Evidence-based guidelines for pharmacological treatment of anxiety disorders

Baldwin, David S., Anderson, Ian M., Nutt, David J., Bandelow, Borwin, Bond, Alyson, Davidson, Jonathan R. T., den Boer, Johan A., Fineberg, Naomi A., Knapp, Martin, Scott, Jan, Wittchen, Hans-Ulrich

30 January 2013

These British Association for Psychopharmacology guidelines cover the range and aims of treatment for anxiety disorders. They are based explicitly on the available evidence and are presented as recommendations to aid clinical decision making in primary and secondary medical care. They may also serve as a source of information for patients and their carers. The recommendations are presented together with a more detailed review of the available evidence. A consensus meeting involving experts in anxiety disorders reviewed the main subject areas and considered the strength of evidence and its clinical implications. The guidelines were constructed after extensive feedback from participants and interested parties. The strength of supporting evidence for recommendations was rated. The guidelines cover the diagnosis of anxiety disorders and key steps in clinical management, including acute treatment, relapse prevention and approaches for patients who do not respond to first-line treatments.

Antiepileptika

Antidepressiva

Antipsychotika

Angststörungen

Anxiolytika

Benzodiazepane

kognitive Verhaltenstherapie

evidenzbasierte Richtlinien

generalisierte Angststörung

Zwangsstörung

Panikstörung

posttraumatische Belastungsstörung

Phobie

Behandlung

SSRI

Venlafaxin

Anticonvulsants

antidepressants

antipsychotics

anxiety disorders

anxiolytics

benzodiazepines

cognitive behaviour therapy

evidence-based guidelines

generalised anxiety disorder

obsessive-compulsive disorder

panic disorder

post-traumatic stress disorder

simple phobia

social phobia

SSRI

treatment

venlafaxine

ddc:150

rvk:CU 3100

rvk:CU 8500

Le contexte comme élément distinctif entre les intrusions normales et les intrusions anormales

Audet, Jean-Sébastien

06 1900

No description available.

trouble obsessionnel compulsif

TOC

confusion inférentielle

croyances obsessionnelles

thérapie cognitive comportementale

TCC

approche basée sur les inférences

contexte

égo-dystonie

obsessive-compulsive disorder

OCD

inferential confusion

obsessive beliefs

cognitive-behaviour therapy

CBT

inference based approach

context

egodystonicity

Ativação cerebral associada à memória episódica verbal no transtorno obsessivo-compulsivo por meio de ressonância magnética funcional / Brain activation associated with verbal episodic memory in obsessivecompulsive disorder using magnetic resonance imaging

Marcelo Camargo Batistuzzo

19 February 2014

O transtorno obsessivo-compulsivo (TOC) é um transtorno psiquiátrico que acomete cerca de 1 a 3,1% das pessoas ao longo da vida. Embora o seu modelo neurobiológico ainda não esteja completamente estabelecido, inúmeras evidências apontam para áreas relacionadas ao circuito córtico-estriado-pálido-talâmico-cortical (CEPTC). Em especial, o córtex órbito-frontal (COF) é uma região que desempenha um papel fundamental dentro da hipótese fisiopatológica do TOC. Paralelamente, esta região já foi associada, em sujeitos saudáveis, com a habilidade de utilização espontânea da estratégia de agrupamento semântico na memorização de palavras - o que facilita sua evocação posterior. Ao mesmo tempo, estudos neuropsicológicos evidenciaram que pacientes com TOC apresentam déficits na memória episódica verbal (MEV) e que tais déficits poderiam ser mediados por dificuldades em funções executivas ligadas ao planejamento, como utilização de estratégias. Portanto, para testar a hipótese de que há diferenças no correlato neural da codificação da MEV entre pacientes com TOC e controles saudáveis, foi utilizado um teste neuropsicológico adaptado para ressonância magnética funcional (RMf): o paradigma tinha apresentação em bloco. O objetivo do presente estudo foi investigar a etapa de codificação da MEV e a capacidade de agrupamento semântico espontâneo em crianças e adolescentes com TOC. Assim, o paradigma foi constituído por duas listas de palavras: uma, semanticamente relacionada (SR), na qual as palavras eram divididas em categorias semânticas e outra, não relacionada (NR), na qual não havia relação aparente entre as palavras. O contraste de maior interesse do estudo foi a diferença entre essas duas condições (SR > NR). O nível de agrupamento semântico foi quantificado por um índice semântico. Os grupos foram formados por 25 crianças e adolescentes com TOC e 25 controles saudáveis, pareados por sexo, idade, escolaridade, preferência manual e QI. Embora os grupos estivessem pareados por essas características, eles se diferiram em sintomas clínicos, tais como sintomas de depressão, ansiedade e necessidade de rotina por parte da criança/adolescente. Os resultados comportamentais do teste de MEV mostraram que os grupos não se diferenciaram: ambos evocaram a mesma quantidade de palavras e não apresentaram diferenças no índice semântico. Apesar disso, a comparação entre os grupos - controlada para variáveis clínicas - revelou menor ativação (sinal BOLD) nos pacientes em diversas regiões cerebrais: frontais, parietais e occipito-temporais. Por outro lado, a análise de interação psicofisiológica (PPI) revelou que os pacientes apresentaram um aumento da conectividade do COF com regiões temporais em relação aos controles. Isso ocorreu para três das quatro regiões de interesse que foram posicionadas no COF: lateral e medial de ambos os hemisférios. Além disso, o grupo de pacientes apresentou uma correlação positiva entre o índice semântico e o efeito BOLD no COF, o que não ocorreu para o grupo controle. Esses resultados indicam diferenças no funcionamento cerebral de crianças e adolescentes com TOC tanto em regiões que estão dentro do modelo neurobiológico proposto para o TOC (circuito CEPTC), como fora dele também. De acordo com os resultados do presente estudo, as diferenças de ativação e de conectividade poderiam ser consideradas como um déficit latente, uma vez que ambos os grupos apresentaram o mesmo desempenho no paradigma / The obsessive-compulsive disorder (OCD) is a psychiatric disorder that affects 1-3.1% of the general population (lifetime rate). Although its neurobiological model has not been completely establish, numerous evidences indicate that areas of the cortico-striatalpale- thalamic-cortical (CSPTC) circuit are engaged in the disease. In particular, the orbitofrontal cortex (OFC) is a region that plays a key role in the pathophysiological hypothesis of OCD. In parallel to this, in healthy controls this region has been associated with the ability of using spontaneous strategies of semantic clustering at the encoding of related words - in a way that facilitates the posterior retrieval of these words. At the same time, neuropsychological studies showed that OCD patients present verbal episodic memory (VEM) deficits, and that these deficits could be mediated by executive dysfunction - like planing and utilization of strategies. Thus, to investigate the hypothesis that there are differences at the neural correlates of VEM encoding between children and adolescents with OCD and healthy controls, we used a blocked design functional Magnetic Resonance Imaging (fMRI) paradigm to evaluate both groups. The main objective of the study was to investigate the VEM encoding and the ability to spontaneously organize words according to their semantic categories. In order to do this, the fMRI paradigm consisted of two kinds of word lists: a semantically related list (SR), in which words were divided into semantic categories and a unrelated list (UR), were there was no apparent relationship between the words. However, the contrast of most interest of this study, was the difference between the conditions (\'SR > UR\'). The semantic clustering level was quantified by a semantic clustering index. Groups were constituted by 25 children and adolescents with OCD and 25 healthy controls paired by gender, age, educational level, handedness and IQ. Although both groups were matched for these characteristics, they differed in clinical symptoms such as depression, anxiety and routines. Behavioral results showed that the groups were similar in terms of retrieved words and semantic index. Nevertheless, the comparison between groups - controlled for clinical variables - showed less activation (BOLD signal) in patients in several brain regions: frontal, parietal and occipito-temporal. On the other hand, the psychophysiological interaction analysis (PPI) revealed that patients have had an increase in the OFC connectivity with the temporal regions. This has occurred in three of the four regions of interest that were placed in the OFC: lateral and medial of both hemispheres. Also, the patients showed a positive correlation between the semantic index and the BOLD effect in the OFC, which was not observed in the control group. These results suggest that there are differences in brain functioning of children and adolescents with OCD in regions that are inside/outside of the neurobiological model for OCD (CSPTC circuit). In accordance with the present results, these differences in brain activation and connectivity could be regarded as a latent deficit, since both groups presented the same behavioral performance

Adolescente

Cognição

Córtex pré-frontal

Criança

Imagem por ressonância magnética

Mapeamento encefálico/psicologia

Memória

Memória episódica

Neuroimagem funcional/psicologia

Psiquiatria biológica

Psiquiatria infantil

Semântica

Testes neuropsicológicos

Transtorno obsessivo-compulsivo

Adolescent

Biological psychiatry

Brain mapping/psychology

Child

Child psychiatry

Cognition

Functional neuroimaging/psychology

Magnetic resonance imaging

Memory

Memory episodic

Neuropsychological tests

Obsessive-compulsive disorder

Prefrontal cortex

Semantics

Evidence-based guidelines for pharmacological treatment of anxiety disorders: Recommendations from the British Association for Psychopharmacology

Baldwin, David S., Anderson, Ian M., Nutt, David J., Bandelow, Borwin, Bond, Alyson, Davidson, Jonathan R. T., den Boer, Johan A., Fineberg, Naomi A., Knapp, Martin, Scott, Jan, Wittchen, Hans-Ulrich

January 2005

These British Association for Psychopharmacology guidelines cover the range and aims of treatment for anxiety disorders. They are based explicitly on the available evidence and are presented as recommendations to aid clinical decision making in primary and secondary medical care. They may also serve as a source of information for patients and their carers. The recommendations are presented together with a more detailed review of the available evidence. A consensus meeting involving experts in anxiety disorders reviewed the main subject areas and considered the strength of evidence and its clinical implications. The guidelines were constructed after extensive feedback from participants and interested parties. The strength of supporting evidence for recommendations was rated. The guidelines cover the diagnosis of anxiety disorders and key steps in clinical management, including acute treatment, relapse prevention and approaches for patients who do not respond to first-line treatments.

info:eu-repo/classification/ddc/150

ddc:150

Overactive Performance Monitoring in Obsessive-Compulsive Disorder: Unraveling Affective Processes and Modulation by Non-Invasive Brain Stimulation

Balzus, Luisa

15 July 2024

Eine überaktive Überwachung eigener Handlungen, welche sich in erhöhten Amplituden der error-related negativity (ERN) zeigt, scheint eine zentrale Rolle in der Pathophysiologie der Zwangsstörung zu spielen. Die funktionelle Bedeutsamkeit der ERN, die Mechanismen, die zur erhöhten ERN bei Zwangsstörungen beitragen und der Nutzen der ERN als Ansatzpunkt für Interventionen sind jedoch nicht vollständig geklärt. Diese Dissertation umfasst drei Studien, deren Ziel es war, diese Aspekte zu untersuchen. Studie 1 untersuchte die affektive Bewertung eigener Handlungen und zeigte, dass Handlungen automatisch affektive Valenz zugeschrieben wird. Darauf aufbauend untersuchte Studie 2, ob die ERN die Valenzbewertung von Fehlern widerspiegelt und ob eine veränderte Fehlerbewertung zur erhöhten ERN bei Zwangsstörungen beiträgt. Die Ergebnisse zeigten, dass Personen mit Zwangsstörung eine verminderte Valenzbewertung von Fehlern aufweisen, lieferten aber keine Hinweise auf einen Zusammenhang zwischen ERN und Fehlerbewertung, was nahelegt, dass eine veränderte Fehlerbewertung nicht der erhöhten ERN bei Zwangsstörungen zugrunde liegt. Studie 3 untersuchte, ob die ERN durch nicht-invasive Hirnstimulation modulierbar ist und lieferte Hinweise darauf, dass kathodale transkranielle Gleichstromstimulation über dem prä-supplementär motorischen Areal die ERN bei gesunden Personen und Personen mit Zwangsstörung reduziert. Zusammenfassend zeigen die Studien, dass die Handlungsüberwachung die affektive Bewertung eigener Handlungen umfasst und dass dieser Prozess bei Zwangsstörungen verändert ist; eine veränderte Fehlerbewertung scheint jedoch nicht der erhöhten ERN bei Zwangsstörungen zugrunde zu liegen. Diese Erkenntnisse tragen zum Verständnis neurokognitiver Veränderungen bei dieser Störung bei. Zudem zeigen die Ergebnisse, dass nicht-invasive Hirnstimulation das Potenzial hat, die ERN bei Personen mit Zwangsstörung abzuschwächen. Dies könnte den Weg für neue Interventionsstrategien ebnen. / Overactive performance monitoring, as indicated by increased amplitudes of the error-related negativity (ERN), is considered to play a central role in the pathophysiology of obsessive-compulsive disorder (OCD). However, the functional significance of the ERN, the mechanisms contributing to increased ERN amplitudes in OCD, and the utility of the ERN as a target for intervention are not fully understood. This dissertation comprises three studies that aimed to shed light on these questions. Study 1 examined the affective evaluation of own actions, revealing that affective valence is automatically assigned to actions. Building upon this, Study 2 investigated whether the ERN reflects the valence evaluation of errors and whether altered error evaluation contributes to heightened ERN magnitude in OCD. The results indicated that individuals with OCD show reduced valence evaluation of errors, yet they provided no evidence for an association between ERN and error evaluation, suggesting that altered error evaluation may not underlie elevated ERN magnitude in OCD. Study 3 investigated whether the ERN can be modulated by non-invasive brain stimulation, and provided tentative evidence that cathodal transcranial direct current stimulation over the presupplementary motor area reduces the ERN in healthy individuals and individuals with OCD. In summary, the studies provide evidence that performance monitoring encompasses the affective evaluation of own actions and demonstrate that this process is altered in OCD; however, aberrant error evaluation does not seem to underlie heightened ERN amplitudes in OCD. These insights contribute to the understanding of neurocognitive alterations in this disorder. Additionally, the results suggest that non-invasive brain stimulation has the potential to attenuate the ERN in individuals with OCD, which may pave the way for novel intervention strategies.

Zwangsstörung

Handlungsüberwachung

Fehlerverarbeitung

affektive Verarbeitung

EEG

ereigniskorrelierte Potentiale

fehlerbezogene Negativierung

nicht-invasive Hirnstimulation

transkranielle Gleichstromstimulation

obsessive-compulsive disorder

performance monitoring

error processing

affective processing

EEG

event-related potentials

error-related negativity

non-invasive brain stimulation

transcranial direct current stimulation

150 Psychologie

ddc:150

Analysis of genetic variation in microrna-mediated regulation and the susceptibility to anxiety disorders

Muiños Gimeno, Margarita

18 December 2009

We have investigated genetic variation in microRNA-mediated regulation as a susceptibility factor for anxiety disorders following two different approaches. We first studied two isoforms of the candidate gene NTRK3 by re-sequencing its different 3'UTRs in patients with Panic (PD) and Obsessive Compulsive disorders (OCD) as well as controls. Two rare variants that altered microRNA-mediated regulation were identified in PD. Conversely, association of a common SNP with OCD hoarding subtype was found. Moreover, we have also studied a possible involvement of microRNAs in anxiety disorders. Consequently, we have analysed the genomic organisation and genetic variation of miRNA-containing regions to construct a panel of SNPs for association analysis. Case-control studies revealed several associations. However, it is worth remarking the associations of miR-22 and miR-488 with PD; two microRNAs for which functional assays and transcriptome analysis after microRNA overexpression showed significant repression of a subset of genes involved in physiological pathways linked to PD development. / Hem investigat la variació genètica a la regulació mediada per microRNAs com a factors de susceptibilitat pels trastorns d'ansietat seguint dues aproximacions diferents. Primer vam estudiar dues isoformes del gen candidat NTRK3 mitjançant la reseqüenciació dels seus diferents 3'UTRs a pacients de pànic (TP), a pacients amb trastorn obsessiu compulsiu (TOC) i a controls. Dues variants rares que alteren la regulació mediada per microRNAs foren identificades per TP. D'altra banda, es trobà associació d'un SNP comú amb el subtipus acumulador de TOC. A més, també hem estudiat la possible implicació dels microRNAs als trastorns d'ansietat. Conseqüentment, hem analitzat l'organització genòmica i la variació genètica a regions que contenen microRNAs per construir un panell d'SNPs per fer anàlisis d'associació. Els estudis cas-control van revelar algunes associacions. Tanmateix, val la pena destacar les associacions del miR-22 i el miR-488 amb TP; dos microRNAs pels quals assajos funcionals i anàlisis de transcriptoma després de la seva sobreexpressió han mostrat una repressió significativa d'un grup de gens implicats en vies fisiològiques lligades al desenvolupament del TP.

isoforma

anàlisi de transcriptoma

PCR

assaig de luciferasa

variant comuna

variant rara

reseqüenciar

estudis d'associació

poly-miRTS

trastorn obsessiu-compulsiu

trastorn de pànic

trastorn d'ansietat

variació genètica intraespecífica

SNP

NTRK3

gen candidat

element regulador

microRNA

variació genòmica

desordres poligènics

trets complexes

isoform

transcriptome analysis

PCR

luciferase assay

common variant

rare variant

re-sequencing

association studies

poly-miRTS

obsessive-compulsive disorder

panic disorder

anxiety disorder

genetic variation within species

SNP

NTRK3

candidate gene

regulatory element

microRNA

genome variation

polygenic disorders

complex traits

57

Evidence-based pharmacological treatment of anxiety disorders, post-traumatic stress disorder and obsessive-compulsive disorder: A revision of the 2005 guidelines from the British Association for Psychopharmacology

Baldwin, David S., Anderson, Ian M., Nutt, David J., Allgulander, Christer, Bandelow, Borwin, den Boer, Johan A., Christmas, David M., Davies, Simon, Fineberg, Naomi, Lidbetter, Nicky, Malizia, Andrea, McCrone, Paul, Nabarro, Daniel, O’Neill, Catherine, Scott, Jan, van der Wee, Nic, Wittchen, Hans-Ulrich

17 September 2019

This revision of the 2005 British Association for Psychopharmacology guidelines for the evidence-based pharmacological treatment of anxiety disorders provides an update on key steps in diagnosis and clinical management, including recognition, acute treatment, longer-term treatment, combination treatment, and further approaches for patients who have not responded to first-line interventions. A consensus meeting involving international experts in anxiety disorders reviewed the main subject areas and considered the strength of supporting evidence and its clinical implications. The guidelines are based on available evidence, were constructed after extensive feedback from participants, and are presented as recommendations to aid clinical decision-making in primary, secondary and tertiary medical care. They may also serve as a source of information for patients, their carers, and medicines management and formulary committees.

info:eu-repo/classification/ddc/610

ddc:610