismes endogènes de freinage de la douleur chez des participants sains. L’étude 2 évalue l’intégrité des mécanismes endogènes de freinage de la douleur chez des patients souffrant de dépression majeure (DM) avant et après un traitement aux antidépresseurs à double action (Duloxétine ou Desvenlafaxine). Les données des patients de l’étude 2 sont aussi comparées à celles d’un groupe de sujets sains pour mieux comprendre l’effet de la DM sur les mécanismes endogènes de freinage de la douleur. L’étude 1 montre que la déplétion aiguë du tryptophane bloque les mécanismes endogènes de freinage de la douleur. L’étude 2 montre que les patients souffrant de DM ont une capacité de freinage de la douleur intacte, qui est réduite par l’administration de médicaments. En conclusion, les mécanismes de freinage de la douleur semblent affectés par la déplétion aiguë du tryptophane. Les participants en DM ont une capacité d’inhibition de la douleur préservée par rapport aux sujets sains et affectée suite à la prise du médicament. Ces résultats permettent d’envisager un écart théorique entre la DM et les douleurs chroniques. / While major depression and chronic pain are distinct set of issues, they share high comorbidity rates and are both detrimental to those who suffer, affecting their quality of life. Based on two studies, this master’s thesis centers on the relationships between these issues. A first study (1) evaluates the effect of acute tryptophan depletion on endogenic mechanisms of pain reduction. A second study (2) assesses the endogenic mechanisms of pain reduction of patients who suffer from major depressive disorders (MDD) before and after the intake of a dual action antidepressant (Duxoletine or Desvenlafaxine). In conclusion, study 1 shows that the acute tryptophan depletion inhibits the endogenic mechanisms of pain reduction. Study 2 shows that patients who suffer from MDD have intact pain reduction mechanisms that are reduced by the intake of medication. The results suggest a theoretical gap between notions of MDD and chronic pain.

dépression majeure

douleur

déplétion aiguë du tryptophane

sérotonine

CIDN

Major Depressive Disorder

Pain

Acute Tryptophane Depletion

Serotonin

Duloxetine

Desvenlafaxine

DNIC

Corrélats neuronaux du circuit des récompenses chez les jeunes à risque parental de troubles de l'humeur

Kraushaar, Caroline

04 1900

Cette thèse a pour objectif l’investigation du circuit des récompenses, sur les plans comportementaux et neuronaux, chez des adolescents à risque parental élevé de dépression majeure et de trouble bipolaire, en comparaison à des jeunes à risque parental peu élevé. Plus précisément, le but est d’identifier des marqueurs comportementaux et neuronaux du risque de développer une dépression majeure ou un trouble bipolaire, afin d’être en mesure de détecter et de prévenir ces troubles le plus tôt possible pour éviter, ou du moins retarder, leur émergence. Pour ce faire, nous avons réalisé deux études, présentées ici dans deux articles empiriques. Dans le premier article, le fonctionnement comportemental et neuronal du circuit des récompenses a été investigué au moyen d’une tâche d’anticipation et d’obtention de gains et de pertes monétaires, chez des adolescents à risque parental de dépression majeure (i.e., jeunes asymptomatiques dont un des parents souffre de dépression majeure), des adolescents à risque parental de trouble bipolaire (i.e., jeunes asymptomatiques dont un des parents souffre de trouble bipolaire) et des adolescents contrôles (i.e., jeunes asymptomatiques dont les deux parents sont en bonne santé mentale). Au niveau comportemental, les résultats ont révélé une meilleure performance chez les jeunes à risque de dépression majeure lorsqu’ils devaient éviter d’obtenir des pertes monétaires de magnitude variée (0,20$, 1$ ou 5$), ainsi qu’une meilleure performance chez les jeunes à risque de trouble bipolaire sur les essais impliquant d’éviter des pertes monétaires de magnitude nulle (0$). Au niveau neuronal, les jeunes à risque de dépression majeure démontraient une diminution de l’activation du cortex préfrontal dorsolatéral lors de l’anticipation de potentielles pertes monétaires de magnitude variée, tandis que les jeunes à risque de trouble bipolaire démontraient une diminution de l’activation du cortex préfrontal dorsolatéral lors de l’anticipation de potentielles pertes monétaires de magnitude nulle. De plus, les jeunes à risque de dépression majeure tendaient à démontrer une augmentation de l’activité du cortex orbitofrontal durant l’évitement réussi de pertes monétaires, tandis que les jeunes à risque de trouble bipolaire tendaient à démontrer une augmentation de l’activité du cortex orbitofrontal lors de l’obtention de pertes monétaires. Dans le deuxième article, l’intégrité structurelle des régions fronto-limbiques a été investiguée, au moyen de mesures du volume, de l’épaisseur corticale et de la superficie corticale. Les résultats ont mis en évidence, chez les jeunes à risque de trouble bipolaire, un volume plus élevé du cortex préfrontal dorsolatéral, par rapport aux jeunes à risque de dépression majeure et contrôles. De plus, les jeunes à risque de trouble bipolaire présentaient un volume plus élevé du cortex cingulaire postérieur, en comparaison aux jeunes à risque de dépression majeure. Enfin, une diminution de l’épaisseur corticale du cortex orbitofrontal et du gyrus frontal moyen a été observée chez les adolescents à risque de trouble bipolaire, en comparaison au groupe contrôle. L’ensemble de ces résultats démontre ainsi l’existence de particularités comportementales et d’altérations neuronales sur les plans fonctionnel et structurel, chez des jeunes à risque élevé de troubles de l’humeur, et ce, avant même l’émergence des premiers symptômes thymiques. Plus particulièrement, ces caractéristiques pourraient constituer des marqueurs du risque de développer un trouble de l’humeur. Par conséquent, ces marqueurs pourraient aider à mieux identifier les jeunes qui sont le plus à risque de développer un trouble de l’humeur, et ainsi permettre la mise en place précoce de stratégies préventives adaptées, afin d’éviter des trajectoires développementales psychopathologiques. / This thesis aims to investigate the behavioral and neural reward circuitry, in youths at high parental risk for major depressive and bipolar disorder, in comparison to youths at low parental risk for mood disorders. More specifically, the goal is to identify behavioral and neural markers of the risk to develop a major depressive or a bipolar disorder in order to early detect and prevent these disorders, and ultimately to avoid, or at least delay, their emergence. To do so, we conducted two experiments, presented herein in two empirical articles. In the first article, behavioral and neuronal reward circuitry were investigated in youths at high parental risk for major depressive disorder (i.e, asymptomatic youths which one of the parents is suffering from major depression), youths at high parental risk for bipolar disorder (i.e, asymptomatic youths which one of the parents is suffering from bipolar disorder) and control youths (i.e, asymptomatic youths from mentally healthy parents). Therefore, we used a monetary incentive delay task allowing the assessment of monetary gain and loss anticipation and outcome. Behaviorally, results revealed a better performance in youths at risk for major depressive disorder on trials involving potential losses of various magnitude (0,20$, 1$ or 5$), as well as a better performance in youths at risk for bipolar disorder on trials involving potential null losses (0$). Regarding imaging data, youths at risk for major depressive disorder demonstrated a reduced activity in the dorsolateral prefrontal cortex during the anticipation of potential monetary losses of various magnitude, while youths at risk for bipolar disorder showed a reduced activity in the dorsolateral prefrontal cortex during the anticipation of potential null losses. Moreover, youths at risk for major depressive disorder tended to have an increased activity in the orbitofrontal cortex during successful avoidance of monetary losses, while youths at risk for bipolar disorder tended to demonstrate an increased activity in the orbitofrontal cortex during feedback of monetary losses. In the second article, structural integrity of fronto-limbic regions was investigated, through volumetric, cortical thickness and surface area measures. Results have highlighted, in youths at risk for bipolar disorder, an increased volume in the dorsolateral prefrontal cortex, compared to both youths at risk for major depressive disorder and controls. Moreover, youths at risk for bipolar disorder showed an increased volume in the posterior cingulate cortex, in comparison to youths at risk for major depressive disorder. Finally, a reduced thickness in the orbitofrontal cortex and middle frontal gyrus were observed in youths at risk for bipolar disorder, in comparison to control youths. Taken together, these results demonstrate the existence of behavioral particularities, and neuronal alterations regarding functional and structural data, in youths at high risk for mood disorders, and this, even before the emergence of the first mood symptoms. More specifically, these characteristics might constitute markers of the risk to develop a mood disorder. Consequently, these markers could help to better identify youths who are most at risk to develop a mood disorder, and thus allow the early implementation of adapted preventive strategies to avoid psychopathological developmental trajectories.

trouble dépressif majeur

trouble bipolaire

risque parental

adolescents

circuit des récompenses

imagerie structurelle

major depressive disorder

bipolar disorder

youths

parental risk

reward circuitry

functional magnetic resonnance imaging

structural imaging

Biomarcadores em líquor e em leucócitos no transtorno depressivo maior, comprometimento cognitivo leve e doença de Alzheimer / Biomarkers in cerebrospinal fluid and leukocytes in Major Depressive Disorder, Mild Cognitive Impairment and Alzheimer\'s disease

Bram, Jéssyka Maria de França Monezi

18 April 2017

O acelerado processo de envelhecimento tem trazido não só mudanças no perfil demográfico, mas também no perfil epidemiológico da população. Entre os problemas de saúde encontrados em idosos, merecem destaque os transtornos mentais, visto que acometem cerca de um terço dessa população, sendo os transtornos depressivos e a demência os problemas de saúde mental mais prevalentes. O transtorno depressivo maior (TDM), bem como o comprometimento cognitivo leve (CCL), tem sido associado prejuízo das funções cognitivas, além de aumentar o risco de desenvolvimento de demência, principalmente doença de Alzheimer (DA). Sendo assim, é importante que haja identificação preventiva de pessoas com maior risco para o desenvolvimento de DA a fim de proporcionar um tratamento precoce. Dessa maneira este estudo objetivou comparar os marcadores biológicos envolvidos na cascata amiloide, expressos em leucócitos e líquor, nas condições clínicas TDM, CCL, DA e controles saudáveis. Para tanto, foi determinada a expressão proteica das secretases ADAM10, BACE1 e PSEN1 e do peptídeo A? em leucócitos e líquor pelos métodos de Western Blotting, ELISA e Luminex. Ao analisarmos a expressão das secretases e do peptídeo Abeta em leucócitos não observamos diferenças estatisticamente significantes entre os grupos, exceto pela expressão da proteína PSEN1, que apresentou menores níveis em DA em relação à TDM. Em relação ao líquor, observamos uma significativa diminuição do peptídeo A? no grupo DA quando comparado aos grupos CCL, TDM e também a controles saudáveis; porém não foram observadas diferenças de expressão desse peptídeo entre CCL, TDM e controles saudáveis. Esses resultados sugerem que a matriz leucocitária, apesar de expressar os componentes desta via, sugerindo dispor da maquinaria enzimática necessária para o processamento da proteína precursora do amiloide (APP), não é a ideal para estudos sobre a cascata amiloide. Além disso, os resultados obtidos em amostras de líquor, de acordo com a casuística analisada, reforçam os dados da literatura que estabelecem a redução da concentração do peptídio Abeta no líquor como um biomarcador da DA, sem termos detectado alterações nos demais grupos estudados. Nossos resultados (negativos) em relação à expressão das APP-secretases no líquor acrescentam dados a este domínio ainda controverso da literatura. Assim sendo, mais estudos devem ser realizados para que possamos compreender melhor as vias relacionadas ao desenvolvimento da DA / The accelerated aging process has brought not only changes in the demographic profile, but also in the epidemiological profile of the population. Among the health problems found in the elderly, mental disorders are worth mentioning, since they affect about a third of this population, being the depressive disorders and dementia the most prevalent mental health problems. Major depressive disorder (MDD), as well as mild cognitive impairment (MCI), have been associated with higher levels of cognitive symptoms and increased risk of developing dementia, especially Alzheimer\'s disease (AD). Therefore, it is important to identify individuals at greater risk for the development of AD in order to provide treatment at early stages of the disease process. In this way, this study aimed to compare the biological markers involved in the amyloid cascade under the clinical conditions TDM, CCL, DA and healthy controls expressed in leukocytes and CSF. We determined the protein expression of ADAM10, BACE1 and PSEN1 and A? peptides in leucocytes and CSF using the Western Blotting, ELISA and Luminex methods. When analyzing the expression of the secretases and the A? peptide in leukocytes, we did not observe statistically significant differences between the groups, except for the expression of the PSEN1 protein, which presented lower levels in AD in relation to MDD. In relation to CSF, we observed a significant reduction of the Abeta peptide in AD when compared to MCI, TDM and also to healthy controls, but no differences in expression of this peptide were observed between MCI, MDD and healthy controls. These results suggest that the leukocytes, although expressing the key components and the enzymatic machinery necessary for the proteolytic processing of the amyloid precursor protein (APP), may not represent an adequate biological matrix for studies addessing the amyloid cascade. In addition, results obtained in CSF samples, according to the analyzed series, reinforce the literature data that establish the reduction of A? peptide concentration in CSF as a biomarker of AD, without detecting alterations in the other groups studied. Our (negative) results in relation to the expression of APP-secretases in CDescriptors: MSF add data to this still controversial domain of the literature. Therefore, more studies should be done so that we can better understand the pathways related to the development of AD

ADAM10

ADAM10

Alzheimer's disease

BACE1

Cerebrospinal fluid

Comprometimento cognitivo leve

Doença de Alzheimer

Leucócitos

Leukocytes

Líquor

Major depressive disorder

Mild cognitive Impairment

Peptide beta-amiloides

Peptídeos beta-amiloides

Presenilina-1

Transtorno depressivo maior