Postpartum Hemorrhage Clinical Trial
Official title:
The Relaxant Effect of Nitroglycerin on Oxytocin Desensitized Human Myometrium and the Return of Contractility on Re-exposure to Oxytocin- an in Vitro Study
Oxytocin causes myometrial contraction via the oxytocin receptor (OTR). Desensitization of
the OTR after exposure to oxytocin has been demonstrated in previous studies. The resultant
need for a higher oxytocin dose to cause adequate uterine contraction in vivo has also been
demonstrated in laboring women having received oxytocin for labor augmentation.
Achieving rapid uterine relaxation can be invaluable for maternal and fetal wellbeing in some
acute obstetric emergency settings. Nitroglycerin has become a commonly used agent for
achieving rapid uterine relaxation amongst obstetric anesthesiologists.
Previous studies have concluded that oxytocin can be used to re-establish uterine tone
following nitroglycerin mediated relaxation. However, no studies to date have looked at the
effects of nitroglycerin mediated relaxation of uterine muscle that has undergone oxytocin
receptor desensitization. Nor has the response to oxytocin re-exposure and return of
contractility in desensitized myometrium (following nitroglycerin) been examined.
The investigators hypothesize that nitroglycerin will reduce and inhibit uterine contractions
in both oxytocin pre-treated myometrium, as well as untreated myometrium in a dose dependent
fashion, but that myometrium that has undergone OTR desensitization will require less
nitroglycerin for contractions to abate.
The investigators also expect that the dose of oxytocin required to re-establish equivalent
contractions will be higher in the myometrial samples which have undergone nitroglycerin
mediated relaxation.
Oxytocin and nitroglycerin have opposing actions on the myometrium. The pharmacological
properties of quick onset and offset of action of nitroglycerin have made this the preferred
drug to be used in acute scenarios where uterine relaxation is necessary.
As nitroglycerin causes changes to intracellular calcium levels and the ability uterine
muscle to engage in effective contraction, it is plausible that the effects of nitroglycerin
may interfere with subsequent uterine contractility and action of oxytocin.
The situation where a difficult fetal extraction is encountered at cesarean section may be in
two broad groups of patients. Those pre-exposed to oxytocin and those with an oxytocin naïve
myometrium. Given the large observational variation in dosages of nitroglycerin usage seen in
the literature we feel it is vital to investigate whether pre-exposure to oxytocin impacts on
the ability of nitroglycerin to relax uterine smooth muscle. Furthermore, once the uterus has
relaxed following nitroglycerin exposure, is there a need for higher doses of oxytocin to be
administered in order to re-engage the uterus in effective contraction? And is this
requirement further exacerbated by the phenomenon of oxytocin receptor desensitization? These
clinically important questions will be addressed by the design of this in vitro myometrial
study.
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