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Pubertal androgens reduce the effects of social stress on anxiety-related behaviors in California mice

TLDR
It is shown that in juveniles, social defeat reduces social approach and increases social vigilance in both males and females, and evidence that androgen receptors play an important role in the development of neural circuits of anxiety is provided.
Abstract
Adolescence is an important developmental period during which anxiety-related behaviors differentiate in males and females. In humans anxiety prevalence increases to a greater degree in women than men after puberty, but the mechanism is unknown. We used social defeat stress to model anxiety behaviors in California mouse, a species in which aggressive females allow for comparison of social anxiety behaviors across sex. Adult female California mice show reduced social approach and increased social vigilance after exposure to stress, while these changes are weaker in males. Here we show that in juveniles, social defeat reduces social approach and increases social vigilance in both males and females. Next, we show that prepubertal castration sensitizes adult males to social defeat. However, when pubertal castration was paired with either testosterone or dihydrostesterone replacement, effects of defeat on social approach and vigilance were blunted in adult males. We also showed that effects of defeat on social behavior in juveniles were oxytocin receptor dependent, as has been described for adult females. This work highlights the importance of pubertal testosterone to the development of sex differences in anxiety behavior, and provides evidence that androgen receptors play an important role in the development of neural circuits of anxiety.

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Enriched laboratory housing increases sensitivity to social stress in female California mice (Peromyscus californicus)

TL;DR: In this article, the authors evaluated the effect of different housing conditions on the behavior of California mice and found that large and large+EE housing increased the sensitivity of these tests to detect stress induced phenotypes in females.
Journal ArticleDOI

Acute intranasal oxytocin dose enhances social preference for parents over peers in male but not female peri-adolescent California mice (Peromyscus californicus).

TL;DR: In this article , an acute intranasal (IN) treatment of 0.5 IU/kg IN AVP and saline control was administered to male and female peri-adolescent mice.
References
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Adolescent Brain Development: A Period of Vulnerabilities and Opportunities. Keynote Address

TL;DR: A conceptual framework for understanding adolescence is provided, which emphasizes how the very nature of this developmental transition requires an interdisciplinary approach—one that focuses on brain/behavior/social‐context interactions during this important maturational period.
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A standardized protocol for repeated social defeat stress in mice

TL;DR: A protocol whereby C57BL/6J mice that are repeatedly subjected to bouts of social defeat by a larger and aggressive CD-1 mouse results in the development of a clear depressive-like syndrome, characterized by enduring deficits in social interactions.
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Pubertal hormones organize the adolescent brain and behavior.

TL;DR: A review of the evidence that steroid-dependent organization of the adolescent brain programs a variety of adult behaviors in animals and humans can be found in this article, where convergence lines of evidence indicate that adolescence may be a sensitive period for steroiddependent brain organization and that variation in the timing of interactions between the hormones of puberty and the adult brain leads to individual differences in adult behavior and risk of sexbiased psychopathologies.
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Functional Cross-Talk Between the Hypothalamic-Pituitary-Gonadal and -Adrenal Axes

TL;DR: A dual approach in the male rat reveals that testosterone can act and interact on different aspects of basal and stress HPA function, and holds great promise in establishing further links between the neuroendocrinology of stress and the central bases of sex‐dependent disorders, including psychiatric, cardiovascular and metabolic disease.
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Incidence of social anxiety disorder and the consistent risk for secondary depression in the first three decades of life.

TL;DR: Social anxiety disorder is an early, adolescent-onset disorder related to a substantially and consistently increased risk for subsequent depression, and targeted prevention is called for with the aim of reducing the burden of SAD and its consequences.
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