Schizophrenia Clinical Trial
— MADOCSOfficial title:
"MADOCS: Manual Dexterity and Oculomotor Control as Vulnerability Markers in Schizophrenia"
The investigators recently showed that visuomotor integration was significantly altered in schizophrenic patients during: (i) a grip force task (Teremetz et al., 2014), and (ii) a saccadic paradigm (oculomotor task)(Amado et al., 2008). Given this findings, the investigators propose a combined study of oculomotor and grip force control to better characterize the sensorimotor integration deficit. This approach may allow for identification of behavioural biomarkers of vulnerability to develop schizophrenia.
Status | Recruiting |
Enrollment | 105 |
Est. completion date | January 2019 |
Est. primary completion date | September 2018 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 18 Years to 50 Years |
Eligibility |
Inclusion Criteria: - All groups: 1. 18>yrs<50 2. Medical visit completed 3. Visual acuity (9/10 for each eye or corrected) 4. Provided written informed consent - Group of patient suffering from schizophrenia: 4. DSM-IV-TR diagnostic criteria for schizophrenia 5. Treatment: stable atypical anti-psychotic medication for >3 months prior to the study - Group of UHR patient: 6. 18>yrs<30 7. Fulfill at risk criteria of CAARMS diagnostic tool Exclusion Criteria: • All groups: 1. IQ<70, 2. Contraindications for TMS protocol: no previous history of neurosurgery or seizures or 1st degree relative with history of seizures, heart disease, drug abuse or addiction in the last 12 months, medications that lower seizure threshold including clozapine, bupropion, méthadone or theophylline. 3. Metallic implant in head (except dental fillings) 4. Pacemaker, or other electronic implanted devices 5. Central neurological disease: parkinsonism, x 6. Severe heart attack 7. Instable clinical state (e.g. stroke) 8. Previous history of drug abuse lasting more than 5 years or during the last year 9. Life event with a moderate to severe impact 10. Caffeine intake in the last two hours preceding visuomotor assessment • Groups of Siblings and Healthy controls: 11. No previous history of psychiatric disease, psychotic spectrum disorder (according to DIGS 3.0) 12. No previous history of antipsychotic medication (entire life) • Groups of UHR patient: 13. Chlorpromazine dose >100mg over more than 12 weeks 14. No previous history of autism spectrum disorder, bipolar disorder or diagnozed schizophrenia (according to DSM-IV-TR criteria), isolated anxiety disorders (e.g. social phobia, agoraphobia) |
Country | Name | City | State |
---|---|---|---|
France | Centre de Recherche Clinique (CRC) - CHSA | Paris | |
France | Service Hospitalo-Universitaire (SHU) - CHSA | Paris |
Lead Sponsor | Collaborator |
---|---|
Centre Hospitalier St Anne | Institut National de la Santé Et de la Recherche Médicale, France, University of Paris 5 - Rene Descartes |
France,
Amado I, Landgraf S, Bourdel MC, Leonardi S, Krebs MO. Predictive saccades are impaired in biological nonpsychotic siblings of schizophrenia patients. J Psychiatry Neurosci. 2008 Jan;33(1):17-22. — View Citation
Teremetz M, Amado I, Bendjemaa N, Krebs MO, Lindberg PG, Maier MA. Deficient grip force control in schizophrenia: behavioral and modeling evidence for altered motor inhibition and motor noise. PLoS One. 2014 Nov 4;9(11):e111853. doi: 10.1371/journal.pone.0111853. eCollection 2014. — View Citation
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Behavioural assessment | Index reflecting motor performance during visuomotor task (including force and oculomotor control) | BASELINE | |
Secondary | Clinical scale : PANSS | Positive and Negative Syndrome Scale: Assess positive and negative symptoms | BASELINE | |
Secondary | Clinical scale : DIGS III | Diagnostic Interview for Genetic Studies 3.0: Overview of clinical state | BASELINE | |
Secondary | Clinical scale : BPRS | Brief Psychiatric Rating Scale: Assess schizophrenic symptoms | BASELINE | |
Secondary | Clinical scale : SAS | Simpson Angus Extra-Pyramidal Scale: Asses extra-pyramidal signs | BASELINE | |
Secondary | Clinical scale : AIMS | Abnormal Involuntary Movements Scale: Assess abnormal involuntary movements | BASELINE | |
Secondary | Clinical scale : TAP | Test battery for Attentional Performance: Assess attentional capacity (e.g. working memory) | BASELINE | |
Secondary | Clinical scale : Stroop | Stroop color naming test: Assess selective attention or inhibition. | BASELINE | |
Secondary | Clinical scale : WASI | Wechsler Abbreviated Scale of Intelligence: Assess intelligence quotient | BASELINE | |
Secondary | Tracking performance (motor task): RMS Error | RMS Error (Root Mean Square) | BASELINE | |
Secondary | Tracking performance (motor task): Coefficient of variability | Coefficient of variability | BASELINE | |
Secondary | Tracking performance (motor task): Timing | Timing/inhibition | BASELINE | |
Secondary | Ocolomotor performance (eye tracker) : Saccade | Saccade error (back up/ catch up saccades) during smooth pursuit and fixation | BASELINE | |
Secondary | Ocolomotor performance (eye tracker): Gain | Gain (target velocity/gaze velocity), Reaction time | BASELINE | |
Secondary | Ocolomotor performance (eye tracker): Amplitude of eye movements | Amplitude (°) and velocity (°/s) of saccadic movements | BASELINE | |
Secondary | Motor noise | Variability of EMG response during visuomotor task | BASELINE | |
Secondary | Cortical excitability (MEP; TMS) | Motor evoked potential (MEP) during visuomotor task (single pulse TMS) | BASELINE | |
Secondary | Cortical inhibition (SICI; TMS) | Cortical inhibition measured during visuomotor task (paired-pulse TMS; MEP) | BASELINE |
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