Prostacyclin primes pregnant human myometrium for an enhanced contractile response in parturition
Kristina M. Fetalvero, … , Roger C. Young, Kathleen A. Martin
Kristina M. Fetalvero, … , Roger C. Young, Kathleen A. Martin
Published November 20, 2008
Citation Information: J Clin Invest. 2008;118(12):3966-3979. https://doi.org/10.1172/JCI33800.
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Research Article

Prostacyclin primes pregnant human myometrium for an enhanced contractile response in parturition

Abstract

An incomplete understanding of the molecular events that regulate the myometrial transition from the quiescent pregnant state to the active contractile state during labor has hindered the development of improved therapies for preterm labor. During myometrial activation, proteins that prime the smooth muscle for contraction are upregulated, allowing maximal responsiveness to contractile agonists and thereby producing strong phasic contractions. Upregulation of one such protein, COX-2, generates PGs that induce contractions. Intriguingly, the predominant myometrial PG produced just prior to labor is prostacyclin (PGI2), a smooth muscle relaxant. However, here we have shown that activation of PGI2 receptor (IP) upregulated the expression of several contractile proteins and the gap junction protein connexin 43 through cAMP/PKA signaling in human myometrial tissue in organ and cell culture. Functionally, these IP-dependent changes in gene expression promoted an enhanced contractile response to oxytocin in pregnant human myometrial tissue strips, which was inhibited by the IP antagonist RO3244794. Furthermore, contractile protein induction was dependent on the concentration and time of exposure to the PGI2 analog iloprost and was blocked by both RO3244794 and PKA knockdown. We therefore propose that PGI2-mediated upregulation of contractile proteins and connexin 43 is a critical step in myometrial activation, allowing for a maximal contractile response. Our observations have important implications regarding activation of the myometrium prior to the onset of labor.

Authors

Kristina M. Fetalvero, Peisheng Zhang, Maureen Shyu, Benjamin T. Young, John Hwa, Roger C. Young, Kathleen A. Martin

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Figure 3

Iloprost increases connexin 43 expression.

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Iloprost increases connexin 43 expression. Protein was isolated from hum...
Protein was isolated from human myometrial tissue in organ culture treated with vehicle or 25 nmol/l iloprost for 48 h. Left: Cell lysates were subjected to Western blot analysis with antibodies to connexin 43 (Cx43) and GAPDH. A representative blot is shown. Right: Densitometric quantitation from 5 independent experiments on samples from 5 different patients. Because connexin 43 is known to migrate as a doublet or triplet spanning the 39- to 44-kDa range, we summed the band intensities for both bands for each sample and corrected the values to the corresponding GAPDH. Results are mean ± SEM. *P < 0.05, paired 1-tailed Student’s t test.