Pregnancy Clinical Trial
Official title:
Effects of Preoperative Sublingual Misoprostol on Uterine Tone During Isoflurane Anaesthesia for Caesarean Section
Misoprostol would reduce the uterine bleeding after caesarean delivery, without harmful effects on either mother or baby. The investigators postulated that the use of sublingual misoprostol during isoflurane anaesthesia for uncomplicated caesarean delivery would reduce maternal haemorrhage, uterine atonic effects, and the need for additional uterotonic agents, without harmful effects on either mother or baby. Therefore, the present study was designed to evaluate the effects of preoperative sublingual misoprostol on maternal blood loss, uterine tone, the need for additional oxytocin and neonatal outcome after elective caesarean delivery under isoflurane anaesthesia.
Volatile anaesthetics including sevoflurane, desflurane, and isoflurane are often used
during general anaesthesia for caesarean delivery. The cost effectiveness of isoflurane
anaesthesia1 for caesarean delivery is widely used at many centres including the authors'
centre, where general anaesthesia is commonly used for caesarean deliveries than did
regional anaesthesia because of the refusal of many ladies for the later, especially in the
light of evidence-based equivocal maternal or neonatal outcomes of both techniques. 2
However, isoflurane in similar to other inhalational anaesthetics have been shown a
dose-dependent (from 0.5 to 2.35 minimum alveolar concentration (MAC)) induced myometrial
relaxation in 25% of parturients with added risks of postpartum haemorrhage, 3-5 which may
be mediated through the inhibition of the oxytocin-induced contraction,6 decrease in
intracellular concentration of free calcium,7 inhibition of voltage-dependent calcium
channels activity,8 and activation of adenosine triphosphate-sensitive potassium channels (K
(ATP))9 of pregnant uterine smooth muscle.
Several uterotonics such as oxytocin reduce postpartum haemorrhage by inducing uterine
contraction, but with added risks of haemodynamic adverse effects. 10 Sublingual or rectal
misoprostol, a prostaglandin E1 analogue, in doses of 100 to 800 µg is safe and as effective
as intravenous infusion of oxytocin in reducing blood loss and the need for additional
oxytocin after caesarean delivery under either spinal or general anaesthesia, with
occurrence of transient side effects such as nausea, shivering and pyrexia. 11-17
Misoprostol possess several advantages over oxytocin, including long shelf life, stability
at room temperature, and possible buccal, rectal and sublingual administration. 11, 16The
later has many advantages such as rapid uptake, long-lasting duration of effect, and
greatest bioavailability, compared with other routes of misoprostol administration. 18 Up to
our best knowledge, this trial was the first one studied the inhibitory effects of
misoprostol on the uterine atonic effects of inhalational anaesthetics.
Based upon previous published data, 19 blood loss after caesarean delivery was normally
distributed with standard deviation 560 ml. A priori power analysis indicated that 174
patients in each group would be sufficient to detect a 20% reduction in blood loss after
caesarean delivery, with a type-I error of 0.05 and a power of 90%. The investigators added
10% more patients to account for patients dropping out during the study.
Patients were randomly allocated to receive sublingual 400 µg of misoprostol or identical
placebo two tablets after tracheal intubation before surgery.
Anaesthetic management was standardized in all studied patients. Oral ranitidine 150 mg was
given the night before and on the morning of surgery, with 0.3 mol/L sodium citrate (30 mL)
given 15 min before induction. In the operating theatre women were positioned supine on the
operating table with 15° firm rubber wedge under the right hip to effect left uterine
displacement. A slow 500-mL i.v. infusion of lactated Ringer's solution was given to all
subjects over 20 min.
Subjects were monitored with electrocardiography, non-invasive blood pressure, pulse
oximetry (SpO2), and end-tidal carbon dioxide concentration (EtCO2). After pre-oxygenation
for 5 min, rapid-sequence induction was performed with propofol 1.5-2 mg/kg followed by
suxamethonium 1.5 mg/kg after loss of verbal response. Cricoid pressure was applied after
loss of consciousness and was released after correct placement of the tracheal tube had been
confirmed.
After tracheal intubation, subjects were allocated randomly to two groups by drawing
sequentially numbered sealed opaque envelopes containing a software-generated randomisation
code (Random Allocation Software, version 1.0.0, Isfahan University of Medical Sciences,
Isfahan, Iran). The parturients in the placebo group (n = 183) received sublingual two
moistened white coated placebo tablets which looked identical in size, colour, and packing
to misoprostol tablet. In the misoprostol group (n = 183), sublingual misoprostol was given
by putting two moistened tablets of misoprostol (400 µg) under the tongue and allowing them
to dissolve (Misotac®, Sigma Pharmaceutical Industries, Egypt) (200 µg/tablet). The
anaesthesiologists who gave the anaesthetics and study tablets were blinded to the study
randomization and were not involved in collecting of the patients' data. All staff in the
operating room were unaware of the randomization code.
Anaesthesia was maintained with 0.5-1 MAC of isoflurane with nitrous oxide 50% in oxygen to
maintain the heart rate and blood pressure within 20% of baseline values. Neuromuscular
block was maintained with vecuronium 0.06 mg/kg. The lungs were ventilated using a tidal
volume of 8 mL/kg, an inspiration-expiration ratio of 1: 2, and at a respiratory rate
necessary to maintain an EtCO2 of 30-35 mm Hg. An infusion of lactated Ringer's solution 800
mL was given to all subjects during the procedure. Induction to delivery (I-D) times was
recorded using a stopwatch.
After the umbilical cord was clamped, a 10-unit infusion of oxytocin in 500 mL of 5% glucose
was started. Intravenous midazolam 0.05 mg/kg and fentanyl 2.0 µg/kg were given and
end-tidal concentration of the nitrous oxide was increased to 70%.
The obstetrician who was blinded to the study group, assessed the uterine tone by palpation
every three minutes after delivery of the placenta and rated the degree of uterine
contraction on a 10-cm VAS (0: well contracted; 10: completely relaxed). If uterine tone
remained unsatisfactory after 3 min, an additional 5-unit bolus of oxytocin was
administered.
All neonates were assessed by a paediatrician unaware of the randomisation code as regarding
their Apgar scores at 1 and 5 min, arterial blood pressure, heart rate, temperature and
arterial oxygen saturation.
At the end of surgery, isoflurane and nitrous oxide were discontinued, residual
neuromuscular block was antagonised and the patients were extubated. Postoperative analgesia
was achieved with morphine, tramadol and paracetamol.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Prevention
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