Practice Bulletin: Management of Preterm Labor
Practice Bulletin: Management of Preterm Labor
Practice Bulletin: Management of Preterm Labor
Myasthenia gravis
loss of deep tendon reflexes,
respiratory depression, and cardiac
arrest; suppresses heart rate,
contractility and left ventricular
systolic pressure when used with
calcium channel blockers; and
produces neuromuscular blockade
when used with calcium-channel
blockers
*Greatest risk associated with use for longer than 48 hours.
The use of magnesium sulfate in doses and duration for fetal neuroprotection alone does not appear to be associated with an increased risk of neonatal depression
when correlated with cord blood magnesium levels (Johnson LH, Mapp DC, Rouse DJ, Spong CY, Mercer BM, Leveno KJ, et al. Association of cord blood magnesium
concentration and neonatal resuscitation. Eunice Kennedy Shriver National Institute of Child Health and Human Development Maternal-Fetal Medicine Units Network.
J Pediatr 2011;DOI: 10.1016/j.jpeds.2011.09.016.).
Modified from Hearne AE, Nagey DA. Therapeutic agents in preterm labor: tocolytic agents. Clin Obstet Gynecol 2000;43:787801.
1312 Practice Bulletin Management of Preterm Labor OBSTETRICS & GYNECOLOGY
Is there a role for nonpharmacologic man-
agement of women with preterm contractions
or preterm labor?
The assessment of preterm delivery risk based on symp-
toms and physical examination alone is inaccurate (17,
76, 77). Previously, when symptoms of possible preterm
labor were present, clinicians recommended reduced
maternal activity and hydration with or without seda-
tives, with the aim of reducing uterine activity. Most
experts advocated awaiting cervical dilation or efface-
ment before administering tocolytic drugs. However,
prophylactic therapy (tocolytic drugs, bed rest, hydra-
tion, and sedation) in asymptomatic women at increased
risk of preterm delivery has not been demonstrated to be
effective (38, 78). Although bed rest and hydration have
been recommended to women with symptoms of preterm
labor to prevent preterm delivery, these measures have
not been shown to be effective for the prevention of
preterm birth and should not be routinely recommended.
Furthermore, the potential harm, including venous throm-
boembolism, bone demineralization, and deconditioning,
and the negative effects, such as loss of employment,
should not be underestimated (1316, 79, 80).
Is preterm labor managed differently in
women with multiple gestations?
The use of tocolytics to inhibit preterm labor in multiple
gestations has been associated with a greater risk of
maternal complications, such as pulmonary edema (81,
82). In addition, prophylactic tocolytics have not been
shown to reduce the risk of preterm birth or improve
neonatal outcomes in women with multiple gestations
(8386). Adequate data do not exist to specifically dem-
onstrate benefit from the use of antenatal corticosteroids
in multiple gestations. However, because of the clear
benefit attributable to the use of antenatal corticosteroids
in singleton gestations, most experts recommend their
use in preterm multiple gestations. Similar extrapolation
could also apply to the use of magnesium sulfate for fetal
neuroprotection in multiple gestations.
Summary of
Recommendations
The following recommendations and conclusions
are based on good and consistent scientific evi-
dence (Level A):
A single course of corticosteroids is recommended
for pregnant women between 24 weeks of gestation
to short-term inpatient use as a tocolytic or for the acute
antepartum therapy of uterine tachysystole.
Should tocolytics be used after acute therapy?
Maintenance therapy with tocolytics is ineffective for
preventing preterm birth and improving neonatal out-
comes and is not recommended for this purpose. A
meta-analysis has not shown any differences between
magnesium sulfate maintenance therapy and either pla-
cebo or beta-adrenergic receptor agonists in preventing
preterm birth after an initial treated episode of threatened
preterm labor (66). Likewise, maintenance beta-agonist
therapy has not been demonstrated to prolong pregnancy
or prevent preterm birth and should not be used for this
purpose (67). The FDA posted warnings specifically
cautioning against the use of maintenance oral terbu-
taline during pregnancy (64). Because of the lack of
efficacy and potential maternal risk, the FDA states that
oral terbutaline should not be used at all to treat preterm
labor. Injectable terbutaline may be used only in an inpa-
tient, monitored setting but should not be used for longer
than 4872 hours (64). When compared with placebo,
maintenance tocolysis with nifedipine does not appear
to confer a reduction in preterm birth or improvement in
neonatal outcomes (68). Atosiban is the only tocolytic
that has demonstrated superiority as maintenance ther-
apy over placebo in prolonging pregnancy, but atosiban
is not available in the United States (69).
Is there a role for antibiotics in preterm labor?
Intrauterine bacterial infection is an important cause of
preterm labor, particularly at gestational ages less than
32 weeks (70, 71). It has been theorized that infection
or inflammation are associated with contractions. Based
on this concept, the utility of antibiotics to prolong preg-
nancy and reduce neonatal morbidity in women with
preterm labor and intact membranes has been evaluated
in numerous randomized clinical trials. However, most
have failed to demonstrate antibiotic benefit; a meta-
analysis of eight randomized controlled trials that com-
pared antibiotic treatment with placebo for patients with
documented preterm labor found no difference between
the antibiotic treatment and placebo for prolonging
pregnancy or preventing preterm delivery, respiratory
distress syndrome, or neonatal sepsis (55). In fact, anti-
biotic use may be associated with long-term harm (72).
Thus, antibiotics should not be used to prolong gestation
or improve neonatal outcomes in women with preterm
labor and intact membranes. This recommendation is
distinct from recommendations for antibiotic use for pre-
term premature rupture of membranes (73) and group B
streptococci carrier status (74, 75).
VOL. 119, NO. 6, JUNE 2012 Practice Bulletin Management of Preterm Labor 1313
and 34 weeks of gestation who are at risk of preterm
delivery within 7 days.
Accumulated available evidence suggests that magne-
sium sulfate reduces the severity and risk of cerebral
palsy in surviving infants if administered when birth
is anticipated before 32 weeks of gestation. Hospitals
that elect to use magnesium sulfate for fetal neuropro-
tection should develop uniform and specific guide-
lines for their departments regarding inclusion criteria,
treatment regimens, concurrent tocolysis, and moni-
toring in accordance with one of the larger trials.
The evidence supports the use of first-line tocolytic
treatment with beta-adrenergic agonist therapy, cal-
cium channel blockers, or NSAIDs for short-term
prolongation of pregnancy (up to 48 hours) to allow
for the administration of antenatal steroids.
Maintenance therapy with tocolytics is ineffective
for preventing preterm birth and improving neonatal
outcomes and is not recommended for this purpose.
Antibiotics should not be used to prolong gestation
or improve neonatal outcomes in women with pre-
term labor and intact membranes.
The following recommendations and conclusions
are based on limited and inconsistent scientific
evidence (Level B):
A single course of repeat antenatal corticosteroids
should be considered in women whose prior course
of antenatal corticosteroids was administered at
least 7 days previously and who remain at risk of
preterm birth before 34 weeks of gestation.
Bed rest and hydration have not been shown to be
effective for the prevention of preterm birth and
should not be routinely recommended.
The positive predictive value of a positive fetal
fibronectin test result or a short cervix alone is poor
and should not be used exclusively to direct man-
agement in the setting of acute symptoms.
Proposed Performance
Measure
The proportion of women with preterm labor at less than
34 weeks of gestation who receive corticosteroid therapy
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Br J Obstet Gynaecol 1990;97:87882. (Level I)
86. Yamasmit W, Chaithongwongwatthana S, Tolosa JE,
Limpongsanurak S, Pereira L, Lumbiganon P. Prophylactic
oral betamimetics for reducing preterm birth in women
with a twin pregnancy. Cochrane Database of Systematic
Reviews 2005, Issue 3. Art. No.: CD004733. DOI: 10.1002/
14651858.CD004733.pub2. (Meta-analysis)
VOL. 119, NO. 6, JUNE 2012 Practice Bulletin Management of Preterm Labor 1317
The MEDLINE database, the Cochrane Library, and the
American College of Obstetricians and Gynecologists
own internal resources and documents were used to con-
duct a lit er a ture search to lo cate rel e vant ar ti cles pub lished
be tween January 1990 and October 2008. The search was
re strict ed to ar ti cles pub lished in the English lan guage.
Pri or i ty was given to articles re port ing results of orig i nal
re search, although re view ar ti cles and com men tar ies also
were consulted. Ab stracts of re search pre sent ed at sym po-
sia and sci en tif ic con fer enc es were not con sid ered adequate
for in clu sion in this doc u ment. Guide lines pub lished by
or ga ni za tions or in sti tu tions such as the Na tion al In sti tutes
of Health and the Amer i can Col lege of Ob ste tri cians and
Gy ne col o gists were re viewed, and ad di tion al studies were
located by re view ing bib liographies of identified articles.
When re li able research was not available, expert opinions
from ob ste tri ciangynecologists were used.
Studies were reviewed and evaluated for qual i ty ac cord ing
to the method outlined by the U.S. Pre ven tive Services
Task Force:
I Evidence obtained from at least one prop er ly
de signed randomized controlled trial.
II-1 Evidence obtained from well-designed con trolled
tri als without randomization.
II-2 Evidence obtained from well-designed co hort or
casecontrol analytic studies, pref er a bly from more
than one center or research group.
II-3 Evidence obtained from multiple time series with or
with out the intervention. Dra mat ic re sults in un con-
trolled ex per i ments also could be regarded as this
type of ev i dence.
III Opinions of respected authorities, based on clin i cal
ex pe ri ence, descriptive stud ies, or re ports of ex pert
committees.
Based on the highest level of evidence found in the data,
recommendations are provided and grad ed ac cord ing to the
following categories:
Level ARecommendations are based on good and con-
sis tent sci en tif ic evidence.
Level BRecommendations are based on limited or in con-
sis tent scientific evidence.
Level CRecommendations are based primarily on con-
sen sus and expert opinion.
Copyright June 2012 by the American College of Ob ste t-
ri cians and Gynecologists. All rights reserved. No part of this
publication may be reproduced, stored in a re triev al sys tem,
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Requests for authorization to make photocopies should be
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The American College of Obstetricians and Gynecologists
409 12th Street, SW, PO Box 96920, Washington, DC 20090-6920
Management of preterm labor. Practice Bulletin No. 127. American
College of Obstetricians and Gynecologists. Obstet Gynecol 2012;
119:130817.