| Literature DB >> 16339042 |
Peter Kirsch1, Christine Esslinger, Qiang Chen, Daniela Mier, Stefanie Lis, Sarina Siddhanti, Harald Gruppe, Venkata S Mattay, Bernd Gallhofer, Andreas Meyer-Lindenberg.
Abstract
In non-human mammals, the neuropeptide oxytocin is a key mediator of complex emotional and social behaviors, including attachment, social recognition, and aggression. Oxytocin reduces anxiety and impacts on fear conditioning and extinction. Recently, oxytocin administration in humans was shown to increase trust, suggesting involvement of the amygdala, a central component of the neurocircuitry of fear and social cognition that has been linked to trust and highly expresses oxytocin receptors in many mammals. However, no human data on the effects of this peptide on brain function were available. Here, we show that human amygdala function is strongly modulated by oxytocin. We used functional magnetic resonance imaging to image amygdala activation by fear-inducing visual stimuli in 15 healthy males after double-blind crossover intranasal application of placebo or oxytocin. Compared with placebo, oxytocin potently reduced activation of the amygdala and reduced coupling of the amygdala to brainstem regions implicated in autonomic and behavioral manifestations of fear. Our results indicate a neural mechanism for the effects of oxytocin in social cognition in the human brain and provide a methodology and rationale for exploring therapeutic strategies in disorders in which abnormal amygdala function has been implicated, such as social phobia or autism.Entities:
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Year: 2005 PMID: 16339042 PMCID: PMC6725903 DOI: 10.1523/JNEUROSCI.3984-05.2005
Source DB: PubMed Journal: J Neurosci ISSN: 0270-6474 Impact factor: 6.167