Vagal afferents mediate antinociception of estrogen in a rat model of visceral pain : The involvement of intestinal mucosal mast cells and 5-hydroxytryptamine 3 signaling

Research output: Journal Publications and ReviewsRGC 21 - Publication in refereed journalpeer-review

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Author(s)

  • Xiu-Juan Yan
  • Chen-Chen Feng
  • Qing Liu
  • Li-Yan Zhang
  • Xiao Dong
  • Zong-Liang Liu
  • Zhi-Jun Cao
  • Jian-Zhong Mo
  • Jing-Yuan Fang
  • Sheng-Liang Chen

Detail(s)

Original languageEnglish
Pages (from-to)204-217
Journal / PublicationJournal of Pain
Volume15
Issue number2
Online published12 Nov 2013
Publication statusPublished - Feb 2014

Abstract

Estrogen reportedly facilitates visceral nociception at the spinal or supraspinal level. The present study was aimed to investigate whether estrogen modulates visceral pain through the vagal pathway. Ovariectomized rats received estradiol, which was administered subcutaneously (to act through both the vagal and spinal pathways) or intraduodenally (to preferentially act through the vagal pathway). Luminally applied estradiol induced a rapid and significant decrease in the visceromotor response to colorectal distension, with increased c-Fos expression in nodose ganglion neurons. Systemically injected estradiol increased visceromotor response and c-Fos expression in both nodose and dorsal root ganglion (T6-12) neurons. The antinociceptive effect of estrogen was abolished by surgical vagotomy or chemical denervation of vagal afferents. Both luminally and systemically administered estradiol elicited selective 5-hydroxytryptamine secretion from the duodenum. Granisetron, a 5-hydroxytryptamine 3 receptor antagonist, reversed the antinociceptive effect of estrogen. Intestinal mucosal mast cell stabilizers prevented estradiol-induced antinociception and 5-hydroxytryptamine secretion. Ultrastructural analysis revealed that estradiol caused piecemeal degranulation of intestinal mucosal mast cells. The actions of estradiol were inhibited by an estrogen receptor β antagonist and mimicked by an estrogen receptor β agonist. These results suggest that estrogen can trigger vagus-mediated antinociception, which is masked by its spinally mediated pronociception. Perspective This study is the first to show a vagus-mediated estrogenic antinociception, in which the nongenomic estrogen receptor β-mediated, intestinal mucosal mast cell-derived 5-hydroxytryptamine/5- hydroxytryptamine 3 receptor pathway is involved. This work may provide new insights into the sex hormone modulation of visceral sensitivity related to irritable bowel syndrome and indicate potential therapeutic targets to manage this disease. © 2014 by the American Pain Society.

Research Area(s)

  • intestinal mucosal mast cells, serotonin, sex hormone, vagal afferents, Visceral pain

Citation Format(s)

Vagal afferents mediate antinociception of estrogen in a rat model of visceral pain: The involvement of intestinal mucosal mast cells and 5-hydroxytryptamine 3 signaling. / Yan, Xiu-Juan; Feng, Chen-Chen; Liu, Qing et al.
In: Journal of Pain, Vol. 15, No. 2, 02.2014, p. 204-217.

Research output: Journal Publications and ReviewsRGC 21 - Publication in refereed journalpeer-review