Centrally released oxytocin mediates mating-induced anxiolysis in male rats

Waldherr, Martin; Neumann, Inga D.

doi:10.1073/pnas.0705860104

Cited by 240 publications

(190 citation statements)

References 39 publications

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“…This could result in impaired discrimination between familiar and unfamiliar female odor, thus, modifying sexual motivation. This is supported by the findings that exposure to the signals of an estrous female results in the activation of brain OT at the level of the paraventricular nucleus of the hypothalamus (Waldherr and Neumann, 2007). Moreover, this OT activation was associated with an anxiolytic response and reduced emotional response to anxiogenic stimuli that is consistent with an enhanced risk taking and boldness.…”

Section: Discussionsupporting

confidence: 73%

Estrogen receptors α and β mediate different aspects of the facilitatory effects of female cues on male risk taking

Kavaliers

Devidze

Choleris

et al. 2008

Psychoneuroendocrinology

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SummaryMale risk taking and decision making are affected by sex-related cues, with men making poorer and riskier decisions in the presence of females and, or their cues. In non-human species, female cues can also increase male risk taking, reducing their responses to predator threat. As estrogen receptors α and β (ERα and ERβ) are involved in the mediation of social and sexual responses, we investigated their roles in determining the effects of female-associated cues on male risk taking. We examined the effects of brief pre-exposure to the odors of either a novel or familiar estrous female on the avoidance of, and aversive responses to, predator threat (cat odor) in ERα and ERβ wild type (αERWT, βERWT) and gene-deleted (knockout, αERKO, βERKO) male mice. Exposure of αERWT and βERWT males to the odors of a novel, but not a familiar, estrous female mouse resulted in enhanced risk taking with the males displaying reduced avoidance of, and analgesic responses to, cat odor. In contrast, αERKO male mice failed to show any changes in risk taking, while βERKO males, although displaying greater risk taking, did not distinguish between novel and familiar females, displaying similarly reduced avoidance responses to cat odor after exposure to either a novel or familiar female odor. These findings indicate that the gene for ERα is associated with the sexual mechanisms (response to estrous female) and the genes for ERβ and ERα with the social (recognition of novel female) mechanisms underlying the effects of female cues on male risk taking. *Corresponding author. kavalier@uwo.ca (M. Kavaliers).

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Section: Discussionsupporting

confidence: 73%

Estrogen receptors α and β mediate different aspects of the facilitatory effects of female cues on male risk taking

Kavaliers

Devidze

Choleris

et al. 2008

Psychoneuroendocrinology

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“…Adult Oxtr Ϫ/Ϫ males show a deficit in social discrimination and an increase in aggressive behavior (Takayanagi et al, 2005). OXT has also been shown to mediate mating-induced anxiolysis in male rat (Waldherr and Neumann, 2007). However, the cellular mechanisms by which the OX-T-OXTR system modulates social and emotional behavior remain unknown.…”

Section: Introductionmentioning

confidence: 99%

“…In the brain, the OXTR is abundantly present in several brain regions (i.e., some cortical areas, the olfactory system, the basal ganglia, the limbic system, the thalamus, the hypothalamus, the brainstem, and the spinal cord) (Yoshimura et al, 1993;Vaccari et al, 1998;Gimpl and Fahrenholz, 2001), suggesting that the OXTR in the CNS has a wide variety of effects. In addition to its classical functions (i.e., induction of labor and milk ejection), OXT plays an important role in regulating social behaviors, anxiety-related behaviors, food intake, stress-related responses, and pain control (Ferguson et al, 2000;Gimpl and Fahrenholz, 2001;Takayanagi et al, 2005;Waldherr and Neumann, 2007).…”

Section: Introductionmentioning

confidence: 99%

Evidence That Oxytocin Exerts Anxiolytic Effects via Oxytocin Receptor Expressed in Serotonergic Neurons in Mice

Yoshida¹,

Takayanagi²,

Inoue³

et al. 2009

J. Neurosci.

519

493

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The oxytocin receptor has been implicated in the regulation of reproductive physiology as well as social and emotional behaviors. The neurochemical mechanisms by which oxytocin receptor modulates social and emotional behavior remains elusive, in part because of a lack of sensitive and selective antibodies for cellular localization. To more precisely characterize oxytocin receptor-expressing neurons within the brain, we generated an oxytocin receptor-reporter mouse in which part of the oxytocin receptor gene was replaced with Venus cDNA (a variant of yellow fluorescent protein). Examination of the Venus expression revealed that, in the raphe nuclei, about one-half of tryptophan hydroxylase-immunoreactive neurons were positive for Venus, suggesting a potential role for oxytocin in the modulation of serotonin release. Oxytocin infusion facilitated serotonin release within the median raphe nucleus and reduced anxiety-related behavior. Infusion of a 5-HT 2A/2C receptor antagonist blocked the anxiolytic effect of oxytocin, suggesting that oxytocin receptor activation in serotonergic neurons mediates the anxiolytic effects of oxytocin. This is the first demonstration that oxytocin may regulate serotonin release and exert anxiolytic effects via direct activation of oxytocin receptor expressed in serotonergic neurons of the raphe nuclei. These results also have important implications for psychiatric disorders such as autism and depression in which both the oxytocin and serotonin systems have been implicated.

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“…Oxytocin's actions in the brain reduce stress-induced corticosterone release and anxiety behavior in rodents 210 and oxytocin was also shown to be a key player in the social buffering of stress. Oxytocin release within the paraventricular nucleus of the hypothalamus, triggered by mating, mediated mating-induced anxiolytic behavior in male rats 211 . Oxytocin release that was independent of mating was involved in the buffering of stress-induced increases in anxiety-like behaviors and circulating corticosterone that occur in female prairie voles if the male partner is present 212 .…”

Section: Box 5 Social Buffering Of Stress In Rodents: Effects and Mementioning

confidence: 99%

Stress and the social brain: behavioural effects and neurobiological mechanisms

2015

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Centrally released oxytocin mediates mating-induced anxiolysis in male rats

Cited by 240 publications

References 39 publications

Estrogen receptors α and β mediate different aspects of the facilitatory effects of female cues on male risk taking

Estrogen receptors α and β mediate different aspects of the facilitatory effects of female cues on male risk taking

Evidence That Oxytocin Exerts Anxiolytic Effects via Oxytocin Receptor Expressed in Serotonergic Neurons in Mice

Stress and the social brain: behavioural effects and neurobiological mechanisms

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