Social approach and social vigilance are differentially regulated by oxytocin receptors in the nucleus accumbens

Alexia V Williams,Stephanie Ramos-Maciel,Bice Chini,Kenneth Jackson,Brian C Trainor,Shanu K Bhela,Natalia Duque-Wilckens,Patricia A Pesavento,Christine K Xu,Katharine L Campi

doi:10.1038/s41386-020-0657-4

Abstract

Oxytocin is currently being considered as a novel therapeutic for anxiety disorders due to its ability to promote affiliative behaviors. In the nucleus accumbens (NAc) activation of oxytocin receptors (OTR) promotes social approach (time spent near an unfamiliar individual). Here, we show that stressful social experiences reduce the expression of NAc OTR mRNA, coinciding with decreases in social approach. Social stressors also increase social vigilance, characterized as orienting to an unfamiliar individual without approaching. Vigilance is a key component of behavioral inhibition, a personality trait that is a risk factor for anxiety disorders. To understand whether NAc OTR can modulate both social approach and vigilance, we use pharmacological approaches to assess the impact of activation or inhibition of NAc OTR downstream pathways on these behaviors. First, we show that in unstressed male and female California mice, inhibition of OTR by an unbiased antagonist (L-368,899) reduces social approach but does not induce social vigilance. Next, we show that infusion of Atosiban, an OTR-Gq antagonist/OTR-Gi agonist, has the same effect in unstressed females. Finally, we show that Carbetocin, a biased OTR-Gq agonist, increases social approach in stressed females while simultaneously inhibiting social vigilance. Taken together these data suggest that OTR in the NAc differentially modulate social approach and social vigilance, primarily through an OTR-Gq mechanism. Importantly, pharmacological inhibition of OTR alone is insufficient to induce vigilance in unstressed mice, suggesting that mechanisms modulating social approach may be distinct from mechanisms modulating social vigilance.

Highlights

Avoidance of social situations is a hallmark symptom of a variety of psychiatric illnesses, including mood disorders, anxiety disorders [1], and several neurodevelopmental disorders such as autism [2, 3]
Across three experiments, using site-specific injections of two different oxytocin receptors (OTR) antagonists, L-368,899 and Atosiban, we show that reduced OTR signaling within the nucleus accumbens (NAc) reduces social approach without increasing social vigilance
Despite its OTR-Gi agonism properties, inhibition of OTR-Gq signaling with Atosiban had similar effects on social approach, suggesting that OTR-Gq in the NAc is necessary to promote social approach

Summary

Introduction

Avoidance of social situations is a hallmark symptom of a variety of psychiatric illnesses, including mood disorders, anxiety disorders [1], and several neurodevelopmental disorders such as autism [2, 3]. Other reports find that intranasal oxytocin treatment can have very different effects, especially in situations where an undercurrent of stress or threat exists [9, 10]. In some cases, intranasal oxytocin has been shown to increase antagonistic social interactions in both humans [11, 12] and female Wistar rats [13,14,15]. Taken together this supports the idea that the impacts of oxytocin on social behavior are complex and differ based on context [16, 17]. Actions of oxytocin appear to be circuit-specific [17], which may be one possible mechanism for its contextdependent actions

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Conclusion