Rodrigo Triana-Del Río scite author profile

The extinction of conditioned fear responses entrains the formation of safe new memories to decrease those behavioral responses. The knowledge in neuronal mechanisms of extinction is fundamental in the treatment of anxiety and fear disorders. Interestingly, the use of pharmacological compounds that reduce anxiety and fear has been shown as a potent co-adjuvant in extinction therapy. However, the efficiency and mechanisms by which pharmacological compounds promote extinction of fear memories remains still largely unknown and would benefit from a validation based on functional neuronal circuits, and the neurotransmitters that modulate them. From this perspective, oxytocin receptor signaling, which has been shown in cortical and limbic areas to modulate numerous functions (Eliava et al. Neuron 89(6):1291-1304, 2016), among them fear and anxiety circuits, and to enhance the salience of social stimuli (Stoop Neuron 76(1):142-59, 2012), may offer an interesting perspective. Experiments in animals and humans suggest that oxytocin could be a promising pharmacological agent at adjusting memory consolidation to boost fear extinction. Additionally, it is possible that long-term changes in endogenous oxytocin signaling can also play a role in reducing expression of fear at different brain targets. In this review, we summarize the effects reported for oxytocin in corticolimbic circuits and on fear behavior that are of relevance for the modulation and potential extinction of fear memories.

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Same-sex cohabitation under the effects of quinpirole induces a conditioned socio-sexual partner preference in males, but not in female rats

Río

Montero-Domínguez

Cibrián‐Llanderal

et al. 2011

Pharmacology Biochemistry and Behavior

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Enhaced D2-type receptor activity facilitates the development of conditioned same-sex partner preference in male rats

Cibrián‐Llanderal

Rosas-Aguilar

Río

et al. 2012

Pharmacology Biochemistry and Behavior

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Conditioned same-sex partner preference in male rats is facilitated by oxytocin and dopamine: Effect on sexually dimorphic brain nuclei

Río

Tecamachaltzi-Silvarán

Díaz-Estrada

et al. 2015

Behavioural Brain Research

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