Major Depressive Disorder Clinical Trial
Official title:
PET Imaging of mGluR5 With Drug Challenge
This study is designed to look at that involvement of a process in the brain called the
glutamate system in depression. Participants will undergo a screening session, up to two
fMRI scans, and up to three PET scans, as well as cognitive testing at each scan session.
For one of the PET scans, a drug (either ketamine or n-acetyl cysteine) will be
administered.
Hypothesis 1: The investigators hypothesize administration of ketamine or n-acetylcysteine
(NAC) will lead to a decrease in mGluR5.
Hypothesis 2: The investigators hypothesize an improvement in memory and attentional skills
after drug challenge.
Hypothesis 3: The investigators hypothesize an increase in mGluR5 availability and change in
MRI measures post drug challenge as compared to baseline, signifying synaptogenesis.
Hypothesis 4: We expect there should not be a significant difference in reduction in mGluR5
availability due to differences in ABP688 radiotracer infusion.
Aim 1: To determine the acute effect of medication-induced glutamate release on mGluR5
availability in human subjects. Hypothesis 1: We hypothesize administration of ketamine or
n-acetylcysteine (NAC) will lead to a decrease in mGluR5 availability.
Aim 2: To determine if glutamate release via administration of ketamine or NAC has pro
cognitive benefits.
Hypothesis 2: We hypothesize an improvement in memory and attentional skills after drug
challenge.
Aim 3: To determine if there is synaptogenesis detectable by PET and MRI post ketamine or
NAC within a week of drug challenge (at the time of greatest antidepressant response).
Hypothesis 3: We hypothesize an increase in mGluR5 availability and change in MRI measures,
post drug challenge as compared to baseline, signifying synaptogenesis.
Aim 4: To determine if there is a difference in reduction of mGluR5 availability after
ketamine administration when radiotracer is administered bolus as compared to bolus to
constant infusion in the same subjects (ABP688 radiotracer only).
Hypothesis 4: We expect there should not be a significant difference in reduction in mGluR5
availability due to differences in ABP688 radiotracer infusion.
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Intervention Model: Single Group Assignment, Masking: Open Label
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