Postpartum Haemorrhage Clinical Trial
Official title:
Tranexamic Acid for the Treatment of Postpartum Haemorrhage: An International Randomised, Double Blind, Placebo Controlled Trial
The WOMAN trial is a large pragmatic randomised double-blind, placebo controlled trial to quantify the effects of the early administration of tranexamic acid on death, hysterectomy and other relevant outcomes. 20,000 adult women, after delivery who have clinically diagnosed postpartum haemorrhage, are eligible if the responsible doctor is for any reason substantially uncertain whether or not to use an antifibrinolytic agent. Additionally, TWO nested studies will be conducted in a subset of women trial participants. The first nested study (ETAC) aims to evaluate the effect of tranexamic acid (TXA) on markers of coagulation in 400 women randomised to the WOMAN trial. The second nested study (ETAPLAT) aims to evaluate the haemostatic effect and antithrombotic effect of TXA in 128 women randomised to the WOMAN trial.
BACKGROUND: Each year, worldwide about 530,000 women die from causes related to pregnancy and
childbirth. Almost all (99%) of the deaths are in low and middle income countries. Obstetric
haemorrhage is the leading cause of maternal mortality accounting for between one quarter and
one third of deaths, most of which occur in the postpartum period. About 14 million mothers
develop postpartum haemorrhage (PPH) each year and about 1-2% of them will die, with an
average interval from onset to death of about 2 to 4 hours. Obstetric haemorrhage is also an
important cause of maternal mortality in high income countries where it accounts for about
13% of maternal deaths.
Anti-fibrinolytic agents are widely used in surgery to reduce blood loss and the need for
blood transfusion. A systematic review of randomised controlled trials of anti-fibrinolytic
agents in elective surgery showed that tranexamic acid (TXA) reduced the risk of blood
transfusion by a relative 39% (RR 0.61, 95% CI 0.54 to 0.69). In those requiring transfusion,
TXA reduced the transfused blood volume by 1.1 units (95% CI 0.64 to 1.59). Anti-fibrinolytic
agents also reduced the need for re-operation due to bleeding (RR=0.52: 95% CI 0.40 to 0.69).
There was no evidence of an increased risk of thrombotic events.
TXA significantly reduces uterine blood loss in women with menorrhagia and is "recommended
for consideration" as a treatment in intractable postpartum haemorrhage in the UK. However,
at present there is little reliable evidence from randomised trials on the effectiveness of
TXA in the treatment of PPH. A systematic review of randomised trials of TXA in PPH conducted
by the applicants identified three trials of the prophylactic use of TXA, including a total
of 460 participants. Although there was a significant reduction in average postpartum blood
loss in women treated with TXA [weighted mean reduction 96 ml (95%CI 76ml to 109ml)] the
quality of the trials was poor. None had adequate allocation concealment and even in
aggregate the trials were too small to assess the effects of TXA on the clinically important
end points of mortality, hysterectomy and thrombotic side effects. The most recently updated
PPH treatment guidelines prepared by the World Health Organization (WHO) state that TXA may
be used in the treatment of PPH if other measures fail, but points out that the quality of
evidence on which this recommendation is based is low and recommends that further clinical
trials of TXA in PPH are conducted.
AIM: The WOMAN Trial aims to determine the effect of the early administration of tranexamic
acid (TXA) on death and hysterectomy in women with a clinical diagnosis of postpartum
haemorrhage. The effect of TXA on the need for surgical interventions, blood transfusion, the
risk of non-fatal vascular events (either haemorrhagic or occlusive), use of health services
and breastfeeding will also be assessed.
OUTCOME: Outcomes will be collected at 42 days after randomisation, at discharge or at death
(whichever occurs first).
TEST PRODUCT, DOSE AND MODE OF ADMINISTRATION: A first dose of Tranexamic acid (1 gram by
intravenous injection) will be given as soon as possible after randomisation. If clinically
indicated due to continued bleeding, a second dose of Tranexamic acid (1 gram by intravenous
injection) will be given if within 4 hours of randomisation.
REFERENCE THERAPY, DOSE AND MODE OF ADMINISTRATION: A placebo (sodium chloride 0.9%) matched
to the active drug will be administered in the same way as the active product. A placebo is
justified in this trial because all women with PPH will receive all other treatments
clinically indicated. Tranexamic acid/placebo will be given as an additional treatment.
SETTING: This trial will be co-ordinated from LSHTM and conducted in hospitals in low, middle
and high income countries. It is likely that most patient recruitment will be in countries
with high rates of mortality and morbidity from postpartum haemorrhage.
DURATION OF TREATMENT AND PARTICIPATION: The first dose will be given immediately after
randomisation. If required, the second dose will be given up to 24 hours after randomisation.
No further trial treatment will be given after 24 hours of randomisation. Participation will
end at discharge, death or at 42 days post randomisation whichever occurs first.
CRITERIA FOR EVALUATION: All patients randomly assigned to one of the treatments will be
analysed together, regardless of whether or not they completed or received that treatment on
an intention to treat basis.
NESTED STUDY 1: Effect of tranexamic acid on coagulation in a sample of 400 participants in
the WOMAN trial (ETAC). This aims to evaluate the effect of TXA on markers of coagulation in
a sample of WOMAN trial participants. Standard coagulation parameters (platelets, fibrinogen,
PT and aPTT time and D-dimer) and ROTEM® parameters measured after in vitro activation with
tissue factor (EXTEM) and inhibition with aprotinin (APTEM) will be determined (maximum
lysis, maximum strength [Maximal Clot Firmness (MCF)], time from start to when the waveform
reaches 2mm above baseline [Clotting Time (CT)], time from 2mm above baseline to 20mm above
baseline [Clot Formation Time (CFT)], time to lysis [CLT (10% difference from MCF)], time to
Maximum strength [MCF-t], Clot elasticity [MCE]).
NESTED STUDY 2: This aims to assess the haemostatic and antithrombotic effect of TXA in a
sample of 128 participants in the WOMAN Trial (ETAPLAT). Platelet function, thrombin
generation, fibrinogen level, D-Dimer and coagulation factors V, VIII and vWF will be
assessed.
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