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Key messages

  • Management should be planned on an individual basis with careful consideration of risk factors and the woman's informed choices.
  • Digital examination should be avoided in the absence of good contractions, as this increases the risk of infection.
  • Intrapartum antibiotic prophylaxis is indicated for ROM >/= 18hrs.
  • The benefit of oral antibiotic prophylaxis prior to spontaneous labour or induction is unclear.
  • Women who are GBS positive should be given parenteral antibiotics and offered induction of labour as soon as possible.
  • Management as an outpatient may be considered in the absence of risk factors and in accordance with the woman's wishes.
  • If chorioamnionitis is suspected, ensure the placenta is sent for histopathological examination.
On this page

    In June 2023, we commenced a project to review and update the Maternity and Neonatal eHandbook guidelines, with a view to targeting completion in 2024. Please be aware that pending this review, some of the current guidelines may be out of date. In the meantime, we recommend that you also refer to more contemporaneous evidence.

    Approximately eight per cent of term pregnancies are complicated by rupture of membranes (ROM) before the onset of labour, with 60 per cent of these women labouring spontaneously within 24 hours.

    Risk factors associated with pre-labour rupture of membranes (PROM) include:

    • infection of the urogenital tract
    • cigarette smoking
    • illicit drug use in pregnancy
    • previous PROM or preterm birth
    • polyhydramnios
    • antepartum haemorrhage (APH).

    However, PROM often occurs in the absence of any known risk factors.

    Management of PROM may be expectant or active. The decision to manage PROM actively or expectantly must be made in consideration of any risk factors, the ability of the service to provide a safe level of care, and the woman's wishes.

    Complications of PROM

    • Infection (2-3 per cent, in the absence of risk factors, for mothers and babies)
    • Placental abruption
    • Umbilical cord prolapse or cord compression
    • Respiratory distress syndrome in the newborn.

    Assessment of PROM

    Link to: Term PROM QRA

    On the telephone

    Careful history taking is essential to determine the possibility of PROM and assess the presence of any complicating risk factors. This assessment is often done over the phone.

    Ask these questions:

    • What time did the membranes rupture?
    • What is the volume, colour and odour of the fluid on the woman's pad (if applicable)?
    • Does the woman feel unwell?
    • Is the baby is moving normally?
    • Does the woman know how her baby was presenting at the last antenatal visit?
    • Has she had any medical problems in her pregnancy?
    • Does she know her GBS status?
    • Is this a singleton pregnancy?
    • Has the woman had a previous caesarean section?

    In the absence of risk factors, advise the woman to present for assessment within 12 hours of ROM.

    If there are any risk factors, advise her to present for assessment as soon as she can attend hospital, without unnecessary delay.

    She should tell her midwife or doctor if contractions begin.

    On presentation

    • Perform a general and obstetric examination.
    • Confirm the presence of liquor on the woman's pad, if relevant.
    • If no evidence of liquor is present, a sterile speculum examination may be indicated.
    • If no liquor is visualised during the speculum examination, a diagnostic tool such as the Amnisure can be used.
    • If no liquor is visualised and no diagnostic tools are available, admit the woman for ongoing observation and continue pad checks to confirm or rule out ROM.
    • Electronic fetal monitoring to assess fetal wellbeing.

    Risk factors that may complicate management of PROM

    • GBS positive in this pregnancy - GBS prevention for neonates - Neonatal eHandbook
    • Previous birth of a baby affected by GBS disease
    • Evidence of infection
    • Meconium stained liquor
    • Abnormal CTG
    • Malpresentation
    • Previous caesarean section
    • History of cervical suture

    Management

    Link to: Term PROM QRA

    Deciding between active and expectant management of PROM depends on identified risk factors, health service capacity and the woman's preference.

    Active management is associated with lower risks of maternal and neonatal sepsis and lower rates of newborn admissions to special care nurseries.

    Table 1. Risk of sepsis associated with active and expectant management of PROM*

      Early onset neonatal sepsis Maternal chorioamnionitis or endometritis
    Active management 12 per 1000 1.2% 54 per 1000 5.4%
    Expectant management 22 per 1000 2.2% 110 per 1000 11%

    * Data from the 2017 Cochrane Review - Quality of evidence (GRADE) identified as lowTable 1. Risk of sepsis associated with active and expectant management of PROM*

    Active management

    Active management is recommended for women with any risk factors and for those women who prefer this option.

    If the woman is GBS positive, IV antibiotics should be commenced immediately and IOL commenced as soon as possible.

    Commencement of active management may be affected by the health service's capacity to safely provide 1:1 midwifery care.

    Oxytocin induction is advised for IOL - See Induction of labour.

    Expectant management

    In the absence of any complicating risk factors, women may be offered the option of expectant management. This may be as an inpatient or, if appropriate (based on individual circumstances such as travel requirements and support), at home.

    The benefit of oral antibiotic prophylaxis prior to spontaneous labour or induction is unclear. For services who choose to offer oral antibiotic prophylaxis, the following regimen is appropriate:

    • Amoxycillin 500mg TDS, from 18 hours post-ROM until commencement of intrapartum antibiotics.

    Download a patient information sheet

    Practice points

    • Discuss the management plan with the woman and her support person or family.
    • Advise four-hourly observations of temperature, PV loss, fetal movement and uterine activity (during waking hours).
    • Ensure the woman understands normal and abnormal parameters and knows to report any abnormal observations.
    • Advise the woman to avoid vaginal intercourse.
    • Admit for active management if labour is not established by 24 hours after ROM - See IOL eHandbook page.
    • Intrapartum antibiotic prophylaxis is indicated for ROM >/= 18 hours:
      • women admitted in labour <18hrs post-ROM - commence antibiotic prophylaxis 18 hours after ROM
      • women admitted >/= 18hrs post-ROM - commence intrapartum antibiotics on admission

    Antibiotics

    Antibiotics for GBS+ or ROM>18 hours

    • IV Benzylpenicillin 3g loading dose
      then
    • IV Benzylpenicillin 1.8g every four hours

     

    If the woman has a penicillin hypersensitivity with no history of anaphylaxis

    • IV Cephazolin 2g loading dose
      then
    • IV Cephazolin 1g every eight hours

    If the woman has a penicillin allergy with history of anaphylaxis

    • IV Clindamycin 900mg every eight hours

    Antibiotics for suspected sepsis/chorioamnionitis

    • IV Amoxycillin 2 g loading dose, continuing 1 g every six hours

    AND

    • IV Gentamycin 5 mg/kg daily

    AND

    • IV Metronidazole 500 mg every 12 hours

    If the woman has a penicillin allergy

    • IV Clindamycin 900 mg every 8 hours

    Postpartum management

    • If chorioamnionitis is suspected, ensure the placenta is sent for histopathological examination.

    See the Neonatal eHandbook Neonatal sepsis strategies flowchart.

    Babies born to well women and who are not symptomatic of infection

    • Routine observations for 12-24 hours post birth as per the VICTOR Newborn chart or your maternity service's schedule of observations
       

    Practice note: 95 per cent of neonates who become symptomatic of infection will do so within 24 hours.

    Babies born to women who have not received adequate antibiotic cover

    Signs of neonatal sepsis:

    • Paediatric assessment
    • FBE, blood cultures, CRP
    • Antibiotics
    • Early CRP may need to be repeated at 6-12 hours
    • Observe in hospital for 24-48 hours

    No signs of neonatal sepsis:

    • Observe in hospital for 24-48 hours

    Observations:

    • As per local guidance
    • Document on health service observation and response charts or VICTOR Newborn charts (where applicable)

    Babies who are symptomatic of infection

    • Perform septic work up and commence antibiotics - Sepsis in neonates - Neonatal eHandbook.
    • These babies require continuous monitoring and should be managed in a facility with the capacity to provide this service.

    More information

    Audit and performance improvement

    All maternity services should have processes in place for:

    • auditing clinical practice and outcomes
    • providing feedback to clinicians on audit results
    • addressing risks, if identified
    • implementing change, if indicated.

    Potential auditable standards for PROM include:

    • rates of expectant management
    • rates of maternal and neonatal sepsis
    • SCN/NICU admission after PROM
    • maternal and neonatal readmission for sepsis
    • adherence to standards of care.

    For further information or assistance with auditing, please contact us.

    References

    Definitions and abbreviations

    Active management Planned intervention to precipitate birth within 24 hours of PROM
    APH Antepartum haemorrhage
    CTG Cardiotocograph
    Expectant management No planned intervention to precipitate birth within 24 hours of PROM
    GBS Group B Streptococcus
    IOL Induction of Labour
    Latency The period of time between ROM and the establishment of labour
    PROM Pre-labour rupture of membranes - not in established labour after a latent period of 4 hours following confirmed ROM
    ROM Rupture of membranes
    SROM Spontaneous rupture of membranes
    Term ≥ 37+0 weeks gestation

    Get in touch

    Clinical Guidance Team
    Safer Care Victoria

    Version history

    First published: August 2017
    Last web update: May 2018
    Due for review by: March 2021

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