Post Partum Haemorrhage Clinical Trial
Official title:
Carbetocin Versus Oxytocin in the Prevention of Post Partum Haemorrhage (PPH) in Women Undergoing Caesarean Sections for Placenta Previa: A Randomised Controlled Trial
The study aims at comparing the roles of carbetocin and oxytocin in the prevention of atonic
PPH in women undergoing CS for placenta previa.
200 women will be randomly divided into 2 equal groups using computer generated random
numbers, Group 1 will receive Carbetocin 100 µgm (Pabal® Ferring, UK) and group 2 will
receive oxytocin 5IU (Syntocinon®, Novartis, Switzerland).
Obstetric haemorrhage remains one of the major causes of maternal death in both developed
and developing countries. Postpartum haemorrhage (PPH) is defined as a blood loss >500 ml
more of blood from the genital tract within 24 hours of the birth of a baby. PPH can be
minor (500-1000 ml) or major (more than 1000 ml) . The most frequent cause of PPH is uterine
atony, contributing up to 80 % of the PPH cases.
Risk factors of atonic PPH include multiple pregnancy, placenta previa, previous PPH, body
mass index (BMI) >30, prolonged labour, fetal macrosomia>4kg and primipara> 40 years.
Placenta praevia exists when the placenta is inserted wholly or in part into the lower
segment of the uterus. It is classified by ultrasound imaging according to what is relevant
clinically: if the placenta lies over the internal cervical os, it is considered a major
praevia; if the leading edge of the placenta is in the lower uterine segment but not
covering the cervical os, minor or partial praevia exists.
Oxytocin is currently the uterotonic of first choice. It has proven to decrease the
incidence of PPH by 40 % and has a rapid onset of action and a good safety profile. A
disadvantage of oxytocin is its short half-life of 4-10 min, regularly requiring a
continuous intravenous infusion or repeated intramuscular injections.
Carbetocin is a long-acting oxytocin analogue indicated for the prevention of uterine atony
after child birth by cesarean section (CS) under epidural or spinal anaesthesia. Carbetocin
has a rapid onset of action (within 1-2 min) and a prolonged duration of action
(approximately 1 h) because of sustained uterine response with contractions of higher
amplitude and frequency. Its safety profile is comparable to that of oxytocin.
The study will be conducted in Cairo university hospitals and BeniSuef university hospitals.
All patients with placenta previa covering, or less than 2cm from the internal cervical os
will be approached in the antenatal clinic. Women will be invited to participate in the
study, the invitation will include a clear full explanation of the study. Only patients
signing informed written consents will participate in the study.
The exclusion criteria will be gestational age <37 weeks, hypertension, preeclampsia,
cardiac, renal or liver diseases, epilepsy, need for general anaesthesia, known
hypersensitivity to carbetocin and suspected placenta accreta.
200 women will be randomly divided into 2 equal groups using computer generated random
numbers, Group 1 will receive Carbetocin 100 µgm (Pabal® Ferring, UK) and group 2 will
receive oxytocin 5IU (Syntocinon®, Novartis, Switzerland). Both drugs will be diluted in
10ml saline and will be given by the anaesthetist slowly intravenously after delivery of the
baby. The investigators will not include a control group for ethical reasons.
The CS will be done in the presence of a consultant Obstetrician and a consultant
anaesthetist, cross-matched blood will be ready and a level 2 critical care bed will be
available. CS will be done through the lower uterine segment, if the placenta is
encountered, it will be pushed aside and the baby will be delivered.
The allocated drug will be diluted in 10ml saline and will be given by the anesthesist
slowly intravenously after delivery of the baby. The uterine tone and amount of bleeding
will be noted and the need for further uterotonic agents will be determined 2 minutes after
giving the drug.
Blood loss will be estimated through weighing the swabs, using pictorial charts and
estimating the amount of blood in the suction containers. Blood haemoglobin will be assessed
24 hours after the CS.
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