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      Stress rapidly suppresses in vivo LH pulses and increases activation of RFRP-3 neurons in male mice

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          Abstract

          Restraint stress is a psychosocial stressor that suppresses reproductive status, including LH pulsatile secretion, but the neuroendocrine mechamisms underlying this inhibition remains unclear. Reproductive neural populations upstream of gonadotropin releasing hormone (GnRH) neurons, such as kisspeptin, neurokinin B, and RFRP-3 (GnIH) neurons, are possible targets for psychosocial stress to inhibit LH pulses, but this has not been well-examined, especially in mice in which prior technical limitations prevented assessment of in vivo LH pulse secretion dynamics. Here we examined whether one-time acute restraint stress alters in vivo LH pulsatility and reproductive neural populations in male mice, and what the time-course is for such alterations. We found that endogenous LH pulses in castrated male mice are robustly and rapidly suppressed by one-time, acute restraint stress, with suppression observed as quickly as 12–18 min. This rapid LH suppression parallels with increased in vivo corticosterone levels within 15 min of restraint stress. Although Kiss1, Tac2, and Rfrp gene expression in the hypothalamus did not significantly change after 90 or 180 min restraint stress, arcuate Kiss1 neural activation was sigmnifciantly decreased after 180 min. Interestingly, hypothalamic Rfrp neuronal activation was strongly increased at early times after restraint stress initiation, but was attenuated to levels lower than controls by 180 min of restraint stress. Thus, the male neuroendocrine reproductive axis is quite sensitive to short-term stress exposure, with significantly decreased pulsatile LH secretion and increased hypothalamic Rfrp neuronal activation occurring rapidly, within minutes, and decreased Kiss1 neuronal activation also occurring after longer stress durations.

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          Author and article information

          Journal
          0375363
          4713
          J Endocrinol
          J. Endocrinol.
          The Journal of endocrinology
          0022-0795
          1479-6805
          14 September 2018
          31 October 2018
          31 October 2018
          31 October 2019
          : 239
          : 3
          : 339-350
          Affiliations
          [1 ]Department of Obstetrics, Gynecology, and Reproductive Sciences, University of California, San Diego, La Jolla, CA 92093
          [2 ]Neuroscience Program, Washington and Lee University, Lexington, Virginia 24450
          Author notes
          Corresponding Author address: Alexander S. Kauffman, Department of Obstetrics, Gynecology, and Reproductive Sciences, University of California, San Diego, 9500 Gilman Drive, MC 0674, La Jolla, CA 92093, akauffman@ 123456ucsd.edu , Telephone: 858-246-0219
          Article
          PMC6214202 PMC6214202 6214202 nihpa1506394
          10.1530/JOE-18-0449
          6214202
          30382693
          f044b2ce-a704-4562-b39f-2759439f44db
          History
          Categories
          Article

          Rfrp,corticosterone,stress,restraint,Kiss1,kisspeptin,GnIH
          Rfrp, corticosterone, stress, restraint, Kiss1, kisspeptin, GnIH

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