Littérature scientifique sur le sujet « Troubles du spectre de la Schizophrénie »
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Articles de revues sur le sujet "Troubles du spectre de la Schizophrénie"
Divo, C., C. Obascz, F. Ligier et B. Kabuth. « Étude dimensionnelle des phases précoces des troubles affectifs et de la schizophrénie – Étude rétrospective comparative à propos de 100 cas ». European Psychiatry 29, S3 (novembre 2014) : 594–95. http://dx.doi.org/10.1016/j.eurpsy.2014.09.186.
Texte intégralYvon, Florence, et Antoinette Prouteau. « Vers une compréhension de la stigmatisation : quel est le stéréotype associé à la schizophrénie ? » Santé mentale au Québec 42, no 2 (16 novembre 2017) : 125–31. http://dx.doi.org/10.7202/1041919ar.
Texte intégralRakova-Carron, Liuba, et Vassilis Kapsambelis. « La troisième psychose ». Psychologie clinique et projective 34, no 2 (19 décembre 2023) : 35–51. http://dx.doi.org/10.3917/pcp.034.0035.
Texte intégralDhaliwal, Arash K., Anees Bahji et Marlon Danilewitz. « Managing Comorbid Tobacco Use Disorder for Individuals With Schizophrenia : Challenges and Opportunities ». Canadian Journal of Addiction 13, no 4 (décembre 2022) : 53–55. http://dx.doi.org/10.1097/cxa.0000000000000164.
Texte intégralBonnot, Olivier, Paula Herrera et Alice Kuster. « Maladies neurométaboliques traitables associées aux troubles du spectre de la schizophrénie ». La Presse Médicale 44, no 9 (septembre 2015) : 889–97. http://dx.doi.org/10.1016/j.lpm.2015.02.023.
Texte intégralKrebs, M. O., O. Gay, G. Martinez et I. Amado. « Signes neurologiques mineurs et contrôle moteur : ce qu’ils nous apprennent sur la schizophrénie, ses mécanismes et ses frontières ». European Psychiatry 29, S3 (novembre 2014) : 580–81. http://dx.doi.org/10.1016/j.eurpsy.2014.09.282.
Texte intégralFrigaux, Antoine, Joëlle Lighezzolo-Alnot, Renaud Evrard, Jean-Yves Chagnon, Thomas Rabeyron, Catherine Weismann-Arcache et Hélène Suarez-Labat. « Diagnostic différentiel entre troubles du spectre autistique et troubles du spectre de la schizophrénie chez l’adulte : sur la voie d’une approche psychanalytique et projective avec le test de Rorschach ». Bulletin de psychologie N° 583, no 1 (18 janvier 2024) : 61–65. http://dx.doi.org/10.3917/bupsy.583.0061.
Texte intégralMarsili, M., A. C. Stona, D. Sebbane, M. Laporta et J. L. Roelandt. « Implication des usagers et des aidants dans le développement de la classification des troubles mentaux et du comportement, CIM-11 ». European Psychiatry 29, S3 (novembre 2014) : 620–21. http://dx.doi.org/10.1016/j.eurpsy.2014.09.107.
Texte intégralLe Gall, E., et G. Iakimova. « Cognition sociale dans la schizophrénie et les troubles du spectre de l’autisme : points de convergences et différences fonctionnelles ». L'Encéphale 44, no 6 (décembre 2018) : 523–37. http://dx.doi.org/10.1016/j.encep.2018.03.004.
Texte intégralLafleur, Alexis, Isabelle Soulières et Baudoin Forgeot d’Arc. « Cognition sociale et sens de l’agentivité en autisme : de l’action à l’interaction ». Santé mentale au Québec 41, no 1 (5 juillet 2016) : 163–81. http://dx.doi.org/10.7202/1036970ar.
Texte intégralThèses sur le sujet "Troubles du spectre de la Schizophrénie"
Coulon, Nathalie. « Liens entre troubles du spectre autistique et schizophrénies précoces ? » Thesis, Paris 6, 2015. http://www.theses.fr/2015PA066430/document.
Texte intégralContext : Autism spectrum disorders (ASD) , early onset schizophrenia (EOS) or even very early onset schizophrenia (VEOS)... so many terms used these days! Although today, classifications are categorical, work is however increasing to deepen and understand a possible link between ASD and schizophrenia spectrum disorders, and especially a link between ASD and early onset schizophrenia. Objective : To clarify clinical and biological links between ASD and EOS (before age 18) and especially links between ASD and VEOS (before age 13). Méthod: 62 subjects, divided into three groups according to age at onset of schizophrenia : strictly before age 13 (VEOS ), between age 13 and 18 (EOS) and after 18 (Adult Onset Schizophrenia, AOS). For each group, two clinical evaluations are assessed: search early symptoms of autism with the ADI-R (Autism Diagnostic Interview-Revised) and phenotypic evaluation with MINI (Mini International Neuropsychiatric Interview), BPRS (Brief Psychiatric Rating Scale), PANSS (Positive And Negative Symptoms Scale for schizophrenia), STAI (State Trait Anxiety Inventory), TAS (Toronto Alexithymia Scale) et NSS (Neurological Soft Signs). Biological analysis is based on salivary cortisol measurements, collected during a 24-h period (0800h-day 1, 1100h, 1600h, 2400h, 0800h-day2), in order to evaluate the stress response of the hypothalamic-pituitary-adrenal axis. Résults: VEOS symptoms > EOS symptoms > AOS symtoms. The earlier the schizophrenia is and the more present premorbid history of autism is and the more abnormal stress response is (abnormal stress response also present in relatives). Conclusion: A clinico-biological link appears between VEOS and ASD, with early symtoms of autism before thirty six months and stress response abnormalities. Are VEOS different from schizophrenia? Anyway, a diagnosis to know better in order to improve patients and families cares
Le, Gall Eva. « Exploration neurocognitive des liens entre les troubles du spectre schizophrénique et les troubles du spectre autistique : Profils communs et différences fonctionnelles dans les domaines du fonctionnement cognitif général, du langage figuré et de la cognition sociale ». Thesis, Nice, 2016. http://www.theses.fr/2016NICE2004/document.
Texte intégralSchizophrenia Spectrum Disorders and Autism Spectrum Disorders (ASD) have similar difficulties in communication, social interaction, affects and emotions. These apparent similarities raise the question whether similar or different neurocognitive processes might underlie similar symptoms and cognitive profiles. However, currently, very few experimental studies directly compare individuals with autism and schizophrenia in different cognition areas.The major aim of the present Doctoral Dissertation was to address these issues by exploring three areas: cognitive profile (the assessment of general cognitive functioning and the quantitative and the qualitative analysis of verbal fluency), pragmatic language (idiom comprehension in context and novels metaphors’ comprehension) and social cognition (facial affect recognition and attributional style). In each of these areas, the major results showed that despite apparent cognitive similarities, neurocognitive functioning observed in patients with schizophrenic disorders and autism were characterized by significant qualitative differences that were examined and discussed in the context of the international literature and in relation to the possible clinical perspectives
Dor-Nedonsel, Emmanuelle. « Les schizophrénies précoces : épidémiologie, exploration clinique et neurocognitive, phénotypage de familles d'enfants avec schizophrénie et autisme ». Electronic Thesis or Diss., Université Côte d'Azur (ComUE), 2017. http://theses.univ-cotedazur.fr/2017AZUR4093.
Texte intégralEarly Onset Schizophrenia (EOS), a rare neurodevelopmental disorder (≈0.01%) is categorized into two types: Very Early Onset Schizophrenia, before age 13 and Adolescent Schizophrenia between ages 13 and 18. This diagnosis is a difficult one to make and considering the lack of knowledge on EOS, we can presume that it is in fact under-diagnosed and that our treatment and management options are still not very specific. We conducted a first epidemiological prevalence study consisted in evaluating: (1) the rate of subjects with EOS diagnostic criteria among 302 children who receive care in psychosocial and sanitary care facilities in the PACA region; (2) the clinical and neurocognitive characteristics of those children with EOS; (3) the rate of children with both EOS and ASD criteria within the same sample. In a second study, focusing on a subgroup of children with comorbid EOS and ASD, we analyzed first-degree relatives from a psychopathological, personality and cognitive viewpoint. The results are: a high rate of patients (8.9%) with an EOS diagnosis, a male gender majority (59.3%), an average age of 12.4 (SD=3.2), an average intelligence quotient of 72.5 (SD=21.4), a rate of 82.8% of subjects with hallucinations, 70% with EOS negative symptoms, 41.2% with comorbid autism, and 51.5% with antipsychotic medications. The study of family members shows that mothers have a higher rate of personality disorders, autistic traits and psychiatric disorders, as well as a lower average IQ. The creation and the characterization of a phenotype of this cohort have led to a family-genetic analysis based on exome sequencing in the parents and children with EOS following this study
Dor-Nedonsel, Emmanuelle. « Les schizophrénies précoces : épidémiologie, exploration clinique et neurocognitive, phénotypage de familles d'enfants avec schizophrénie et autisme ». Thesis, Université Côte d'Azur (ComUE), 2017. http://www.theses.fr/2017AZUR4093/document.
Texte intégralEarly Onset Schizophrenia (EOS), a rare neurodevelopmental disorder (≈0.01%) is categorized into two types: Very Early Onset Schizophrenia, before age 13 and Adolescent Schizophrenia between ages 13 and 18. This diagnosis is a difficult one to make and considering the lack of knowledge on EOS, we can presume that it is in fact under-diagnosed and that our treatment and management options are still not very specific. We conducted a first epidemiological prevalence study consisted in evaluating: (1) the rate of subjects with EOS diagnostic criteria among 302 children who receive care in psychosocial and sanitary care facilities in the PACA region; (2) the clinical and neurocognitive characteristics of those children with EOS; (3) the rate of children with both EOS and ASD criteria within the same sample. In a second study, focusing on a subgroup of children with comorbid EOS and ASD, we analyzed first-degree relatives from a psychopathological, personality and cognitive viewpoint. The results are: a high rate of patients (8.9%) with an EOS diagnosis, a male gender majority (59.3%), an average age of 12.4 (SD=3.2), an average intelligence quotient of 72.5 (SD=21.4), a rate of 82.8% of subjects with hallucinations, 70% with EOS negative symptoms, 41.2% with comorbid autism, and 51.5% with antipsychotic medications. The study of family members shows that mothers have a higher rate of personality disorders, autistic traits and psychiatric disorders, as well as a lower average IQ. The creation and the characterization of a phenotype of this cohort have led to a family-genetic analysis based on exome sequencing in the parents and children with EOS following this study
Remy, Irving. « Les fonctions visuelles rétiniennes et corticales dans les troubles du spectre de la schizophrénie et les situations à risque de psychose ». Electronic Thesis or Diss., Strasbourg, 2024. http://www.theses.fr/2024STRAJ030.
Texte intégralPsychotic disorders are characterized by severe functional consequences, with emerging evidence of impairment in low-level visual functions. Most notably, the anatomical and functional link between the retina and the visual cortex led to hypotheses concerning the association between alterations in both visual stages. We investigated retinal and cortical visual electrophysiological measurements in schizophrenia spectrum disorders and situations at risk of psychosis, of which regular cannabis use and early phases of psychosis are an integral part. The results highlighted alterations in most retinal cells and deficits in the primary visual cortex, with a potential link between both measures in schizophrenia. The relevance of electrophysiological biomarkers also lies in the link described with psychotic symptoms, motivating them to be used more widely in clinical practice to improve diagnosis
Martinez, Gilles. « Continuum autisme-schizophrénie : apport de l’étude de la cognition sociale et de marqueurs phénotypiques développementaux ». Thesis, Sorbonne Paris Cité, 2017. http://www.theses.fr/2017USPCB065/document.
Texte intégralAutism and schizophrenia are both neurodevelopmental psychiatric disorders. Research on early-onset schizophrenia, commonly associated to autism spectrum disorders (ASD), suggested a possible developmental continuum between both of these disorders. Clinical and epidemiological evidence, and research from molecular genetics or brain imaging, come to support this hypothesis. In this context, social cognition is a matter of special interest. Impairments are reported both in the two disorders, but with inconsistent results, revealing common features as well as differences. Otherwise, links between social cognition impairments and neurodevelopmental burden have been until now poorly explored. Through the contribution of our three studies, we confirmed the importance of social cognition impairment in autism and schizophrenia. The MASC test (Movie for the Assessment of Social Cognition), an original tool which was by our findings validated in a French version, revealed higher overall impairment of mentalizing capabilities in ASD than in schizophrenia. Animated Shapes (non verbal test of attribution of intentions) revealed qualitative differences: whereas hypomentalizing is common both to ASD and schizophrenia, overmentalizing seemed to be more important in schizophrenia. Furthermore, along a continuum between autism and schizophrenia, social cognition impairment was linked to thought and language disorganization, and to neurological soft signs (a marker for neurodevelopmental load). In addition, in subjects with schizophrenia, overmentalizing was correlated to the precocity of onset of the disease. Altogether, our results highlight the need to screen developmental feature in adulthood. In that way, we presented preliminary results in order to validate a developmental disorders screening self-rated questionnaire. As a conclusion, our results bring evidence in favour of a hypothesis of a continuum between autism and schizophrenia, showing a social cognition impairment in both disorders, correlated to the neurodevelopmental load existing in both of them in a transnosographic way. We contributed to emphasize the sub-group of subjects with schizophrenia with early-onset of disease, characterized by a tendency to overmentalizing and presenting a marked disorganization. Our work provides avenue to further studies, integrating neuroimaging and genetic data, that will help to advance in a deeper comprehension of the pathophysiology of autism and schizophrenia. Furthermore, we used and validated in this work promising tools to improve finely psychopathological evaluation and differential diagnosis in adults suffering from autism and from schizophrenia
Bussière, Sylvain. « Prédiction de l'employabilité à partir du potentiel d'apprentissage chez les personnes présentant un trouble du spectre de la schizophrénie ». Thèse, Université du Québec à Trois-Rivières, 2012. http://depot-e.uqtr.ca/6151/1/030404053.pdf.
Texte intégralFernandez, Arnaud. « Exploration du profil clinique et génétique des patients atteints de schizophrénie précoce et de leurs apparentés au 1er degré - un protocole d’étude familiale et multicentrique en population française : Protocole GenAuDiss ». Electronic Thesis or Diss., Université Côte d'Azur, 2021. http://theses.univ-cotedazur.fr/2021COAZ6010.
Texte intégralEarly-onset schizophrenia (EOS) is a rare, severe and neurodevelopmental form of schizophrenia beginning before the age of 18. In order to better understand the complex genetic basis of this disorder, we have developed a pilot project with the main objective of clinically and genetically characterize EOS patients presenting additional neurodevelopmental disabilities. Given the clinical and genetic overlap of EOS with other neurodevelopmental disorders, including Autism Spectrum Disorder (ASD) and Attention Deficit Hyperactivity Disorder (ADHD), we paid particular attention to the genes involved in neurodevelopment.This is a multi-center study carried out from April 2014 to May 2023 in a paediatric population. Inclusion criteria are: age 7-22 years, a diagnosis of EOS (K-SADS-PL DSM-5) with premorbid autistic symptoms (ADI-R 0-5 years) and IQ > 40; parents and siblings are included. Clinical profile explorations are performed using standardized tools (KSADS-PL and PANSS) and included neurocognitive assessments (WISC-V/WAIS-IV), the search for psychiatric co-morbidities, neurodevelopmental disorders and associated extracerebral somatic pathologies. The exploration of the genetic profile consists in identifying genetic mutations by a hierarchical approach searching for Fragile-X Syndrome (PCR), CGH-array and, in case of negativity of the previous examinations, DNA sequencing (exome) in trio (mother, father, child). Finally; we proceed to the prioritization of genes by combining multiple bioinformatics tools.20 subjects were included: 15 boys and 5 girls. The mean age of onset of the disorder was 8.90 years (+/-2.30). Psychiatric comorbidities (DSM-5) were ADHD (15/20 patients), anxiety disorders (14/20) and ASD (13/20). The mean IQ was 70.26 (+/-18.09). Language delay and school disruption were noticed in 18/20 patients. The main associated somatic condition was asthma (15/20 patients). Genetically, we report a 10q26.3 324 kb microduplication in one patient (with familial segregation), encompassing part of the INPP5A gene. We have shown that its homologue 5PtaseI is specifically expressed in the Drosophila central nervous system. Furthermore, we have identified, through DNA sequencing of 9 exomes of patients in trio (27 subjects with mother, father and child) and bioinformatics tools, the presence of variants in genes belonging to the Wnt, cadherin and cholecystokinin signaling pathways.In our EOS patients, we have shown a large clinical heterogeneity with psychiatric co-morbidities and neurodevelopmental disorders systematically associated. INPP5A is expressed in the brain (human, mouse and Drosophila), is highly conserved between species and encodes a InsP3 5-phosphatase whose hydrolysis products mobilize intracellular calcium, essential for the morphogenesis of dendritic spines in neurons. The alteration of this process, by the InsP3/Ca2+ signaling pathway, is found in both schizophrenia and ASD, strengthening the link between these disorders. In addition, we have made the first description of the potential involvement of the Wnt, Cadherin and Cholecystokinin signaling pathways in EOS. The already described involvement of these different pathways in other neurodevelopmental and/or psychiatric disorders underlines the genetic heterogeneity of this disorder. Therefore, elucidating the molecular mechanisms of EOS and paving the way for specific therapeutic interventions will require systematic and large-scale: 1) definition of the precise syndromic diagnosis of EOS with an exact age of onset and determination of the premorbid neurodevelopmental phenotype, psychiatric comorbidities and associated extracerebral somatic pathologies; 2) genetic evaluation using a hierarchical approach up to whole genome sequencing; 3) data sharing between teams on an international scale with the constitution of specific, comparable, genetic, and molecular databases correlated to the precise phenotypes of the different forms of EOS
Rothärmel, Maud. « La résistance pharmacologique dans les pathologies psychiatriques : Exemple de la dépression, la schizophrénie et l'autisme. Identification of potential genetic risk factors for bipolar disorder by whole-exome sequencing Les traitements pharmacologiques dans les troubles du spectre de l’autisme Troubles de l’humeur ? Quand recourir à la stimulation magnétique transcrânienne ? Repeated transcranial magnetic stimulation (rTMS) to improve electroconvulsive therapy (ECT) in TReatment-Resistant Depression : a report of two cases ». Thesis, Normandie, 2019. http://www.theses.fr/2019NORMR125.
Texte intégralDrug resistance is a common problem in medicine, that also concerns psychiatry. As there are resistant epilepsies, there are resistant depression or schizophrenia. Autism is in a slightly different situation as there is no reference treatment for neurodevelopmental disorders. These three disorders constitue major public health issues from both the economic and social perspective with important functional impact of the disease. After focusing on the definition of drug resistance in depression, schizophrenia and autism and on the hypothetical underlying pathophysiological processes, we investigated what could be common to these disorders. This allowed us to understand how to optimize their treatments. Several augmentation methods are possible, such as the potentiation of drugs between them or the potentiation of drugs by neurostimulation (electroconvulsive therapy, ECT, repetitive transcranial magnetic stimulation, rTMS, transcranial direct current stimulation, tDCS). In the second part of this work, we studied the effects of different ways to optimizing treatments : the use of clozapine on aggressive behaviors for patients with autism spectrum disorders (ASD) ; the use of tDCS on executive functions in patients with ASD ; the clozapine augmentation strategie by ECT in ultra-resistant schizophrenia and the ECT augmentation strategie by rTMS in treatment-resistant depression. Our encouraging results led us to focus on the mechanisms of these potentiation strategies, including ECT and on the development of new protocols to confirm our results
Faget-Agius, Catherine. « Etude des bases neurales structurales et fonctionnelles des troubles cognitifs et de la qualité de vie dans la schizophrénie par imagerie cérébrale multimodale ». Thesis, Aix-Marseille, 2015. http://www.theses.fr/2015AIXM5050/document.
Texte intégralWe conducted a multimodal neuroimaging approach combining the study of working memory activation with fMRI, the study of microstructural abnormalities associated with impaired QoL using MTI and the study of the functional brain substrate of QoL using SPECT. We aimed to characterize structural and functional neural basis of cognitive impairment and QoL in schizophrenia. We secondarily aimed to test the predictive value of cognitive impairment and QOL for the evolution and functioning in schizophrenia.First, we explored brain activation during a working memory task between patients with short disease duration and patients with long disease duration. We found a functional reorganization in patients with long schizophrenia duration having brain hyperactivations relative to short schizophrenia duration patients. Secondly, we investigated and compared microstructural abnormalities in patients with preserved Qol and impaired QoL. We showed that patients with impaired QoL had more microstructural changes in brain regions affected by the disease process of schizophrenia.Finally, we studied the neural substrate of QoL in schizophrenia. We reported that brain regions involved in cognitions, emotional information processing and social cognition underlie the different QoL dimensions in schizophrenia. On the one hand, our findings suggest that a functional reorganization in the working memory neural network plays a compensatory role in the schizophrenia course. On the other hand, our results suggest that QoL could be the early expression of brain abnormalities induced by the disease process of schizophrenia
Livres sur le sujet "Troubles du spectre de la Schizophrénie"
Gourion, David. Les troubles schizophréniques. Paris : Ellipses, 2004.
Trouver le texte intégralde, Clercq Michel, et Peuskens Joseph, dir. Les Troubles schizophréniques. Paris : De Boeck Université, 2000.
Trouver le texte intégralCullere-Crespin, Graciela. Traitements des troubles du spectre autistique : À la recherche d'un modèle français. Toulouse : Éditions Érès, 2013.
Trouver le texte intégralCullere-Crespin, Graciela. APPROCHES CLINIQUES ET PÉDAGOGIQUES DES TROUBLES DU SPECTRE AUTISTIQUE (TSA) - Cahiers de Préaut. Paris : Editions L'Harmattan, 2011.
Trouver le texte intégralAlberta. Direction de l'éducation française. Éléments essentiels du programme d'adaptation scolaire destiné aux élèves ayant des troubles du spectre autistique. Edmonton : Alberta Education, Direction de l'éducation française, 2006.
Trouver le texte intégralSilverberg, Renee. Understanding children & families with autism spectrum disorders. Houston, [Texas] : Strategic Book Publishing and Rights Co., 2014.
Trouver le texte intégralauteur, Hannah Susan 1956, et Sengmueller Elke 1972 auteur, dir. Les troubles du spectre de l'autisme : Guide de santé et d'alimentation : 175 recettes pour aider votre enfant à manger. Montréal (Québec) : Trécarré, 2015.
Trouver le texte intégralPeggy M. P. C. Bosch et Maurits W. M. L. van den Noort. Schizophrenia, sleep, and acupuncture. Cambridge, MA : Hogrefe, 2008.
Trouver le texte intégralErvas, Fulvio. N'aie pas peur si je t'enlace. Paris : L. Levi, 2013.
Trouver le texte intégralHarrop, Chris. Why does schizophrenia develop at late adolescence ? : A cognitive-developmental approach to psychosis. Hoboken, N.J : Wiley, 2003.
Trouver le texte intégralChapitres de livres sur le sujet "Troubles du spectre de la Schizophrénie"
Amado, Isabelle. « Chapitre 10. Cognition sociale et schizophrénie ». Dans Neuropsychologie et remédiations des troubles du spectre de l’autisme, 291–303. De Boeck Supérieur, 2018. http://dx.doi.org/10.3917/dbu.breti.2018.01.0291.
Texte intégralServant, Dominique. « Troubles de la personnalité dans le spectre de la schizophrénie ». Dans Les Troubles de la personnalité, 171–78. Elsevier, 2024. http://dx.doi.org/10.1016/b978-2-294-78349-4.00017-5.
Texte intégralBesche-Richard, Chrystel, Sarah Terrien, Romina Rinaldi, Frédéric Verhaegen, Laurent Lefebvre et Michel Musiol. « Chapitre 6. Les troubles du spectre de la schizophrénie ». Dans Psychopathologie cognitive, 153–79. Dunod, 2018. http://dx.doi.org/10.3917/dunod.besce.2018.01.0153.
Texte intégralLaurent-Levinson, Claudine. « Épisodes psychotiques aigus – Schizophrénies à début précoce – Troubles du spectre de la schizophrénie ». Dans Médecine et Santé de L'adolescent, 381–85. Elsevier, 2019. http://dx.doi.org/10.1016/b978-2-294-75919-2.00049-7.
Texte intégralSperanza, Mario, et Franck Hazane. « 18. Psychoses et troubles du spectre de la schizophrénie à l’adolescence ». Dans Troubles psychiques et comportementaux de l'adolescent, 183. Lavoisier, 2017. http://dx.doi.org/10.3917/lav.duver.2017.01.0183.
Texte intégralFranck, Nicolas. « Chapitre 13. Remédiation cognitive dans les troubles du spectre de la schizophrénie ». Dans Neuropsychologie en psychiatrie, 257–70. De Boeck Supérieur, 2019. http://dx.doi.org/10.3917/dbu.amiev.2019.01.0257.
Texte intégralFranck, Nicolas. « Chapitre 13. Remédiation cognitive dans les troubles du spectre de la schizophrénie ». Dans Neuropsychologie en psychiatrie, 257–70. De Boeck Supérieur, 2019. http://dx.doi.org/10.3917/dbu.amiev.2019.01.0257.
Texte intégralVioleau, Louis, et Antoinette Prouteau. « Chapitre 10. Troubles du spectre schizophrénique et fonctionnement cognitif ». Dans Neuropsychologie en psychiatrie, 207–16. De Boeck Supérieur, 2019. http://dx.doi.org/10.3917/dbu.amiev.2019.01.0207.
Texte intégralLaloyaux, Julien, et Frank Larøi. « Chapitre 12. Mécanismes cognitifs sous-tendant les symptômes positifs des Troubles du Spectre Schizophrénique ». Dans Neuropsychologie en psychiatrie, 231–56. De Boeck Supérieur, 2019. http://dx.doi.org/10.3917/dbu.amiev.2019.01.0231.
Texte intégralGut-Fayand, Anne. « La schizophrénie ». Dans Troubles mentaux et psychothérapies, 85. Editions Sciences Humaines, 2016. http://dx.doi.org/10.3917/sh.marmi.2016.01.0085.
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