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Title		Authors	PubMed ID
1	Disaster-related prenatal maternal stress predicts HPA reactivity and psychopathology in adolescent offspring: Project Ice Storm.	Yong Ping E, Laplante DP, Elgbeili G, Jones SL, Brunet A, King S	32442863 PSYCHOLOGY
2	Aromatization Is Not Required for the Facilitation of Appetitive Sexual Behaviors in Ovariectomized Rats Treated With Estradiol and Testosterone.	Jones SL, Rosenbaum S, Gardner Gregory J, Pfaus JG	31447629 CSBN
3	Age-specific associations between oestradiol, cortico-amygdalar structural covariance, and verbal and spatial skills.	Nguyen TV, Jones SL, Gower T, Lew J, Albaugh MD, Botteron KN, Hudziak JJ, Fonov VS, Louis Collins D, Campbell BC, Booij L, Herba CM, Monnier P, Ducharme S, Waber D, McCracken JT	30776161 PSYCHOLOGY
4	Sensitization of sexual behaviors in ovariectomized Long-Evans rats is induced by a subthreshold dose of estradiol benzoate and attenuated by repeated copulation.	Jones SL, Pfaus JG	25251978 PSYCHOLOGY
5	The inhibitory effects of corncob bedding on sexual behavior in the ovariectomized Long-Evans rat treated with estradiol benzoate are overcome by male cues.	Jones SL, Antonie RA, Pfaus JG	25960082 PSYCHOLOGY
6	Repeated administration of estradiol promotes mechanisms of sexual excitation and inhibition: Glutamate signaling in the ventromedial hypothalamus attenuates excitation.	Jones SL, Farisello L, Mayer-Heft N, Pfaus JG	26008158 PSYCHOLOGY
7	Behavioral defeminization by prenatal androgen treatment in rats can be overcome by sexual experience in adulthood.	Jones SL, Cordeaux E, Germé K, Pfaus JG	26163151 PSYCHOLOGY
8	RU486 facilitates or disrupts the sensitization of sexual behaviors by estradiol in the ovariectomized Long-Evans rat: Effect of timecourse.	Jones SL, Gardner Gregory J, Pfaus JG	26210062 PSYCHOLOGY
9	Vaginocervical stimulation attenuates the sensitization of appetitive sexual behaviors by estradiol benzoate in the ovariectomized rat.	Jones SL, Germé K, Graham MD, Roy P, Gardner Gregory J, Rosenbaum S, Parada M, Pfaus JG	26278846 PSYCHOLOGY
10	Facilitation of sexual behavior in ovariectomized rats by estradiol and testosterone: A preclinical model of androgen effects on female sexual desire.	Jones SL, Ismail N, Pfaus JG	28278441 PSYCHOLOGY

Title:	Aromatization Is Not Required for the Facilitation of Appetitive Sexual Behaviors in Ovariectomized Rats Treated With Estradiol and Testosterone.
Authors:	Jones SL, Rosenbaum S, Gardner Gregory J, Pfaus JG
Link:	https://www.ncbi.nlm.nih.gov/pubmed/31447629?dopt=Abstract
DOI:	10.3389/fnins.2019.00798
Publication:	Frontiers in neuroscience
Keywords:	aromatase; estradiol; fadrozole; preclinical model; sexual desire; testosterone;
PMID:	31447629	Category:	Front Neurosci	Date Added:	2019-08-27
Dept Affiliation:	CSBN 1 Department of Psychology, Center for Studies in Behavioral Neurobiology, Concordia University, Montreal, QC, Canada.

Description:

Aromatization Is Not Required for the Facilitation of Appetitive Sexual Behaviors in Ovariectomized Rats Treated With Estradiol and Testosterone.

Front Neurosci. 2019;13:798

Authors: Jones SL, Rosenbaum S, Gardner Gregory J, Pfaus JG

Abstract

Testosterone can be safely and effectively administered to estrogen-treated post-menopausal women experiencing hypoactive sexual desire. However, in the United States and Canada, although it is often administered off-label, testosterone co-administered with estradiol is not a federally approved treatment for sexual arousal/desire disorder, partly because its mechanism is poorly understood. One possible mechanism involves the aromatization of testosterone to estradiol. In an animal model, the administration of testosterone propionate (TP) given in combination with estradiol benzoate (EB) significantly increases sexually appetitive behaviors (i.e., solicitations and hops/darts) in ovariectomized (OVX) Long-Evans rats, compared to those treated with EB-alone. The goal of current study was to test whether blocking aromatization of testosterone to estradiol would disrupt the facilitation of sexual behaviors in OVX Long-Evans rats, and to determine group differences in Fos immunoreactivity within brain regions involved in sexual motivation and reward. Groups of sexually experienced OVX Long-Evans rats were treated with EB alone, EB+TP, or EB+TP and the aromatase inhibitor Fadrozole (EB+TP+FAD). Females treated with EB+TP+FAD displayed significantly more hops and darts, solicitations and lordosis magnitudes when compared to EB-alone females. Furthermore, TP, administered with or without FAD, induced the activation of Fos-immunoreactivity in brain areas implicated in sexual motivation and reward including the medial preoptic area, ventrolateral division of the ventromedial nucleus of the hypothalamus, the nucleus accumbens core, and the prefrontal cortex. These results suggest that aromatization may not be necessary for TP to enhance female sexual behavior and that EB+TP may act via androgenic pathways to increase the sensitivity of response to male-related cues, to induce female sexual desire.

PMID: 31447629 [PubMed]

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