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Orgasms, sexual pleasure, and opioid reward mechanisms

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Abstract Introduction Sexual activity produces pleasure related to sexual arousal, desire, and genitosensory and erogenous stimulation. Orgasms produce a whole brain and body rush of ecstatic pleasure followed by relaxation and refractoriness. This pleasure results from the activation of neurochemical reward pathways in the brain. This is differentiated by spinal pathways that control climax, the particular motor movements of the pelvic floor and the experience of tension release. Objectives To relate the activation of key neurochemical reward and bonding systems, notably dopamine, oxytocin, and opioids, to the pleasure of sexual activity in general and orgasms in particular. Methods A narrative review of the neurochemical and neuroanatomical mechanisms activated during sexual stimulation and orgasm in rats and humans, and how they are related overall to the generation of sexual pleasure and reward. Results Appetitive sexual pleasure involves the activation of dopamine and oxytocin release in hypothalamic and mesolimbic regions that regulate sexual arousal and desire, and are reinforced by localized opioid activity. Orgasms are thought to result in part from a massive release of opioids into these regions that inhibits dopamine and oxytocin transmission, but that initiates molecular changes to sensitize both systems and induce sexually conditioned place and partner preferences. Serotonin is also activated at orgasm and contributes to feelings of satiety and refractoriness. Orgasm disorders are distressing, cause resentment and conflict in a relationship, and diminish overall sexual health and well-being. Conclusions Orgasms are an important component of sexual pleasure for humans and perhaps all vertebrates. Endogenous opioids like β-endorphin that bind to mu opioid receptors are likely responsible for sexual pleasure and reward.
Oxford University Press (OUP)
Title: Orgasms, sexual pleasure, and opioid reward mechanisms
Description:
Abstract Introduction Sexual activity produces pleasure related to sexual arousal, desire, and genitosensory and erogenous stimulation.
Orgasms produce a whole brain and body rush of ecstatic pleasure followed by relaxation and refractoriness.
This pleasure results from the activation of neurochemical reward pathways in the brain.
This is differentiated by spinal pathways that control climax, the particular motor movements of the pelvic floor and the experience of tension release.
Objectives To relate the activation of key neurochemical reward and bonding systems, notably dopamine, oxytocin, and opioids, to the pleasure of sexual activity in general and orgasms in particular.
Methods A narrative review of the neurochemical and neuroanatomical mechanisms activated during sexual stimulation and orgasm in rats and humans, and how they are related overall to the generation of sexual pleasure and reward.
Results Appetitive sexual pleasure involves the activation of dopamine and oxytocin release in hypothalamic and mesolimbic regions that regulate sexual arousal and desire, and are reinforced by localized opioid activity.
Orgasms are thought to result in part from a massive release of opioids into these regions that inhibits dopamine and oxytocin transmission, but that initiates molecular changes to sensitize both systems and induce sexually conditioned place and partner preferences.
Serotonin is also activated at orgasm and contributes to feelings of satiety and refractoriness.
Orgasm disorders are distressing, cause resentment and conflict in a relationship, and diminish overall sexual health and well-being.
Conclusions Orgasms are an important component of sexual pleasure for humans and perhaps all vertebrates.
Endogenous opioids like β-endorphin that bind to mu opioid receptors are likely responsible for sexual pleasure and reward.

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