ClinicalTrials.gov processed this data on March 28, 2024Link to the current ClinicalTrials.gov record.https://clinicaltrials.gov/ct2/show/NCT0002585702000702-M-0007NCT00025857Brain Function in Mentally Ill AdolescentsAdolescent Medial Temporal Lobe Function in Health and IllnessNational Institute of Mental Health (NIMH)NIH
The purpose of this study is to use brain imaging technology to examine the brain activity of
adolescents with post-traumatic stress disorder (PTSD) and/or major depressive disorder (MDD)
before and after treatment.
Adults with PTSD or MDD exhibit abnormalities in the structure and function of certain parts
of the brain. Although PTSD and MDD are psychiatric disorders that often emerge in childhood,
the relationship between these disorders and brain structures has not been thoroughly studied
in adolescents with the disorders. This study will use functional magnetic resonance imaging
(fMRI) to study the parts of the brain that are involved in PTSD and MDD in adolescents.
Adolescents with PTSD and/or MDD will be enrolled along with healthy adolescents with or
without a history of abuse. Healthy adults will also be enrolled. Participants will be
screened with a physical examination; blood tests; and interviews about mood, general degree
of nervousness, and behavior. Adolescents and their parents will be interviewed separately
and together. Following the interviews, participants will undergo psychological tests.
Participants with PTSD and/or MDD will have two weekly sessions of talk therapy. Participants
who continue to experience PTSD or MDD symptoms after the talk therapy may continue the talk
therapy alone, begin treatment with fluoxetine (Prozac ) alone, or begin fluoxetine in
addition to the talk therapy. Participants who take fluoxetine will have blood collected
before treatment and 8 weeks after treatment has begun. If participants do not respond to the
treatment, the treatment will be stopped and the participants will be offered another
treatment. Participants who respond to treatment will continue treatment at NIH until a
referral to an outside physician is made. Depending on the experiment in which they are
enrolled, participants will undergo one or four MRI scans. Participants who will have four
MRI scans will undergo the scans on separate days. During the MRI, participants will complete
tasks on a computer. Saliva samples will be collected before and after the scans.
Participants with PTSD and/or MDD will collect their saliva one or two days before the MRI
scan.
Adults with post-traumatic stress disorder (PTSD) or major depressive disorder (MDD) exhibit
abnormalities in the structure and function of the amygdala and hippocampus (temporal lobe),
as well as in the prefrontal cortex (PFC) and striatum (four brain structures underlying the
emotional processing and reward systems). However, while these psychiatric disorders often
emerge in childhood, the integrity of these neural structures has been minimally studied in
psychiatrically impaired children and adolescents. In the current proposal, functional MRI
(fMRI) will be used to evaluate the amygdala, hippocampus, PFC and striatum in (1)
psychiatrically healthy adolescents; (2) adolescents with trauma history and PTSD or anxiety
symptoms; (3) adolescents with trauma history, symptoms of depression and either PTSD or
anxiety symptoms; and (4) adolescents with only major depressive or PTSD/anxiety symptoms;
(5) adolescents with trauma and no trauma related symptoms. The proposed study is conducted
in three separate experiments.
At this stage of the protocol, we completed experiment 1, and a pilot study to help guide
experiments 2 and 3. In Experiment 1, we determined whether a fear conditioning paradigm
elicited amygdala activity in healthy adolescents. The pilot study examined test-retest
reliability of the fMRI signal in healthy adolescents and adults.
In Experiment 2, we will examine the functioning of the amygdala, hippocampus, PFC and
striatum in healthy adolescents and those with the psychiatric conditions described above.
During image acquisition, four cognitive tasks, targeting these regions, will be used: 1) a
social interaction task, 2) an inhibition task (the Stop task or the antisaccade task), 3) an
emotional rating/explicit memory task and 4) a probe detection task. One hundred twenty five
participants (25 in five groups) will be recruited in experiment 2.
Experiment 3 will address the same question as in experiment 2 in relation to treatment
response. In other words, in contrast to experiment 2, patients will be studied prior and
after treatment of the psychopathology associated with their traumatic experience. The sample
will include 125 patients (25 in each of the 4 groups) and 25 controls.
CompletedOctober 22, 2001June 29, 2012ObservationalNo105HealthyPosttraumatic Stress DisorderMajor Depressive Disorder
- INCLUSION CRITERIA:
All subjects 7-18 (adolescents).
Consent: can give consent/assent.
IQ: all subjects will have IQ greater than 70.
Subjects currently on antidepressants or benzodiazepines medication.
Subjects suffering from ADHD and currently on stimulants.
SUBJECTS WITH MAJOR DEPRESSION:
Diagnosis: Current diagnosis of MDD.
Clinical Impairment: CGAS less than 60.
SUBJECTS WITH PTSD:
Diagnosis: current diagnosis of PTSD.
Clinical Impairment: CGAS of less than 60.
SUBJECTS WITH HISTORY OF TRAUMA:
Trauma (i.e., sexual or physical abuse, exposure to an accident, etc.) will be defined
according to the KSADS, the Child Trauma Questionnaire, the Life Events Survey and the
history of adoption.
EXCLUSION CRITERIA:
Any medical condition that increases risk for MRI (e.g. pacemaker, metallic foreign
material in eye).
Any medical condition that increases risk for fluoxetine treatment for patients with
MDD/PTSD.
Pregnancy.
Participants suffering from acute psychosis or suicidal ideation; current abuse/dependency
to alcohol or drugs.
Currently in an abusive situation at home.
Weight that is 15% more or less than ideal body weight for sex and height.
Current tobacco use.
All7 Years18 YearsNoMonique Ernst, M.D.Principal InvestigatorNational Institute of Mental Health (NIMH)National Institutes of Health Clinical Center, 9000 Rockville PikeBethesdaMaryland20892United StatesUnited StatesBernstein DP, Fink L, Handelsman L, Foote J, Lovejoy M, Wenzel K, Sapareto E, Ruggiero J. Initial reliability and validity of a new retrospective measure of child abuse and neglect. Am J Psychiatry. 1994 Aug;151(8):1132-6. doi: 10.1176/ajp.151.8.1132.8037246Birmaher B, Dahl RE, Ryan ND, Rabinovich H, Ambrosini P, al-Shabbout M, Novacenko H, Nelson B, Puig-Antich J. The dexamethasone suppression test in adolescent outpatients with major depressive disorder. Am J Psychiatry. 1992 Aug;149(8):1040-5. doi: 10.1176/ajp.149.8.1040.1636803Blair RJ, Morris JS, Frith CD, Perrett DI, Dolan RJ. Dissociable neural responses to facial expressions of sadness and anger. Brain. 1999 May;122 ( Pt 5):883-93. doi: 10.1093/brain/122.5.883.10355673June 29, 2012October 26, 2001October 26, 2001October 28, 2001November 30, 2019November 30, 2019December 3, 2019fMRIDepressionPTSDEmotionMagnetic Resonance ImagingAnxietyNormal VolunteersAdolescenceMemoryPhysical/Sexual Abuse HistoryPost-Traumatic Stress DisorderAdolescentHealthy VolunteerHVNormal ControlDepressive DisorderDepressive Disorder, MajorStress Disorders, TraumaticStress Disorders, Post-Traumatic