Participation of Prostaglandin E<sub>2</sub> in Contractile Activity of Inflamed Porcine Uterus

Jana, Barbara; Jaroszewski, Jerzy; Kucharski, Jan; Koszykowska, Marlena; Górska, Jolanta; Markiewicz, Włodzimierz

doi:10.2754/avb201079020249

Acta Veterinaria > Archive > 2010, Vol. 79 > Issue 2 > Participation of Prostaglandin…

Acta Vet. Brno 2010, 79: 249-259

https://doi.org/10.2754/avb201079020249

Participation of Prostaglandin E₂ in Contractile Activity of Inflamed Porcine Uterus

Barbara Jana¹, Jerzy Jaroszewski², Jan Kucharski¹, Marlena Koszykowska¹, Jolanta Górska¹, Włodzimierz Markiewicz²

¹Division of Reproductive Endocrinology and Pathophysiology, Institute of Animal Reproduction and Food Research, Polish Academy of Sciences, Olsztyn, Poland,
²Division of Pharmacology, Department of Pathology and Pharmacology, Faculty of Veterinary Medicine, University of Warmia and Mazury, Olsztyn, Poland

Received February 10, 2009
Accepted December 3, 2009

The aim of our study was to estimate the participation of prostaglandin E₂ (PGE₂) in the contractile activity of inflamed porcine uterus. On day 3 of the oestrous cycle, 50 ml of saline or 50 ml of Escherichia coli suspension, containing 10⁹ colony-forming units/ml, was injected into each uterine horn in the control or experimental group, respectively. Seven days later the uteri were collected. Endometritis developed in all bacteria-inoculated gilts. Endometrium/myometrium and myometrium strips were incubated with PGE₂ alone or together with PGE₂ receptor (EP) subtypes (EP₂, EP₄, EP₁ and EP₃) blockers: AH 6809 (BEP₂), ONO-AE₂ (BEP₄), ONO-AE₃-240 (BEP₁) and SC19220 (BEP₃), respectively. In the control group, PGE₂ (10^-8 and 10^-7 M) increased the intensity of contractions in endometrium/myometrium, and at the higher dose in myometrium. PGE₂ (10^-8 M) decreased the contraction intensity of the strips from inflamed uteri. After the use of BEP₂, PGE₂ (10^-7 M) increased the values of this indicator in endometrium/myometrium and myometrium from the control gilts. In these animals, PGE₂ (10^-8 M) in the presence of BEP₄ reduced the contraction intensity in endometrium/myometrium. In the bacterial group, PGE₂ (10^-8 M) in the presence of BEP₂ and BEP₄ enhanced the intensity of contractions in myometrium. Similar reaction was evoked by PGE₂ (10^-7 M) in endometrium/myometrium of the inflamed uteri in the presence of BEP₄. The intensity of contractions in myometrium from the inflamed uteri significantly decreased after the use of BEP₁ and PGE₂ (10^-7 M). PGE₂ (10^-7 M) administered after BEP₃, significantly decreased the intensity of contractions in myometrium of the control gilts. These results show that PGE₂ decreases the contraction intensity of inflamed porcine uteri. Further studies are needed to closely determine the role of PGE₂ and other prostanoids in the contractile activity of inflamed uterine tissue.