Prostaglandin (PG) D2, a
prostanoid known to have hypotensive effect, can evoke increased in vitro prepartum myometrial contraction resulting from up-regulation of the F
prostanoid (FP) receptor. The present study further determined postpartum rat uterine responses to
PGD2 to evaluate the possibility of the
prostanoid becoming a therapeutic for postpartum
uterine atony, a major cause of
postpartum hemorrhage that can lead to maternal morbidity. In vitro and in vivo postpartum uterine responses to
PGD2 were determined and compared to those of prepartum rats. Here we show that in postpartum myometrial strips
PGD2 did evoke a contraction sensitive to
FP receptor antagonism. Interestingly, this response was not only to a greater extent than that of prepartum rats, but also comparable with the contraction obtained with PGF2α, a therapeutic for postpartum
uterine atony but contradicted in conditions including
hypertension. Indeed,
PGD2 was also found to cause increases of basal uterine contraction under in vivo conditions. Western blots revealed that the expression of FP receptors in postpartum myometrium was higher than that of prepartum rats. Moreover, we noted that the amount of
PGD2 produced in postpartum uteri, although lower than that of prepartum rats, was increased compared to non-pregnant conditions. These results thus demonstrate that due to a further up-regulation or high expression of myometrial FP receptors,
PGD2 can evoke potent uterine contraction postpartum, and hence the
prostanoid, which is naturally synthesized in uterine tissues, could be a potential therapeutic for postpartum
uterine atony, especially in settings, such as
hypertension.