- ICH GCP
- US Clinical Trials Registry
- Clinical Trial NCT05650788
Exploration of Differences in Metabolite Concentrations by NMR Spectroscopy in the Ventral Striatum, Anterior Cingulate Cortex and Prefrontal Cortex in Euthymic Patients With Unipolar and Bipolar Type II Mood Disorders, as Well as in Healthy Subjects (RMN-UNIBI)
Study Overview
Status
Conditions
Intervention / Treatment
Detailed Description
Depression meets the same clinical diagnostic criteria whether it is the expression of a bipolar or unipolar mood disorder. It is essential to distinguish between these two disorders because the pharmacological management of this episode and the follow-up of the patient will be different. The risk of iatrogenesis is significant if the diagnosis is incorrect. Currently, there is no biomarker that can help the clinician in his diagnostic approach and to differentiate between bipolar and unipolar mood disorder (Grande et al., 2016; Vieta et al., 2018).
Many research, particularly in neuroimaging, explore these mood disorders to identify morphological, functional and metabolic signatures both in the state phase and in the asymptomatic phase.
Functional imaging work, carried out at the Cardiff University Brain Research Imaging Center in Wales in collaboration with the team 7280 from Clermont Auvergne University, is part of this research. The object of this work was to study the dopaminergic system, and in particular the meso-cortico-limbic pathway, which is the anatomical and functional substrate of the reward circuit. The activity of this system, when measured on functional MRI in the ventral striatum during an activation paradigm of the "anticipation of a reward during a monetary task" type, shows variations in the disorders of mood, in the state phase as well as in the asymptomatic phase. These activation differences are significantly different between healthy, unipolar and bipolar asymptomatic subjects.
The cerebral neurochemical processes involved in the physiopathology of mood disorders being still little studied at the present time and in order to complete these observations, the measurement and comparison of the concentrations of metabolites by NMR spectroscopy in these same regions (the meso -cortico-limbic) and under these same conditions will make it possible to specify the physiopathology of mood disorders. NMR spectroscopy, unlike functional MRI, allows us not only to compare groups, but also to measure concentrations in absolute values. Data from the literature show that these explorations are feasible in humans and meta-analyses suggest that a direct comparison could make it possible to discriminate mood disorders by the clinical dimension "capacity to experience pleasure" - or "hedonic capacity".
We hypothesize that there is a significant difference between the mean glutamate concentrations in the ventral striatum (right and left) of the two groups of unipolar and bipolar type II patients. The average glutamate concentration would be higher for participants in the group of type II bipolar patients.
This exploratory study will allow a better understanding of the pathophysiological mechanisms involved in the development of mood disorders and in particular in their clinical dimension "hedonic capacity", as well as to test the relevance of this potential biomarker (glutamate) than the current state of Art allows us to consider. The measurements in the control group will allow us to approach the values of the physiological norm. The measurements in the clinical groups will allow us to understand whether the "mood disorder" condition, even in remission, constitutes a sufficient factor of variation in this standard to allow them to be detected. This work would represent a first fundamental step in the understanding of pathophysiological mechanisms and the establishment of this measure as a biomarker for screening mood disorders and for discriminating between a unipolar disorder and a bipolar disorder and could thus guide the clinician in his diagnostic and therapeutic approach.
The constraints for the participants will be minimal with only two visits to the CHU. A first for the inclusion of a duration of 60 minutes. A second for the 120-minute measurement visit. The inclusion of patients will be done if possible during their regular follow-up to limit travel. Since MRI is a non-invasive technique used routinely in hospital practice, the risks incurred by patients are almost nil, subject to compliance with the contraindications of MRI
Study Type
Enrollment (Estimated)
Phase
- Not Applicable
Contacts and Locations
Study Contact
- Name: Lise Laclautre
- Phone Number: 334.73.754.963
- Email: promo_interne_drci@chu-clermontferrand.fr
Study Locations
-
-
-
Clermont-Ferrand, France
- Recruiting
- Chu Clermont-Ferrand
-
Principal Investigator:
- Etienne Allauze
-
Contact:
- Lise Laclautre
-
-
Participation Criteria
Eligibility Criteria
Ages Eligible for Study
Accepts Healthy Volunteers
Description
BIPOLAR DISORDERS GROUP :
Inclusion criteria :
- Patients with a diagnosis of bipolar type II disorder stabilized in remission, according to DSM 5 criteria, with mood stabilizer treatment (lithium, anticonvulsant or antipsychotic) at an effective dose, with possible antidepressant treatment (SSRI, SNRI, tricyclics )
- Right handed
- Aged 18 to 40
- Having completed the MRI compatibility questionnaire and having no contraindication to MRI
- Having given their written, free and informed consent
- Affiliated to a social security scheme
- Effective contraception for participants of childbearing age
- ECOG performance index < 2
Exclusion criteria :
- Age < 18 or > 40
- BMI > 30kg/m2
- Current episode. (MADRS score > 15 or YMRS score > 12, Montgomery, 1979, Young et al, 1978)
- Unbalanced psychiatric pathology.
- Neurological pathology (e.g. parkinsonian syndrome, stroke, migraine, fibromyalgia, etc.)
- Psychiatric pathology other than bipolar mood disorder (e.g. schizophrenia, severe anxiety disorder, severe personality disorder, instinctual behavior disorder, autism spectrum disorder, disorder related to the use of psychoactive substances excluding tobacco.)
- Under current psychotropic treatment other than antidepressants (SSRI, SNRI, tricyclics) or mood stabilizer (lithium, anticonvulsant or antipsychotic) at an effective dose. Treatment with benzodiazepine possible if possibility of deferring this line of treatment when carrying out the NMR acquisition.
- Alcohol consumption >3 units of alcohol/day (30g/day) for men and >2 units of alcohol/day (20g/day) for women.
- Unbalanced progressive condition (hepatic failure, renal failure with creatinine clearance <30mL/min, respiratory failure, congestive heart failure, myocardial infarction during the last 6 months, etc.)
- Any active cancer
- Holders of a pacemaker, cochlear implants, metallic implants or any magnetic element
- Claustrophobia
- Pregnant and breastfeeding women
- Legal incapacity (person deprived of liberty or under guardianship)
- Who, for psychological, social, family or geographical reasons, cannot be followed and/or compliant with the requirements of the study
- Already included in another clinical trial
MOOD DEPRESSIVE DISORDERS GROUP :
Inclusion criteria :
- Patients with a diagnosis of unipolar mood disorder stabilized in remission, according to DSM 5 criteria, with or without antidepressant treatment (SSRI, SNRI, tricyclics)
- Right handed
- Aged 18 to 40
- Having completed the MRI compatibility questionnaire and having no contraindication to MRI
- Having given their written, free and informed consent
- Affiliated to a social security scheme
- Effective contraception for participants of childbearing age
- ECOG performance index < 2
Exclusion criteria :
- Age < 18 or > 40
- BMI > 30kg/m2
- Current episode. (MADRS score > 15 or YMRS score > 12, Montgomery, 1979, Young et al, 1978)
- Unbalanced psychiatric pathology.
- Neurological pathology (e.g. parkinsonian syndrome, stroke, migraine, fibromyalgia, etc.)
- Psychiatric pathology other than mood depressive disorder (e.g. schizophrenia, severe anxiety disorder, severe personality disorder, instinctual behavior disorder, autism spectrum disorder, disorder related to the use of psychoactive substances excluding tobacco.)
- Under current psychotropic treatment other than antidepressants (SSRI, SNRI, tricyclics) or mood stabilizer (lithium, anticonvulsant or antipsychotic) at an effective dose. Treatment with benzodiazepine possible if possibility of deferring this line of treatment when carrying out the NMR acquisition.
- Alcohol consumption >3 units of alcohol/day (30g/day) for men and >2 units of alcohol/day (20g/day) for women.
- Unbalanced progressive condition (hepatic failure, renal failure with creatinine clearance <30mL/min, respiratory failure, congestive heart failure, myocardial infarction during the last 6 months, etc.)
- Any active cancer
- Holders of a pacemaker, cochlear implants, metallic implants or any magnetic element
- Claustrophobia
- Pregnant and breastfeeding women
- Legal incapacity (person deprived of liberty or under guardianship)
- Who, for psychological, social, family or geographical reasons, cannot be followed and/or compliant with the requirements of the study
- Already included in another clinical trial
HEALTHY GROUP :
Inclusion criteria :
- People for whom no psychiatric diagnosis can be retained, according to DSM 5 criteria, naïve to psychotropic treatments
- Right handed
- Aged 18 to 40
- Having completed the MRI compatibility questionnaire and having no contraindication to MRI
- Having given their written, free and informed consent
- Affiliated to a social security scheme
- Effective contraception for participants of childbearing age
- ECOG performance index < 2
Exclusion criteria :
- Age < 18 or > 40
- BMI > 30kg/m2
- Current episode. (MADRS score > 15 or YMRS score > 12, Montgomery, 1979, Young et al, 1978)
- Unbalanced psychiatric pathology.
- Neurological pathology (e.g. parkinsonian syndrome, stroke, migraine, fibromyalgia, etc.)
- Psychiatric pathology (e.g. bipolar disorder, mood depressive disorder, schizophrenia, severe anxiety disorder, severe personality disorder, instinctual behavior disorder, autism spectrum disorder, disorder related to the use of psychoactive substances excluding tobacco.)
- Under current psychotropic treatment other than antidepressants (SSRI, SNRI, tricyclics) or mood stabilizer (lithium, anticonvulsant or antipsychotic) at an effective dose. Treatment with benzodiazepine possible if possibility of deferring this line of treatment when carrying out the NMR acquisition.
- Alcohol consumption >3 units of alcohol/day (30g/day) for men and >2 units of alcohol/day (20g/day) for women.
- Unbalanced progressive condition (hepatic failure, renal failure with creatinine clearance <30mL/min, respiratory failure, congestive heart failure, myocardial infarction during the last 6 months, etc.)
- Any active cancer
- Holders of a pacemaker, cochlear implants, metallic implants or any magnetic element
- Claustrophobia
- Pregnant and breastfeeding women
- Legal incapacity (person deprived of liberty or under guardianship)
- Who, for psychological, social, family or geographical reasons, cannot be followed and/or compliant with the requirements of the study
- Already included in another clinical trial
Study Plan
How is the study designed?
Design Details
- Primary Purpose: Diagnostic
- Allocation: Non-Randomized
- Interventional Model: Parallel Assignment
- Masking: None (Open Label)
Arms and Interventions
Participant Group / Arm |
Intervention / Treatment |
---|---|
Experimental: Bipolar disorder group
Patients with a diagnosis of bipolar II mood disorder stabilized in remission, according to DSM 5 criteria, with mood stabilizer treatment (lithium, anticonvulsant or antipsychotic) at an effective dose, with possible antidepressant treatment (SSRI, SNRI, tricyclics )
|
The MRI protocol will be carried out at 3 Tesla (3T) on a Siemens NMR imaging system (Magnetom Vida, Siemens Healthcare, Erlangen, Germany), the emission of radiofrequency waves and the reception of the signal will be done using a resonator in quadrature head (64-channel phase-array antenna). The MRI protocol will take place in two phases:
|
Experimental: Mood depressive disorder group
Patients with a diagnosis of unipolar mood disorder stabilized in remission, according to DSM 5 criteria, with or without antidepressant treatment (SSRI, SNRI, tricyclics)
|
The MRI protocol will be carried out at 3 Tesla (3T) on a Siemens NMR imaging system (Magnetom Vida, Siemens Healthcare, Erlangen, Germany), the emission of radiofrequency waves and the reception of the signal will be done using a resonator in quadrature head (64-channel phase-array antenna). The MRI protocol will take place in two phases:
|
Experimental: Healthy volunteer
People for whom no psychiatric diagnosis can be retained, according to DSM 5 criteria and naïve to psychotropic treatments
|
The MRI protocol will be carried out at 3 Tesla (3T) on a Siemens NMR imaging system (Magnetom Vida, Siemens Healthcare, Erlangen, Germany), the emission of radiofrequency waves and the reception of the signal will be done using a resonator in quadrature head (64-channel phase-array antenna). The MRI protocol will take place in two phases:
|
What is the study measuring?
Primary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Glutamate concentration in ventral striatum
Time Frame: Within 3 months after inclusion
|
The main objective of the study is to compare the mean concentrations of glutamate in the ventral striatum (right and left), between two groups of treated, asymptomatic patients: unipolar vs bipolar type II disorder.
Patients will also be compared to a sample of healthy controls.
|
Within 3 months after inclusion
|
Secondary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Metabolites concentration in interest structures
Time Frame: Within 3 months after inclusion
|
Comparison of mean concentrations of metabolites (Choline, myo-inositol, N-acetylaspartate, creatine, glutamate/glutamine, lactate, taurine, GABA) in the Ventral Striatum (VS), Anterior Cingulate Cortex (ACC) and Prefrontal Cortex (PFC) ) between the three groups
|
Within 3 months after inclusion
|
Metabolites relationships with Seniority, severity of the disorder
Time Frame: Within 3 months after inclusion
|
Study of the relationships between the concentrations of metabolites with Seniority, severity of the disorder measured by MADRS questionnaire
|
Within 3 months after inclusion
|
Metabolites relationships with Predominant polarity
Time Frame: Within 3 months after inclusion
|
Study of the relationships between the concentrations of metabolites with Predominant polarity by YMRS questionnaire
|
Within 3 months after inclusion
|
Metabolites relationships with Dimension Anhedonia
Time Frame: Within 3 months after inclusion
|
Study of the relationships between the concentrations of metabolites with Dimension Anhedonia by SHAP questionnaire
|
Within 3 months after inclusion
|
Metabolites relationships with Operation
Time Frame: Within 3 months after inclusion
|
Study of the relationships between the concentrations of metabolites with Operation by FAST questionnaire
|
Within 3 months after inclusion
|
Metabolites relationships with Quality of life by MARS questionnaire
Time Frame: Within 3 months after inclusion
|
Study of the relationships between the concentrations of metabolites with Quality of life
|
Within 3 months after inclusion
|
Metabolites relationships with Compliance with treatment
Time Frame: Within 3 months after inclusion
|
Study of the relationships between the concentrations of metabolites with Compliance with treatment by WHOQOL-BREF questionnaire
|
Within 3 months after inclusion
|
Metabolites relationships with description ofPharmacological class of the antidepressant
Time Frame: Within 3 months after inclusion
|
Study of the relationships between the concentrations of metabolites with Pharmacological class of the antidepressant by
|
Within 3 months after inclusion
|
Metabolites relationships with description of Pharmacological class of mood stabilizer.
Time Frame: Within 3 months after inclusion
|
Study of the relationships between the concentrations of metabolites with description of Pharmacological class of mood stabilizer.
|
Within 3 months after inclusion
|
Collaborators and Investigators
Investigators
- Principal Investigator: Etienne ALLAUZE, University Hospital, Clermont-Ferrand
Study record dates
Study Major Dates
Study Start (Actual)
Primary Completion (Estimated)
Study Completion (Estimated)
Study Registration Dates
First Submitted
First Submitted That Met QC Criteria
First Posted (Actual)
Study Record Updates
Last Update Posted (Actual)
Last Update Submitted That Met QC Criteria
Last Verified
More Information
Terms related to this study
Additional Relevant MeSH Terms
Other Study ID Numbers
- AOI 2019 ALLAUZE
- 2019-A02607-50 (Other Identifier: 2019-A02607-50)
Drug and device information, study documents
Studies a U.S. FDA-regulated drug product
Studies a U.S. FDA-regulated device product
This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.
Clinical Trials on Bipolar Disorder Type II
-
Örebro County CouncilSchool of Law, Psychology and Social Work, Örebro UniversityCompletedBipolar Disorder, Type IISweden
-
ProgenaBiomeRecruitingBipolar Disorder | Bipolar I Disorder | Bipolar II Disorder | Bipolar Type I Disorder | Bipolar Disorder Mild | Bipolar Disorder Moderate | Bipolar Disorder SevereUnited States
-
University of ChicagoCompleted
-
Douglas Mental Health University InstituteNational Alliance for Research on Schizophrenia and DepressionActive, not recruitingDepression, Bipolar | Bipolar Type II DisorderCanada
-
Medical University of South CarolinaMilken InstituteCompletedBipolar Disorder | Bipolar I Disorder | Bipolar II DisorderUnited States
-
University of PittsburghNational Alliance for Research on Schizophrenia and DepressionCompletedBipolar I Disorder | Bipolar II Disorder | Bipolar Disorder NOSUnited States
-
Joshua RosenblatRecruitingBipolar Disorder | Bipolar Depression | Bipolar I Disorder | Bipolar II DisorderCanada
-
National Cheng-Kung University HospitalUnknownBipolar Disorder IITaiwan
-
University Hospital, GrenobleActive, not recruitingBipolar Disorder | Bipolar I Disorder | Bipolar II DisorderFrance
-
Ege UniversityActive, not recruitingBipolar Disorder | Bipolar I Disorder | Bipolar II DisorderTurkey
Clinical Trials on NMR spectrometry
-
Taipei Medical University WanFang HospitalCompletedPhonocardiographyTaiwan
-
University of OklahomaNational Cancer Institute (NCI)Completed
-
University of MinnesotaCompletedLung CancerUnited States
-
University Hospital Bispebjerg and FrederiksbergProff Dr Jürgen Popp, Leibniz Institute, IPHT, Jena, Germany; Karin Mogensen... and other collaboratorsRecruitingEndoscopic Bladder Cancer Diagnosis With RamanDenmark
-
Assistance Publique - Hôpitaux de ParisInstitut Curie; Sainte Anne hospitalCompleted
-
Assistance Publique - Hôpitaux de ParisCompletedJuvenile Idiopathic Arthritis | Arthritis, Septic | Arthritis, UnspecifiedFrance
-
Cliniques universitaires Saint-Luc- Université...RecruitingRare Diseases | Inborn Errors of MetabolismBelgium
-
Hopital FochRecruiting
-
University Hospital, MontpellierNot yet recruitingNarcolepsy | Cataplexy | Idiopathic Hypersomnia
-
Hopital FochRecruitingTransplant; Complication, RejectionFrance