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Tocolysis for Women
in Preterm Labour
Green-top Guideline
RCOG, 2011
Prof Aboubakr Elnashar
Aboubakr Elnashar
Use of a tocolytic drug is associated with a
prolongation of pregnancy for up to 7 days but with
no significant effect on preterm birth and no clear
effect on perinatal or neonatal morbidity.
There is no clear evidence that tocolytic drugs
improve outcome and therefore it is reasonable not
to use them.
However, tocolysis should be considered if the few
days gained would be put to good use, such as
completing a course of corticosteroids or in utero
transfer.
Aboubakr Elnashar
Use of a tocolytic drug is not associated with a
clear reduction in perinatal or neonatal mortality, or
neonatal morbidity.
Aboubakr Elnashar
Tocolysis may be considered for women with
suspected preterm labour who have had an
otherwise uncomplicated pregnancy.
It is reasonable not to use any tocolytic drug.
Women most likely to benefit from use of a
tocolytic drug are those who are in
very preterm labour,
those needing transfer to a hospital which can
provide neonatal intensive care and
those who have not yet completed a full course of
corticosteroids.
Tocolysis should not be used where there is a
contraindication to prolonging pregnancy.
Aboubakr Elnashar
Nifedipine and atosiban have comparable
effectiveness in delaying birth for up to 7 days.
Compared with beta-agonists, nifedipine is
associated with improvement in neonatal outcome,
although there are no long-term data.
Aboubakr Elnashar
Beta-agonists have a high frequency of adverse
effects.
Nifedipine, atosiban and the COX inhibitors have
fewer types of adverse effects, and they occur less
frequently than for beta-agonists but how they
compare with each other is unclear.
Using multiple tocolytic drugs appears to be
associated with a higher risk of adverse effects and
so should be avoided.
Aboubakr Elnashar
The comparative effects for the baby of
alternative drugs are unclear. Most drugs have
been compared with beta-agonists.
There are insufficient data on long-term follow-up
for reliable conclusions about the effects on the
baby for any of these tocolytic drugs.
Aboubakr Elnashar
Dose of nifedipine:
an initial oral dose of 20 mg followed by 10–20 mg
three to four times daily, adjusted according to
uterine activity for up to 48 hours.
A total dose above 60 mg appears to be
associated with a three- to four-fold increase in
adverse events.
Dose of atosiban
an initial bolus dose of 6.75 mg over 1 minute,
followed by an infusion of 18 mg/hour for 3 hours,
then 6 mg/hour for up to 45 hours (to a maximum
of 330 mg).
Aboubakr Elnashar
Cost effectiveness has not been reported but the
purchase price of atosiban is nearly ten times that
of nifedipine.
Aboubakr Elnashar
There is insufficient evidence for any firm
conclusions about whether or not tocolysis leads
to any benefit in preterm labour in multiple
pregnancy.
Aboubakr Elnashar
There is insufficient evidence for any firm
conclusions about whether or not maintenance
tocolytic therapy following threatened preterm
labour is worthwhile. Thus, maintenance therapy is
not recommended.
Aboubakr Elnashar
Summary
Use of a tocolytic drug is not associated with a
clear reduction in perinatal or neonatal mortality or
neonatal morbidity.
The main effect of tocolytic drugs when used for
women in preterm labour is to reduce the numbers
who deliver within 48 hours or within 7 days of
commencing the drug.
Aboubakr Elnashar
Data on long-term outcome are sparse. It
remains plausible that, for selected women, such
as those who require transfer for neonatal care or
time to complete a course of corticosteroids, there
may be benefit associated with tocolysis. However,
this benefit has not been formally evaluated in
randomised trials.
Aboubakr Elnashar
If reliable prediction of which women in suspected
preterm labour are likely to have a preterm birth
were possible, the use of tocolysis could be
reserved for these women. Unfortunately, few tests
offer useful predictive value. Fetal fibronectin has
been advocated as a promising predictive test but it
may have limited accuracy in predicting preterm
birth within 7 days for women with symptoms of
preterm labour.
Aboubakr Elnashar
Ultrasound assessment of cervical length is also
a promising predictive test for symptomatic women.
It remains unclear whether any predictive test, or
combination of tests, is sufficiently accurate to be
cost effective.
Aboubakr Elnashar
If the decision is made to use a tocolytic drug,
nifedipine and atosiban appear to have comparable
effectiveness in delaying delivery, with fewer
maternal adverse effects and less risk of rare
serious adverse events than alternatives such as
ritodrine or indomethacin.
There is limited evidence that use of nifedipine,
rather than a beta-agonist, is associated with
improved short-term neonatal outcome. There is
little information about the long-term growth and
development of the child for any of the drugs.
Aboubakr Elnashar
Ritodrine and atosiban are licensed in the UK for
the treatment of threatened preterm labour.
Although the use of nifedipine for preterm labour is
an unlicensed indication, it has the advantages of
oral administration and a low purchase price.
Aboubakr Elnashar
Thanks
Aboubakr Elnashar

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Tocolysis for preterm labour: RCOG Guidelines

  • 1. Tocolysis for Women in Preterm Labour Green-top Guideline RCOG, 2011 Prof Aboubakr Elnashar Aboubakr Elnashar
  • 2. Use of a tocolytic drug is associated with a prolongation of pregnancy for up to 7 days but with no significant effect on preterm birth and no clear effect on perinatal or neonatal morbidity. There is no clear evidence that tocolytic drugs improve outcome and therefore it is reasonable not to use them. However, tocolysis should be considered if the few days gained would be put to good use, such as completing a course of corticosteroids or in utero transfer. Aboubakr Elnashar
  • 3. Use of a tocolytic drug is not associated with a clear reduction in perinatal or neonatal mortality, or neonatal morbidity. Aboubakr Elnashar
  • 4. Tocolysis may be considered for women with suspected preterm labour who have had an otherwise uncomplicated pregnancy. It is reasonable not to use any tocolytic drug. Women most likely to benefit from use of a tocolytic drug are those who are in very preterm labour, those needing transfer to a hospital which can provide neonatal intensive care and those who have not yet completed a full course of corticosteroids. Tocolysis should not be used where there is a contraindication to prolonging pregnancy. Aboubakr Elnashar
  • 5. Nifedipine and atosiban have comparable effectiveness in delaying birth for up to 7 days. Compared with beta-agonists, nifedipine is associated with improvement in neonatal outcome, although there are no long-term data. Aboubakr Elnashar
  • 6. Beta-agonists have a high frequency of adverse effects. Nifedipine, atosiban and the COX inhibitors have fewer types of adverse effects, and they occur less frequently than for beta-agonists but how they compare with each other is unclear. Using multiple tocolytic drugs appears to be associated with a higher risk of adverse effects and so should be avoided. Aboubakr Elnashar
  • 7. The comparative effects for the baby of alternative drugs are unclear. Most drugs have been compared with beta-agonists. There are insufficient data on long-term follow-up for reliable conclusions about the effects on the baby for any of these tocolytic drugs. Aboubakr Elnashar
  • 8. Dose of nifedipine: an initial oral dose of 20 mg followed by 10–20 mg three to four times daily, adjusted according to uterine activity for up to 48 hours. A total dose above 60 mg appears to be associated with a three- to four-fold increase in adverse events. Dose of atosiban an initial bolus dose of 6.75 mg over 1 minute, followed by an infusion of 18 mg/hour for 3 hours, then 6 mg/hour for up to 45 hours (to a maximum of 330 mg). Aboubakr Elnashar
  • 9. Cost effectiveness has not been reported but the purchase price of atosiban is nearly ten times that of nifedipine. Aboubakr Elnashar
  • 10. There is insufficient evidence for any firm conclusions about whether or not tocolysis leads to any benefit in preterm labour in multiple pregnancy. Aboubakr Elnashar
  • 11. There is insufficient evidence for any firm conclusions about whether or not maintenance tocolytic therapy following threatened preterm labour is worthwhile. Thus, maintenance therapy is not recommended. Aboubakr Elnashar
  • 12. Summary Use of a tocolytic drug is not associated with a clear reduction in perinatal or neonatal mortality or neonatal morbidity. The main effect of tocolytic drugs when used for women in preterm labour is to reduce the numbers who deliver within 48 hours or within 7 days of commencing the drug. Aboubakr Elnashar
  • 13. Data on long-term outcome are sparse. It remains plausible that, for selected women, such as those who require transfer for neonatal care or time to complete a course of corticosteroids, there may be benefit associated with tocolysis. However, this benefit has not been formally evaluated in randomised trials. Aboubakr Elnashar
  • 14. If reliable prediction of which women in suspected preterm labour are likely to have a preterm birth were possible, the use of tocolysis could be reserved for these women. Unfortunately, few tests offer useful predictive value. Fetal fibronectin has been advocated as a promising predictive test but it may have limited accuracy in predicting preterm birth within 7 days for women with symptoms of preterm labour. Aboubakr Elnashar
  • 15. Ultrasound assessment of cervical length is also a promising predictive test for symptomatic women. It remains unclear whether any predictive test, or combination of tests, is sufficiently accurate to be cost effective. Aboubakr Elnashar
  • 16. If the decision is made to use a tocolytic drug, nifedipine and atosiban appear to have comparable effectiveness in delaying delivery, with fewer maternal adverse effects and less risk of rare serious adverse events than alternatives such as ritodrine or indomethacin. There is limited evidence that use of nifedipine, rather than a beta-agonist, is associated with improved short-term neonatal outcome. There is little information about the long-term growth and development of the child for any of the drugs. Aboubakr Elnashar
  • 17. Ritodrine and atosiban are licensed in the UK for the treatment of threatened preterm labour. Although the use of nifedipine for preterm labour is an unlicensed indication, it has the advantages of oral administration and a low purchase price. Aboubakr Elnashar