Literature DB >> 21635894

Mechanisms responsible for progesterone's protection against lordosis-inhibiting effects of restraint I. Role of progesterone receptors.

James Hassell1, Chandra Suma Johnson Miryala, Cindy Hiegel, Lynda Uphouse.   

Abstract

Progestins and antiprogestins are widely used therapeutic agents in humans. In many cases, these are indicated for the treatment of reproductive activities. However, progesterone has widespread physiological effects including a reduction of the response to stress. We have reported that 5 min of restraint reduced lordosis behavior of ovariectomized rats hormonally primed with estradiol benzoate. When ovariectomized rats received both estradiol benzoate and progesterone priming, restraint had minimal effects on lordosis. Progesterone influences behavior through classical intracellular progesterone receptor-mediated nuclear events as well as extranuclear events. How these multiple events contribute to the response to stress is unclear. The current project was designed to initiate examination of the mechanisms responsible for progesterone's ability to protect against the effects of the restraint. In the first experiment, ovariectomized rats, primed with 10 μg estradiol benzoate, received 500 μg progesterone 4 h, 1 h, or 30 min before restraint. When progesterone was injected 4h before restraint, progesterone eliminated the effects of restraint. In contrast, progesterone 30 min before restraint offered no protection. Effects of progesterone 1h before restraint were equivocal allowing the suggestion that less than 4h of progesterone priming might be sufficient. In the second experiment, the synthetic progestin, medroxyprogesterone, was shown to mimic effects of progesterone in preventing effects of restraint. Finally, the progesterone receptor antagonist, RU486, attenuated progesterone's protection against restraint. These findings offer evidence that ligand-activated progesterone receptor mechanisms contribute to the maintenance of lordosis behavior in the presence of mild stress.
Copyright © 2011 Elsevier Inc. All rights reserved.

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Year:  2011        PMID: 21635894      PMCID: PMC3126914          DOI: 10.1016/j.yhbeh.2011.05.006

Source DB:  PubMed          Journal:  Horm Behav        ISSN: 0018-506X            Impact factor:   3.587


  58 in total

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1.  Prior hormonal treatment, but not sexual experience, reduces the negative effects of restraint on female sexual behavior.

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Authors:  Lynda Uphouse
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4.  Repeated estradiol benzoate treatment protects against the lordosis-inhibitory effects of restraint and prevents effects of the antiprogestin, RU486.

Authors:  Lynda Uphouse; Cindy Hiegel; Giovanny Martinez; Christian Solano; William Gusick
Journal:  Pharmacol Biochem Behav       Date:  2015-07-17       Impact factor: 3.533

5.  Allopregnanolone's attenuation of the lordosis-inhibiting effects of restraint is blocked by the antiprogestin, CDB-4124.

Authors:  Lynda Uphouse; Cindy Hiegel
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6.  An antiprogestin, CDB4124, blocks progesterone's attenuation of the negative effects of a mild stress on sexual behavior.

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7.  RU486 blocks effects of allopregnanolone on the response to restraint stress.

Authors:  Lynda Uphouse; Sarah Adams; Chandra Suma Johnson Miryala; James Hassell; Cindy Hiegel
Journal:  Pharmacol Biochem Behav       Date:  2012-10-06       Impact factor: 3.533

  7 in total

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