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Keywords

Sexual “Unseen” Activation Affects Amphetamine Cord Cues D2 Dopamine Drug Dysfunction Erectile Function Gastrin-Releasing Implications

Month Published

 

Jan 2008 Dec 2009

Country


  • United States 2 (%)
  • Canada 1 (%)
  • Japan 1 (%)

Institution

( see all 8)

  • Department of Neurology, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania, United States of America 1 (%)
  • Department of Psychiatry, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania, United States of America 1 (%)
  • Department of Psychology 1 (%)
  • Falk Center for Molecular Therapeutics, Northwestern University, Evanston, Illinois, United States of America 1 (%)
  • Kyoto Prefectural University of Medicine 1 (%)

Author

( see all 27)

  • Breedlove, S. Marc 1 (%)
  • Burgdorf, Jeffrey 1 (%)
  • Childress, Anna Rose 1 (%)
  • Detre, John 1 (%)
  • Ehrman, Ronald N. 1 (%)

Publication


  • PLoS ONE 3 (%)

Publication Type


  • Journal 3 (%)

Publisher


  • PubMed Central [x] 3 (%)

Subject

( see all 26)

  • Behavioral Neuroscience 3 (%)
  • Neuroscience 3 (%)
  • Sexual Dysfunction [x] 3 (%)
  • Cognitive Neuroscience 2 (%)
  • Mental Health 2 (%)

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  • 3 Articles
  • 27 Authors
  • 8 Institutions
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Stress Affects a Gastrin-Releasing Peptide System in the Spinal Cord That Mediates Sexual Function: Implications for Psychogenic Erectile Dysfunction

PLoS ONE (2009): 4 , January 26, 2009

By  Sakamoto, Hirotaka; Matsuda, Ken-Ichi; Zuloaga, Damian G.; Nishiura, Nobuko; Takanami, Keiko; Jordan, Cynthia L.; Breedlove, S. Marc; Kawata, Mitsuhiro Show all (8)

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Background

Many men suffering from stress, including post-traumatic stress disorder (PTSD), report sexual dysfunction, which is traditionally treated via psychological counseling. Recently, we identified a gastrin-releasing peptide (GRP) system in the lumbar spinal cord that is a primary mediator for male reproductive functions.

Methodology/Principal Findings

To ask whether an acute severe stress could alter the male specific GRP system, we used a single-prolonged stress (SPS), a putative rat model for PTSD in the present study. Exposure of SPS to male rats decreases both the local content and axonal distribution of GRP in the lower lumbar spinal cord and results in an attenuation of penile reflexes in vivo . Remarkably, pharmacological stimulation of GRP receptors restores penile reflexes in SPS-exposed males, and induces spontaneous ejaculation in a dose-dependent manner. Furthermore, although the level of plasma testosterone is normal 7 days after SPS exposure, we found a significant decrease in the expression of androgen receptor protein in this spinal center.

Conclusions/Significance

We conclude that the spinal GRP system appears to be a stress-vulnerable center for male reproductive functions, which may provide new insight into a clinical target for the treatment of erectile dysfunction triggered by stress and psychiatric disorders.

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Prelude to Passion: Limbic Activation by “Unseen” Drug and Sexual Cues

PLoS ONE (2008): 3 , January 30, 2008

By  Childress, Anna Rose; Ehrman, Ronald N.; Wang, Ze; Li, Yin; Sciortino, Nathan; Hakun, Jonathan; Jens, William; Suh, Jesse; Listerud, John; Marquez, Kathleen; Franklin, Teresa; Langleben, Daniel; Detre, John; O'Brien, Charles P. Show all (14)

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Background

The human brain responds to recognizable signals for sex and for rewarding drugs of abuse by activation of limbic reward circuitry. Does the brain respond in similar way to such reward signals even when they are “unseen”, i.e., presented in a way that prevents their conscious recognition? Can the brain response to “unseen” reward cues predict the future affective response to recognizable versions of such cues, revealing a link between affective/motivational processes inside and outside awareness?

Methodology/Principal Findings

We exploited the fast temporal resolution of event-related functional magnetic resonance imaging (fMRI) to test the brain response to “unseen” (backward-masked) cocaine, sexual, aversive and neutral cues of 33 milliseconds duration in male cocaine patients (n = 22). Two days after scanning, the affective valence for visible versions of each cue type was determined using an affective bias (priming) task. We demonstrate, for the first time, limbic brain activation by “unseen” drug and sexual cues of only 33 msec duration. Importantly, increased activity in an large interconnected ventral pallidum/amygdala cluster to the “unseen” cocaine cues strongly predicted future positive affect to visible versions of the same cues in subsequent off-magnet testing, pointing both to the functional significance of the rapid brain response, and to shared brain substrates for appetitive motivation within and outside awareness.

Conclusions/Significance

These findings represent the first evidence that brain reward circuitry responds to drug and sexual cues presented outside awareness. The results underscore the sensitivity of the brain to “unseen” reward signals and may represent the brain's primordial signature for desire. The limbic brain response to reward cues outside awareness may represent a potential vulnerability in disorders (e.g., the addictions) for whom poorly-controlled appetitive motivation is a central feature.

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Ultrasonic Vocalizations Induced by Sex and Amphetamine in M2, M4, M5 Muscarinic and D2 Dopamine Receptor Knockout Mice

PLoS ONE (2008): 3 , April 02, 2008

By  Wang, Haoran; Liang, Shuyin; Burgdorf, Jeffrey; Wess, Jurgen; Yeomans, John Show all (5)

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Adult mice communicate by emitting ultrasonic vocalizations (USVs) during the appetitive phases of sexual behavior. However, little is known about the genes important in controlling call production. Here, we study the induction and regulation of USVs in muscarinic and dopaminergic receptor knockout (KO) mice as well as wild-type controls during sexual behavior. Female mouse urine, but not female rat or human urine, induced USVs in male mice, whereas male urine did not induce USVs in females. Direct contact of males with females is required for eliciting high level of USVs in males. USVs (25 to120 kHz) were emitted only by males, suggesting positive state; however human-audible squeaks were produced only by females, implying negative state during male-female pairing. USVs were divided into flat and frequency-modulated calls. Male USVs often changed from continuous to broken frequency-modulated calls after initiation of mounting. In M2 KO mice, USVs were lost in about 70–80% of the mice, correlating with a loss of sexual interaction. In M5 KO mice, mean USVs were reduced by almost 80% even though sexual interaction was vigorous. In D2 KOs, the duration of USVs was extended by 20%. In M4 KOs, no significant differences were observed. Amphetamine dose-dependently induced USVs in wild-type males (most at 0.5 mg/kg i.p.), but did not elicit USVs in M5 KO or female mice. These studies suggest that M2 and M5 muscarinic receptors are needed for male USV production during male-female interactions, likely via their roles in dopamine activation. These findings are important for the understanding of the neural substrates for positive affect.

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