Membrane Sweeping to Prevent Post-term Pregnancy: The MILO Study

Not Applicable

• Conditions: Pregnancy, Prolonged; Induced; Birth; Pregnancy Related
• Interventions: Procedure: Amniotic membrane sweep

• Registration Number: NCT04307199
• Lead Sponsor: National University of Ireland, Galway, Ireland

Brief Summary

Multicentre, pragmatic, parallel group, pilot randomised controlled trial with an embedded factorial design.

Detailed Description

The primary aim of the MILO study is to inform the optimal design of a future definitive randomised trial to evaluate the effectiveness (including optimal timing and frequency) of membrane sweeping to prevent post-term pregnancy. We will also assess the acceptability and feasibility of the proposed trial interventions to clinicians and women (through focus group interviews).

Methods/Design

Multicentre, pragmatic, parallel group, pilot randomised controlled trial with an embedded factorial design. Pregnant women with a live, singleton fetus ≥ 38 weeks gestation, cephalic presentation, longitudinal lie, intact membranes, English speaking and ≥18 years of age will be randomised in a 2:1 ratio to:

• Membrane sweep versus no membrane sweep

Women allocated randomly to a sweep will then be randomised further (factorial component) to:

* early (from 39 weeks) versus late (from 40 weeks) sweep commencement; and

* a single verses weekly sweep

The proposed feasibility study consists of four work packages i.e., (1) a multicentre, pilot randomised trial, 2) a health economic analysis and 3) a qualitative study (4) a study within the host trial (a SWAT).

Study Timeline

• Study First Submitted: 2020-01-17
• Study First Submitted QC: 2020-03-10
• Study First Posted: 2020-03-13
• Status Verified: 2020-05
• Last Update Submitted: 2020-05-12
• Last Update Posted: 2020-05-14
• Study Start: 2020-07-30
• Primary Completion: 2021-03-30
• Study Completion: 2021-12-30

Recruitment & Eligibility

• Status: UNKNOWN
• Sex: Female
• Target Recruitment: 132

Inclusion Criteria

• Pregnant women carrying a live singleton fetus ≥ 38 weeks completed gestation.
• (Gestational age will be calculated from the first day of the last menstrual period and an
• ultrasound examination carried out in the 2nd trimester)
• Longitudinal lie
• Cephalic presentation
• Intact amniotic
• ≥ 18 years of age on enrollment

Exclusion Criteria

• Not able to communicate in english
• contraindications to a vaginal examination
• contraindications to a vaginal birth

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: FACTORIAL

Arm && Interventions

Group	Intervention	Description
Group A	Amniotic membrane sweep	Membrane sweep @ 39 weeks' gestation only
Group C	Amniotic membrane sweep	Membrane sweep @ 39, 40 and 41 weeks' gestation or until onset of labour
Group D	Amniotic membrane sweep	Membrane sweep @ 40 and 41 weeks' gestation or until onset of labour
Group B	Amniotic membrane sweep	Membrane sweep @ 40 weeks' gestation only

Primary Outcome Measures

Name	Time	Method
Adherence with the trial interventions.	At month 15 approximately	Evaluation of adherence with the trial interventions, and reasons for non-compliance assessed by study-specific checklists. Data will be extracted from routinely collected data and focus group interviews with clinicians and participants at six weeks post intervention.
Evaluation of the data collection process through study specific checklists	At month 21 approximately	Evaluated, statistically and narratively, by assessing the completeness of outcome measurements at baseline and postnatal (6 weeks) through study specific checklists. Researchers will manually examine the data collected. They will assess the proportion of complete data collection forms, the quality of data collected and the applicability of this data in facilitating pilot trial outcomes.
Evaluation of the data analysis process	At month 21 approximately	As this is a feasibility study formal hypothesis testing will not be undertaken. Researchers will manually examine the data collected. Evaluation of the data analysis process will be undertaken through the assessment of gaps and limitations to the analysis process measured by study-specific checklist. Findings will be reported through descriptive statistics and graphical summaries.
Feasibility of the cost effectiveness analyses	At month 21 approximately	Assessment of the mechanism and utilisation of the incremental cost-effectiveness ratio (ICER), through study specific checklists.
Evaluation of attrition rates	At month 15 approximately	Evaluation of attrition rates assessed by study-specific checklists. Data will be extracted from routinely collected data.
Evaluation of the types of attrition	At month 21 approximately	Evaluation of the types of attrition assessed by case report forms. Data will be extracted from routinely collected data.
Feasibility of cost analyses process through analysis of study specific documentation.	At month 21 approximately	Assessment of data collection tools to undertake cost effectiveness analysis through study specific documentation. Researchers will manually examine data to assess the mechanism of, timing of and delivery of the cost analysis tools.
Evaluation of the EQ5D	At month 21 approximately	Assessment of the mechanism of, timing of and delivery of the EQ5D through study specific checklists.
Recruitment	Duration of the recruitment process (approximately 8 months )	Evaluation of the number and percentage of eligible women who are recruited and randomised to the study. Assessed by study-specific checklists.
Retention	At month 15 approximately	Evaluation of the number and percentage of eligible women who are randomised, take part in and adhere to the study protocols. Data will be extracted from routinely collected data.
Evaluation of the randomisation process.	At month 15 approximately	Evaluation of effective allocation of participants to the intervention/control group assessed by study-specific checklists and evaluation of the randomisation protocol throughout the randomisation period.
Estimate the main effect of individual intervention components and their interactions	At month 21 approximately	Estimates (with measures of uncertainty) of the main effect of individual intervention components and any interaction effect between the main effects of the embedded factorial design will be assessed and reported using regression analysis.

Secondary Outcome Measures

Name	Time	Method
Number of participants achieving a spontaneous vaginal birth	From time of randomisation to birth of baby (up to 5 weeks)	Spontaneous vaginal birth
Caesarean Section	From time of randomisation to birth of baby (up to 5 weeks)	Birth which is achieved through the surgical procedure caesarean section.
Uterine hyperstimulation with/without fetal heart rate (FHR) changes	From time of randomisation to birth of baby (up to 5 weeks)	Uterine hyperstimulation defined as uterine tachysystole (more than five contractions per ten minutes for at least twenty minutes) and uterine hypersystole/hypertonicity (a contraction lasting at least two minutes). These may or not be associated with changes in the fetal heart rate pattern (persistent decelerations, tachycardia or decreased short term variability.
Uterine rupture	From time of randomisation to birth of baby (up to 5 weeks)	All clinically significant ruptures of unscarred or scarred uteri. Trivial scar dehiscence noted incidentally at the time of surgery will be excluded
Admission to neonatal intensive care unit or equivalent	From time of birth to six weeks postnatal.	Admission of infant to neonatal intensive care unit or equivalent
Length of time from membrane sweep to birth of baby.	From time of membrane sweep to birth of baby (up to 4 weeks)	Length of time from membrane sweep to birth of baby .
Number of participants who underwent an induction of labour	From time of randomisation to commencement of formal induction of labour (up to 5 weeks).	Formal induction of labour using pharmacological or surgical methods.
Epidural analgesia	From time of randomisation to birth of baby (up to 5 weeks)	Introduction of a local anaesthetic into the epidural space of the vertebral canal.
Perinatal death	From time of randomisation to seven completed days after birth of baby (up to 6 weeks)	The perinatal period is defined as "commences at 22 completed weeks (154 days) of gestation and ends seven completed days after birth of baby."
Neonatal encephalopathy	From time of birth to six weeks postnatal.	Severity of hypoxic ischaemic encephalopathy assessed using Sarnat staging; i)Stage 1 (mild): hyper-alertness, hyper-reflexia, dilated pupils, tachycardia, absence of seizures; ii)Stage 2 (moderate): lethargy, hyper-reflexia, miosis, bradycardia, seizures, hypotonia with weak suck and Moro reflexes; iii)Stage 3 (severe): stupor, flaccidity, small to mid-position pupils which react poorly to light, decreased stretch reflexes, hypothermia and absent Moro reflex.
Length of time from formal induction of labour to birth of baby.	From time of formal induction of labour to birth of baby (up to 2 weeks)	Length of time from formal induction of labour to birth of baby.
Post-Partum Haemorrhage ≥ 500mls	From time of birth to 24 hours after the birth of baby.	Blood loss ≥ 500mls within the first 24 hours of the birth of a baby
Antepartum haemorrhage requiring hospital admission	From 24+0 weeks of pregnancy to birth of baby (up to 18 weeks)	Bleeding from the genital tract, from 24+0 weeks of pregnancy and before the birth of the baby.
Augmentation of labour	From commencement of established labour to birth of baby (up to 2 days)	The stimulation of uterine contractions using pharmacologic methods or artificial rupture of membranes to increase their frequency and/or strength following the onset of spontaneous labor or contractions following spontaneous rupture of membranes (ACOG 2014)
Pyrexia in labour	From commencement of established labour to birth of baby (up to 2 days)	Pyrexia that developed anytime after onset of labour.
Number of participants achieving a spontaneous onset of labour	From time of randomisation to commencement of spontaneous onset of labour or formal induction of labour or caesarean section (up to 5 weeks)	Labour which begins spontaneously.
Instrumental birth	From time of randomisation to birth of baby (up to 5 weeks)	Vaginal birth which is assisted with the use of instruments.
Serious maternal death or morbidity	From time of randomisation to six weeks postnatal (up to 11 weeks).	Serious maternal death or morbidity (e.g. uterine rupture, admission to intensive care unit, septicaemia)
EQ5D-5L	From time of randomisation to six weeks postnatal (up to 11 weeks)	EuroQol EQ5D-5L survey instrument.
Serious neonatal morbidity	From time of birth of baby to six weeks postnatal.	e.g. seizures, birth asphyxia defined by trialists, neonatal encephalopathy, disability in childhood, Proven and suspected neonatal sepsis
Apgar score < 7 at five minutes.	From birth of baby to five minutes of life.	The Apgar score provides an accepted and convenient method for reporting the status of the newborn infant immediately after birth and the response to resuscitation if needed (ACOG 2015).
Cord PH < 7.20	From birth of infant to collection of cord bloods after delivery of the placenta (an average of 15 minutes)	Umbilical cord blood gas test.
Length of infant stay in neonatal intensive care unit or equivalent	From time of birth to six weeks postnatal.	Length of infant stay in neonatal intensive care unit or equivalent
Overall length of maternal hospital stay	From time of randomisation to six weeks postnatal (up to 11 weeks).	Overall length of maternal hospital stay