Effects of Endothelin Receptor Type-A and Type-B Antagonists on Prostaglandin F2alpha-Induced Luteolysis of the Sheep Corpus Luteum

doi:10.1095/biolreprod.107.064105

HOME

QUICK SEARCH:

	Author:		Keyword(s):
Year:		Vol:		Page:

BOR - Papers in Press, published online ahead of print December 12, 2007.
Biol Reprod 2007, 10.1095/biolreprod.107.064105

This Article

	Full Text (Rapid PDF)
	All Versions of this Article: 78/4/688 most recent biolreprod.107.064105v1
	Alert me when this article is cited
	Alert me if a correction is posted

Services

	Email this article to a friend
	Similar articles in this journal
	Similar articles in PubMed
	Alert me to new issues of the journal
	Download to citation manager


Citing Articles

	Citing Articles via Google Scholar

Google Scholar

	Articles by Doerr, M. D.
	Articles by Flores, J. A.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Doerr, M. D.
	Articles by Flores, J. A.

Agricola

	Articles by Doerr, M. D.
	Articles by Flores, J. A.

Submitted July 6, 2007
Returned for revision August 4, 2007
Accepted December 3, 2007

Ovary

Effects of Endothelin Receptor Type-A and Type-B Antagonists on Prostaglandin F_2alpha-Induced Luteolysis of the Sheep Corpus Luteum

Matthew D. Doerr , Madhusudan P. Goravanahally , Justin D. Rhinehart , E. Keith Inskeep , and Jorge A. Flores ^*

^* To whom correspondence should be addressed. E-mail: jflores{at}wvu.edu.

Abstract
Three experiments were designed to examine the mechanisms thatgovern PGF_2alpha-induced regression of the sheep corpus luteum(CL). Evidence is presented supporting the involvement of endothelin1 (EDN1) in PGF_2alpha-induced luteolysis. Experiment 1measuredeffects of PGF_2alpha when actions of EDN1 were blocked by sustainedadministration of a type-A endothelin (EDNRA) or type-B endothelin(EDNRB) antagonist in vivo. Experiment 2 examined anti-steroidogenicactions of PGF_2alpha and EDN1 in the presence of an EDNRA orEDNRB antagonist in d-8 luteal minces. In experiment 3, lutealcellular expression of EDNRA and EDNRB was determined immunohistochemically.Relative gene expression of EDNRA and EDNRB receptors was examinedby real-time RT-PCR in d-8 sheep CL. EDNRA, but not EDNRB, participatedin anti-steroidogenic actions of EDN1. During the first 12 hafter PGF_2alpha, EDNRA antagonist did not prevent decline inserum progesterone. Early actions of PGF_2alpha are either director mediated by other than EDN1. However, beyond 12 h afterPGF_2alpha, serum progesterone increased in EDNRA antagonist-treatedanimals until not different from saline-treated controls, whereasan EDNRB antagonist had no effect in vivo or in vitro. The EDNRAantagonist negated the antisteroidogenic actions of EDN1 butonly partially abolished the actions of PGF_2alpha in vitro.In contrast, the EDNRB antagonist was ineffective in abolishingantisteroidogenic actions of EDN1 and PGF_2alpha. Whereas real-timeRT-PCR demonstrated high expression of EDNRA and low expressionof EDNRB, immunohistochemically, only EDNRA was located in smallsteroidogenic, endothelial, and smooth muscle cells. In summary,studies in ovine CL provided strong evidence that: 1) EDNRA,but not EDNRB, mediate anti-steroidogenic actions of EDN1; 2)actions of PGF_2alpha are both independent of and dependent upon,mediation by EDN1; and 3) small steroidogenic cells are targetsfor anti-steroidogenic effects of EDN1. Furthermore, the resultsfrom experiment 1 suggest that the intermediary role of EDN1may be more important in later stages of luteal regression.

Key words: Ovary • Corpus luteum • Corpus luteum function • Progesterone • Steroid hormones