Oxytocin Clinical Trial
Official title:
Disentangling Effects of Oxytocin on Cognitive and Reactive Fear and the Moderating Role of the Receptor for Advanced Glycation End-products
The study examines the (sub)regional specificity of anxiolytic oxytocin (OXT) effects on emotional face processing and reactive and cognitive fear. Preliminary data indicate that the Receptor for Advanced Glycation End Products (RAGE) may regulate oxytocin transport into the brain. Thus, the study aims to replicate previous observations of oxytocin effects on the processing of fearful faces in the centro-medial amygdala and to assess whether a RAGE polymorphism (-374 T/A: rs1800624; TT vs. TA/AA), that has been shown to alter transcriptional activity, modulates anxiolytic OXT effects.
So far, no study examined selective oxytocin (OXT) effects on reactive (midbrain
periaqueductal gray (PAG), central amygdala (CeA), hypothalamus, and the midcingulate cortex
(MCC)) and cognitive fear (ventromedial prefrontal cortex (vmPFC), posterior cingulate cortex
(PCC), hippocampus, and basolateral amygdala) and the reward system (striatum) with high
spatial resolution. Previous studies showed that 7T functional magnetic resonance imaging
(fMRI) results in a higher spatial resolution and specificity than 3T MRI in these brain
regions and would thus allow for a more detailed characterization of the neural effects.
To disentangle (sub)region-specific effects of OXT on task-related activations of the
cingulate structures, the amygdala, the striatum, PAG and VMPFC, the investigators plan to
acquire ultra-high field 7T fMRI data from healthy male participants while they perform (i)
an emotional face matching task and (ii) a flight initiation distance (FID) task involving
fast- or slow-attacking virtual predators that elicit distinct activations in the reactive
and cognitive fear circuits. Furthermore, participants will be pre-stratified depending on
RAGE polymorphisms to elucidate possible RAGE-related differential OXT effects.
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