Biophysical Profile For Fetal Assessment in High R
Biophysical Profile For Fetal Assessment in High R
Biophysical Profile For Fetal Assessment in High R
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Biophysical profile for fetal assessment in high risk pregnancies
(Review)
www.cochranelibrary.com
Biophysical profile for fetal assessment in high risk pregnancies (Review)
Copyright © 2012 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd.
Cochrane Trusted evidence.
Informed decisions.
Library Better health. Cochrane Database of Systematic Reviews
TABLE OF CONTENTS
HEADER......................................................................................................................................................................................................... 1
ABSTRACT..................................................................................................................................................................................................... 1
PLAIN LANGUAGE SUMMARY....................................................................................................................................................................... 2
BACKGROUND.............................................................................................................................................................................................. 3
OBJECTIVES.................................................................................................................................................................................................. 4
METHODS..................................................................................................................................................................................................... 4
RESULTS........................................................................................................................................................................................................ 6
DISCUSSION.................................................................................................................................................................................................. 7
AUTHORS' CONCLUSIONS........................................................................................................................................................................... 7
ACKNOWLEDGEMENTS................................................................................................................................................................................ 8
REFERENCES................................................................................................................................................................................................ 9
CHARACTERISTICS OF STUDIES.................................................................................................................................................................. 11
DATA AND ANALYSES.................................................................................................................................................................................... 15
Analysis 1.1. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 1 Perinatal deaths 15
including major malformations...........................................................................................................................................................
Analysis 1.2. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 2 Apgar score < 7 at or after 16
5 minutes (all infants included)...........................................................................................................................................................
Analysis 1.3. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 3 Admission to neonatal 16
intensive care unit................................................................................................................................................................................
Analysis 1.4. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 4 Length of stay in neonatal 16
intensive care unit................................................................................................................................................................................
Analysis 1.5. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 5 Birthweight < 10th 17
centile.....................................................................................................................................................................................................
Analysis 1.6. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 6 Meconium..................... 17
Analysis 1.7. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 7 Respiratory distress 17
syndrome...............................................................................................................................................................................................
Analysis 1.8. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 8 Induction for abnormal 18
fetal assessment (biophysical profile or cardiotocograph)................................................................................................................
Analysis 1.9. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 9 Caesarean section........ 18
Analysis 1.10. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 10 Caesarean section for 18
fetal distress..........................................................................................................................................................................................
Analysis 1.11. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 11 Caesarean section for 19
intrapartum fetal distress.....................................................................................................................................................................
Analysis 1.12. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 12 Induction of labour..... 19
Analysis 2.1. Comparison 2 Biophysical profile versus conventional monitoring (CTG) - high-quality trials, Outcome 1 Apgar 19
score < 7 at or after 5 minutes.............................................................................................................................................................
Analysis 2.2. Comparison 2 Biophysical profile versus conventional monitoring (CTG) - high-quality trials, Outcome 2 Caesarean 20
section....................................................................................................................................................................................................
APPENDICES................................................................................................................................................................................................. 20
WHAT'S NEW................................................................................................................................................................................................. 21
HISTORY........................................................................................................................................................................................................ 21
CONTRIBUTIONS OF AUTHORS................................................................................................................................................................... 22
DECLARATIONS OF INTEREST..................................................................................................................................................................... 22
SOURCES OF SUPPORT............................................................................................................................................................................... 22
INDEX TERMS............................................................................................................................................................................................... 22
[Intervention Review]
1School of Nursing and Midwifery, Trinity College Dublin, Dublin, Ireland. 2Department of Obstetrics and Gynaecology, University of
Ibadan, Ibadan, Nigeria. 3Department of Women's and Children's Health, The University of Liverpool, Liverpool, UK. 4School of Nursing
and Midwifery, National University of Ireland Galway, Galway, Ireland
Contact address: Joan G Lalor, School of Nursing and Midwifery, Trinity College Dublin, 24 D'Olier Street, Dublin, 2, Ireland.
[email protected].
Citation: Lalor JG, Fawole B, Alfirevic Z, Devane D. Biophysical profile for fetal assessment in high risk pregnancies. Cochrane Database
of Systematic Reviews 2008, Issue 1. Art. No.: CD000038. DOI: 10.1002/14651858.CD000038.pub2.
Copyright © 2012 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd.
ABSTRACT
Background
A biophysical profile (BPP) includes ultrasound monitoring of fetal movements, fetal tone and fetal breathing, ultrasound assessment of
liquor volume with or without assessment of the fetal heart rate. The BPP is performed in an effort to identify babies that may be at risk
of poor pregnancy outcome, so that additional assessments of wellbeing may be performed, or labour may be induced or a caesarean
section performed to expedite birth.
Objectives
To assess the effects of the BPP when compared with conventional monitoring (CTG only or MBPP) on pregnancy outcome in high-risk
pregnancies.
Search methods
We searched the Cochrane Pregnancy and Childbirth Group's Trials Register (October 2007), CENTRAL (The Cochrane Library 2006, Issue 4),
MEDLINE (1966 to November 2006), EMBASE (1974 to November 2006) and CINAHL (1980 to November 2006).
We updated the search of the Cochrane Pregnancy and Childbirth Group's Trials Register (10 January 2012) and added the results to the
awaiting classification section.
Selection criteria
Randomised and quasi-randomised controlled trials involving a comparison of fetal BPP with other forms of antepartum fetal assessment
in women with high-risk pregnancies.
Main results
We included five trials, involving 2974 women. Most trials were not of high quality. Although the overall incidence of adverse outcomes
was low, available evidence from randomised controlled trials does not support the use of BPP as a test of fetal wellbeing in high-risk
pregnancies. We found no significant differences between the groups in perinatal deaths (relative risk (RR) 1.33, 95% confidence interval (CI)
0.60 to 2.98) or in Apgar score less than seven at five minutes (RR 1.27, 95% CI 0.85 to 1.92).Combined data from the two high-quality trials
suggest an increased risk of caesarean section in the BPP group RR 1.60, 95% CI 1.05 to 2.44, n = 280, interaction test P = 0.03. However, the
number of participating women was relatively small (n = 280). Therefore, additional evidence is required in order to be definitive regarding
the efficacy of this test in high-risk pregnancies. Furthermore, the impact of the BPP on other interventions, length of hospitalisation,
serious short-term and long-term neonatal morbidity and parental satisfaction requires further evaluation.
Authors' conclusions
At present, there is insufficient evidence from randomised trials to support the use of BPP as a test of fetal wellbeing in high-risk
pregnancies.
[Note: The three citations in the awaiting classification section of the review may alter the conclusions of the review once assessed.]
PLAIN LANGUAGE SUMMARY
Not enough evidence to support use of biophysical profile (BPP) for the assessment of fetal well-being in high-risk pregnancies.
Monitoring the baby's well-being in the uterus in pregnancy is often undertaken using a cardiotocograph (CTG) machine. A CTG assesses
the pattern of the baby's heartbeats alongside the size of the mother's contractions. However, this is not a very accurate test on its own. So
monitoring the baby's movements has also been suggested as a useful addition to predict babies in difficulty. This is because a reduction
in fetal movement sometimes precedes a baby's death. It is thought that if the oxygen supply to the baby through the afterbirth (placenta)
is insufficient, the baby responds by moving less often. As fetal movement patterns may vary considerably, multiple fetal activities might
be a better predictor of poor outcome. Consequently, the biophysical profile (BPP) and modified biophysical profile (MBPP) have been
introduced. The BPP uses ultrasound to assess 1) fetal movement, 2) tone, 3) breathing and 4) the amniotic fluid volume that surrounds
the baby. In addition, the baby's heartbeat is monitored over a 20-minute period using a CTG machine. This produces a paper tracing of the
baby's heart rate, the mother's contractions and when the baby moves. Sometimes a modified BPP is used first (MBPP), involving the CTG
trace and the amniotic fluid volume only. If this indicates a possible abnormality, then the full BPP is used. This review of trials compared
the BPP (or MBPP) with conventional monitoring (CTG only) on pregnancy outcome in high-risk pregnancies. Five trials involving 2974
women with pregnancies with a high risk of poorer fetal outcome were found. There was no difference between the groups in the number of
babies that died, nor in the number of babies who had low Apgar scores. However, although the number of women involved was small, the
BPP was associated with a significant increase in induction and caesarean section. However, the data are insufficient to reach a conclusion
about the benefit or otherwise of the BPP as a test of fetal wellbeing.
BACKGROUND movements within 30 minutes; (ii) fetal tone - one or more episode
of active extension with return to flexion of fetal limb(s) or trunk
Fetal movement is one of the first signs of fetal life and is regarded (opening and closing of hands are considered normal tone); (iii)
as a manifestation of fetal wellbeing (Marsal 1983; Rayburn 1990). fetal breathing movement - at least one episode of fetal breathing
Pregnant women frequently become aware of fetal activity from 18 lasting more than 20 seconds within 30 minutes; (iv) amniotic
to 20 weeks' gestation and maternal perceptions of a reduction or fluid volume - one or more pockets of amniotic fluid measuring
cessation of fetal movements is reported frequently by pregnant more than 2 cm in the vertical axis. These pockets must be free of
women as a cause for concern. The observation that decreased umbilical cord or fetal small parts (the measurement of the single
fetal activity preceded fetal death (Sadovsky 1973) stimulated deepest pool (SDP) is recorded in order to calculate the overall BPP
investigations into the value of the monitoring of fetal movements score) and (v) fetal heart rate reactivity, i.e. two or more episodes
as a mechanism to predict fetal wellbeing (Grant 1989; Rayburn of fetal heart rate acceleration of more than 15 beats per minute
1982). It has been suggested that in the presence of a persistently and of more than 15 seconds duration within 20 minutes. Equal
(chronic) inadequate oxygen supply (hypoxia), the fetus attempts to weight is given to each of the five parameters. A maximum score
reduce the level of oxygen consumption (ACOG 2000; Baskett 1989) of 10 can be achieved and the test is complete once all of the
through reducing fetal activity. Consequently, maternal counting variables have been observed. For the test to be judged abnormal
of fetal movements was proposed as a useful strategy to monitor and a score of zero awarded for the absence of fetal movement,
the fetal condition, with a view to reducing the rate of intrauterine fetal tone or fetal breathing movements, a period of not less than
deaths from hypoxia (Moore 1989). Whilst several studies have 30 minutes must have elapsed. When each of the four ultrasound
demonstrated that diminishing or cessation of fetal activity may variables are normal, the CTG may be excluded as it adds little to the
result in poor pregnancy outcomes (Leader 1981; Moore 1989; predictive accuracy of the BPP, as a BPP score of 8/8 is reassuring
Valentin 1986), others have reported the converse (Harrington (Manning 1995). However, if one or more of the four ultrasound
1998), arguing that reduced fetal movements may indicate that variables are abnormal, the antenatal CTG should be performed.
fetal wellbeing is already compromised (Valentin 1987). In the Observational data have shown that at a cut off score < or = 4,
absence of conclusive evidence that counting fetal movements the sensitivity of the scoring system (i.e. the ability of the test to
reduces the antepartum fetal death rate, alternative methods of correctly identify those babies who are truly not compromised)
fetal assessment such as the biophysical profile (BPP) and the was 12.5% and specificity 99.23%. At a score of < or = 8, sensitivity
cardiotocograph (CTG) have been introduced. and specificity were 70.83% and 91.53%. When compared to each
individual assessment variable, the positive predictive value for
Methods of antenatal assessment of fetal health abnormal perinatal outcome improved when all variables were
Many efforts have been made to develop non-invasive forms combined (Begum 1996) .
of antenatal assessment of fetal wellbeing. As fetal sleeping
The modified BPP (CTG and ultrasonic assessment of amniotic
periods can lead to falsely non-reactive CTG patterns, vibration
fluid)
and sound stimulation (East 2005) and manual fetal manipulation
(Tan 2001) have been used in conjunction with fetal heart rate The BPP is relatively time consuming to perform and consequently
monitoring (Pattison 1999). Such stimuli are intended to provoke several groups (Clark 1989; Nageotte 1994) have made minor
fetal movement and a concurrent acceleration in the fetal heart amendments to the BPP as originally conceived, including
rate, which is an indicator of fetal wellbeing. The concept of variations in the method of estimating amniotic fluid. A shortened
simultaneous evaluation of multiple fetal activities using real time version of the BPP, known as the modified biophysical profile
ultrasonography led to the introduction of the BPP in the early (MBPP), consists of: (i) recording an antenatal CTG (with or
1980s. The BPP is a form of fetal assessment that combines the without vibroacoustic stimulation) combined with (ii) ultrasound
measurement of five biophysical variables as a means of assessing measurement of the amniotic fluid. The MBPP is employed as a
overall fetal wellbeing. The BPP, like other methods of antepartum first-line screening test (Archibong 1999) and should be followed
fetal assessment, is usually started at a gestational age when by the complete BPP as a back-up test when indicated. The
extra-uterine survival or active intervention for fetal compromise is amniotic fluid can be assessed using one of two techniques: (i)
considered feasible (from 24 weeks). measurement of the SDP or (ii) measurement of the Amniotic
fluid index (AFI). AFI assessment is performed according to the
The intervention - BPP technique described by Phelan 1987, whereby the pregnant uterus
The BPP combines the assessment of electronic fetal heart rate is divided into four quadrants and the deepest pocket of amniotic
monitoring (CTG) with four biophysical features, namely (i) fetal fluid in each quadrant is obtained. The AFI is the sum of these four
movements, (ii) fetal tone, (iii) fetal breathing and (iv) estimation measurements.
of amniotic fluid volume. These latter four variables are observed
Conventional monitoring - usually CTG only
using real-time ultrasonography. The fetal heart rate is recorded,
usually over a 20-minute period, and is achieved by using a The antenatal CTG assesses fetal heart rate pattern in response
Doppler ultrasound transducer to monitor the fetal heart through to fetal movement. In the past, the term non-stress test has been
the mother's abdomen. Uterine contractions are monitored used synonymously with antenatal CTG monitoring in order to
simultaneously by a pressure transducer on the mother's abdomen. highlight the absence of uterine activity or contractions. However,
Both transducers are linked to a monitor and this results in a paper when used in isolation from other methods of assessment of
trace known as a CTG. In the original BPP proposed by Manning fetal wellbeing, the antenatal CTG is associated with high false-
1980, two points are awarded for each of the following parameters negative and high false-positive results (Evertson 1979; Schifrin
when present, and zero when absent (there is no intermediate score 1979). Therefore, it was suggested that the combination of multiple
of one): (i) gross body movements - two or more discrete body/limb biophysical variables would reduce both the false-negative and
the high false-positive results associated with measuring a single with four biophysical features namely, (i) fetal movements, (ii)
variable only (Manning 1980; Vintzileos 1983). fetal tone, (iii) fetal breathing and (iv) estimation of amniotic fluid
volume) with conventional monitoring (usually CTG) or MBPP as in
Physiological basis of the ultrasound parameters of the BPP the Alfirevic 1995 trial). As earlier trials may not have used strictly
The physiological and pathological basis of the BPP is the observed random allocation, we planned to include trials that employed
association between hypoxia (low levels of oxygen) and alterations a quasi-randomised method of treatment allocation, such as
of measures of central nervous system performance such as fetal alternation by hospital number or woman's date of birth.
heart rate patterns, fetal movement and fetal tone, which have
Types of participants
been observed in both human and animal fetuses (Manning 1980;
Natale 1979). Hypoxaemia (reduced blood oxygen levels) results Pregnant women with singleton, high-risk pregnancies at greater
in the redistribution of regional blood flow, leading to a reduction than 24 completed weeks' gestation not in labour, and their
in fetal renal blood and fetal oliguria (reduced urine production) babies. High-risk pregnancies included the presence of any one
and, thus, less amniotic fluid. However, it is known that factors or more of the following risk factors: hypertension, intrauterine
other than hypoxaemia may affect BPP parameters. These include growth restriction, post-term (i.e. greater than 42 completed
gestational age (Baskett 1988), administration of steroids (Deren weeks' gestation), intrauterine infection, preterm rupture of
2001), magnesium sulphate (Carlan 1991; Peaceman 1989) and the membranes, diabetes, previous stillbirth/intrauterine death,
excessive transducer pressure on maternal abdomen (Flack 1994). history of decreased fetal movements, antepartum haemorrhage,
As a result, concerns have been raised regarding the limitations premature labour, Rhesus disease, and anaemia during pregnancy.
of individual tests, i.e. CTG or BPP only for the assessment
of fetal wellbeing. Consequently, other tests such as doppler Types of interventions
velocimetry (Neilson 1996) have also been proposed, in addition Biophysical profile versus conventional monitoring (usually CTG or
to or instead of the BPP. Although observational studies have MBPP).
suggested that the BPP confers benefits for those tested by a
reduction in the fetal death rate (Platt 1985), given the considerable For the purpose of this review, the following operational definitions
financial and manpower costs involved in performing the BPP and are used.
potential for harm by increasing the risk of obstetric interventions
(labour induction, caesarean section) that may conceivably lead to The biophysical profile includes ultrasound monitoring of fetal
prematurity and maternal complications, it is important to examine movements, tone, breathing, ultrasound assessment of amniotic
if the BPP confers benefit or harm for the individual woman carrying fluid volume and an antenatal CTG. The antenatal CTG is defined
a high-risk pregnancy. as a hard copy recording of the fetal heart rate and uterine activity
performed on the woman during pregnancy. The MBPP is any
Indication for additional methods of assessment of fetal modification in scoring components, duration of examination or
health definitions of normality/abnormality, or both.
Although the majority of pregnancies proceed without Control group of interest includes: conventional monitoring.
complication and culminate in the birth of a healthy baby to
a well mother, some pregnancies are more complex. High-risk Types of outcome measures
pregnancy is one in which a particular condition places the
mother, the developing fetus, or both at higher-than-normal Outcomes of interest for the infant
risk for complications. These may occur antenatally, in labour (1) Perinatal mortality in normally formed infants.
or postnatally. Factors can be divided into maternal and fetal (2) Severe neonatal morbidity.
causes such as high blood pressure in the mother or growth
restriction in the fetus. For example, growth restriction secondary Short-term/condition at birth
to placental insufficiency is a significant cause of perinatal mortality (3) Acidemia as indicated by umbilical arterial cord blood or
(stillbirth or neonatal death) and morbidity (complications neonatal blood within one hour of birth (or both) with a pH less than
of prematurity) internationally. High-risk pregnancies require seven or base deficit greater than 12 mmol/l, or both.
additional monitoring. However the outcome varies, depending on (4) Five minute Apgar score less than seven.
the particular condition and its severity. (5) Hypoxic ischemic encephalopathy (HIE). This is an identified
cause of brain damage in newborns and refers to a diminished
OBJECTIVES
amount of oxygen in the blood, and a reduced amount of blood
The objective of this review is to assess the effects of the BPP when perfusing the brain. Infants with HIE may show evidence of
compared with conventional monitoring (CTG only or MBPP) on compromise in utero, prolonged low Apgar scores with neurological
pregnancy outcome in high-risk pregnancies. symptoms such as coma, hypotonia/or seizures, respiratory
symptoms such as periodic breathing or apnoea, or develop
METHODS haemorrhagic lesions after birth.
(6) Evidence of multi-organ compromise within the first 24 hours
Criteria for considering studies for this review after birth: for example, renal failure, hepatic injury, cardiac
damage, respiratory complications, or haematological insult.
Types of studies
All randomised and quasi-randomised studies comparing the fetal
biophysical profile (scoring system derived from the assessment
of electronic fetal heart rate monitoring (cardiotocograph (CTG))
Biophysical profile for fetal assessment in high risk pregnancies (Review) 4
Copyright © 2012 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd.
Cochrane Trusted evidence.
Informed decisions.
Library Better health. Cochrane Database of Systematic Reviews
Long-term ordinator searches the register for each review using the topic list
(7) Cognitive impairment - decrease in developmental quotient (70 rather than keywords.
or less). In addition, we searched CENTRAL (The Cochrane Library 2006,
(8) Disability to include non-ambulant cerebral palsy at or after 12 Issue 4), MEDLINE (1966 to November 2006), CINAHL (1982 to
months of age or sensory impairment (visual/hearing), or both. November 2006) and EMBASE (1974 to November 2006) using the
Other search strategies given in Appendix 1.
(9) Incidence of admission to neonatal special care or intensive care We did not apply any language restrictions.
unit, or both.
(10) Respiratory distress syndrome. Data collection and analysis
(11) Transient tachypnoea of the newborn. The methods of the review were developed in light of the advice
(12) Sepsis. contained in the Cochrane Handbook for Systematic Reviews of
(13) Prematurity. Interventions (Higgins 2005).
(14) Length of stay in neonatal special care or intensive care unit,
or both. Study identification
(15) Birthweight less than 10th centile.
All randomised and quasi-randomised trials involving a
Outcomes of interest for the mother comparison of biophysical profile with a) no fetal monitoring and
b) any other form of antenatal fetal monitoring. A full text copy
1. Induction of labour. of each potentially eligible trial identified by the search strategy
2. Induction of labour for abnormal fetal assessment (abnormal was independently assessed for inclusion by Joan Lalor (JGL)
CTG tracing or biophysical profile score). and Bukola Fawole (BF). There were no disagreements regarding
3. Caesarean section. eligibility for inclusion that needed to be resolved by discussion
4. Caesarean section for abnormal fetal assessment. with Declan Devane. We did encounter problems with missing
5. Caesarean section for intrapartum fetal acidosis as defined by information, resulting in two studies being classified as 'Study
fetal blood sample (FBS) pH less than 7.2 or for abnormal fetal awaiting assessment'. We attempted to contact the authors, but
heart rate pattern where a FBS was not taken. were unsuccessful.
6. Incidence of antenatal admissions. Quality assessment of included studies
7. Incidence of fetal blood sampling.
Two review authors (JGL and BF) independently assessed the
8. Length of postnatal hospital stay. quality of all included trials, namely selection and attrition bias.
With regard to performance bias, due to the modus operandi
Search methods for identification of studies
of the biophysical profile (BPP) when compared with antenatal
Electronic searches cardiotocograph (CTG) and other forms of assessment of fetal
wellbeing, it is unlikely that clinicians or women will have been
We searched the Cochrane Pregnancy and Childbirth Group's Trials
blinded to the intervention. Therefore, lack of blinding was not
Register by contacting the Trials Search Co-ordinator (October
considered to undermine the validity of the studies.
2007). We updated this search on 10 January 2012 and added the
results to Studies awaiting classification. Selection bias
The Cochrane Pregnancy and Childbirth Group’s Trials Register is We allocated studies a grade on the basis of allocation concealment
maintained by the Trials Search Co-ordinator and contains trials as per criteria outlined in Higgins 2005, i.e. (A) adequate, (B) unclear
identified from: for trials where randomisation is not clearly described or prone to
bias (e.g. open card, coin toss), (C) for quasi-randomised designs
1. quarterly searches of the Cochrane Central Register of such as alternate allocation and use of record numbers.
Controlled Trials (CENTRAL);
2. weekly searches of MEDLINE; Attrition bias
3. weekly searches of EMBASE; Due to inadequacies in reporting how losses of participants (e.g.
4. handsearches of 30 journals and the proceedings of major withdrawals, dropouts, protocol deviations) were handled, the
conferences; review authors were cautious about implicit accounts of follow
5. weekly current awareness alerts for a further 44 journals plus up. Given that study reports on attrition after allocation have not
monthly BioMed Central email alerts. been found to be consistently related to bias, we did not exclude
studies on the basis of attrition. Studies were, however, graded
Details of the search strategies for CENTRAL, MEDLINE and EMBASE, for completeness of follow up using the following criteria. For
the list of handsearched journals and conference proceedings, and completeness of follow up:
the list of journals reviewed via the current awareness service can (A) less than 3% of participants excluded;
be found in the ‘Specialized Register’ section within the editorial (B) 3% to 9.9% of participants excluded;
information about the Cochrane Pregnancy and Childbirth Group. (C) 10% to 19.9% of participants excluded;
(D) more than 20% of participants excluded.
Trials identified through the searching activities described above
are each assigned to a review topic (or topics). The Trials Search Co-
Data extraction on the basis of normal or abnormal test results (without reference
to the test performed) in the Manning 1984, Lewis 1999 and Alfirevic
Two review authors (JGL and BF) independently extracted the
1995 trials. Blinding was either not reported or not done in the
data using data extraction forms designed specifically for the
Nageotte 1994 and Platt 1985 trials. Although not all trials reported
review, the fields of which had been agreed by all review
the gestational age range of included pregnancies, it is of interest to
authors. We extracted data by allocated intervention, irrespective
note that the majority of included pregnancies were at or close to
of compliance with allocated intervention, in order to allow an
term (36.2 to greater than 42 weeks in the Manning 1984; Platt 1985;
'intention-to-treat' analysis. Women who were randomised, and
Nageotte 1994; Alfirevic 1995 trials (n = 2829)), whereas the mean
then either excluded or lost to follow up, were assumed to have
gestational age in the Lewis 1999 trial (n = 135) was 24.2 weeks.
no event in the main analysis, and denominators were altered
(There are three trial reports in Studies awaiting classification to be
to reflect when this occurred. Study eligibility was re-confirmed
assessed.)
at the time of data extraction. Two review authors (JGL and BF)
independently entered data onto the Review Manager (RevMan Outcomes of interest to the fetus
2003) computer programme, independently checked them for
accuracy and analysed them using RevMan 2003. Four studies provided data on perinatal deaths (Alfirevic 1995;
Manning 1984; Nageotte 1994; Platt 1985) and all included trials
Data analysis provided data on the five-minute Apgar score after birth. Data for
several neonatal outcomes were available from one study only,
We performed statistical analysis with RevMan 2003. We reported
i.e. admission to the neonatal unit (Alfirevic 1995), birthweight
dichotomous (or binary) outcomes using the 'relative risk'
less than the 10th centile (Platt 1985), and the presence of intra-
summary statistic and their 95% confidence intervals. We reported
amniotic infection (Lewis 1999).
continuous data using the standard mean differences (due to non-
normal distribution) and their 95% confidence intervals. We used Outcomes of interest to the mother
a fixed-effect model of meta-analysis for summarising the results
of studies in the absence of substantial heterogeneity between The data for induction of labour were available from one trial
trials (measured using the I2 statistic). The statistic is more robust (Alfirevic 1995) and outcome data for caesarean section were
than the Chi-squared test, as it is less affected by the number available in four studies (Alfirevic 1995; Lewis 1999; Nageotte 1994;
of trials in the analysis (Higgins 2005). I2 values of 30% to 50% Platt 1985).
suggest mild heterogeneity and more than 50% implies substantial Where an outcome is not listed in the comparison section, no data
heterogeneity (Higgins 2005). were available in a usable format from any study for that a priori
Sensitivity analysis defined outcome.
We performed sensitivity analysis based on quality, comparing Risk of bias in included studies
high-quality trials (allocation concealment and attrition classified
Five trials met our inclusion criteria. Two trials included in the
as 'A' (adequate, less than 3%)) with trials of lower quality for
review ran the risk of biased allocation through the use of coin
two outcomes: caesarean section and Apgar score, as data were
flip (Manning 1984) or unblinded alternate allocation (Platt 1985).
available in a usable format for these outcomes from each trial.
There was a significant and unexplained imbalance in the numbers
RESULTS of randomised participants in the Platt 1985 trial (279 in the
experimental group compared with 373 in the control group).
Description of studies For one trial, it is unclear as to whether there was adequate
concealment of allocation (Nageotte 1994).
Our search strategy identified 498 citations corresponding to 73
studies for potential inclusion. We excluded 55 studies during An 'intention-to-treat analysis' was used in four of the five trials
the initial screening and assessed 17 studies on the basis of (Alfirevic 1995; Lewis 1999; Manning 1984; Nageotte 1994). The
their full text paper (or abstract) based on the inclusion and original report by Platt 1985 included only women who delivered
exclusion criteria indicated above. Of those, we excluded 10 studies within seven days of a test (76% in the experimental group and
from the review (see 'Characteristics of excluded studies' ). We 74% in the control group). Additional unpublished data on the other
encountered difficulties with missing information in two studies. women recruited in this trial were supplied by Dr Platt.
There was insufficient information on the trial design and attrition
rates in the Lien 1994 study, and on the trial design and event In the Lewis 1999 trial, women were randomly allocated to
rates in the Petrovic 1998 study. Efforts to contact the authors receive a daily biophysical profile (BPP) or a daily cardiotocograph
were unsuccessful; consequently these studies remain classified (CTG). The last test score obtained before the mother gave birth
as 'Studies awaiting assessment'. (Three reports are awaiting was used in evaluating the effectiveness of the BPP and the
assessment.) Five trials met the inclusion criteria for this review (see CTG for predicting infectious complications for the mother or
'Characteristics of included studies' table). Four studies, with 2829 fetus. However, abnormal results in the CTG group led to further
participating women, compared biophysical profile (BPP) with evaluation with a biophysical profile. In two trials (Manning 1984;
cardiotocograph (CTG) (Lewis 1999; Manning 1984; Nageotte 1994; Platt 1985), the BPP was performed on all women, but where a
Platt 1985) and one trial (Alfirevic 1995), with 145 participating woman had been allocated to the control group, then CTG results
women, compared complex BPP (a modified biophysical profile alone were disclosed to clinicians. There was no attempt to conceal
(MBPP) comprising computerised CTG, AFI and assessment of fetal allocation from participants after randomisation in the Nageotte
breathing, tone and gross body movements) with CTG and amniotic 1994 and Alfirevic 1995 trials. Group allocation was concealed from
fluid assessment using SDP technique. Pregnancies were managed managing physicians in the Platt 1985 trial, as results were reported
as either normal, suspicious or abnormal, whereas all test results fetuses at increased risk of poor outcomes in pregnancies with
were reviewed by a member of the fetal medicine faculty in the identified obstetric risk factors. Available evidence from the
Lewis 1999 trial. randomised trials included here does not support the use of BPP
as a test of fetal wellbeing in high-risk pregnancies. However,
Effects of interventions the findings should be considered, taking cognisance of the fact
that the total number of women included in this meta-analysis
(1) Biophysical profile (BPP) versus conventional monitoring
remains small at 2974, and some of the studies carry a high risk
Five randomised trials have been included in this review with of bias (large imbalance in the numbers of women in each group
2974 participating women. When the biophysical profile (BPP) is in the Platt 1985 trial, randomisation using a coin flip in Manning
compared with conventional fetal monitoring (cardiotocograph 1984 trial). The overall incidence of adverse outcomes was low
(CTG) or modified biophysical profile (amniotic fluid assessment (perinatal deaths = 0.81%, Apgar score at or below seven at five
and CTG), we found no significant differences between the groups minutes = 2.9%); thus additional evidence is required to support
in perinatal deaths in infants (including those with congential the value of the test in high-risk pregnancies. In order to derive any
malformations) (relative risk (RR) 1.33, 95% confidence interval (CI) meaningful conclusions about the impact of the BPP on perinatal
0.60 to 2.98, n = 2839, four trials), Apgar score less than seven at mortality, in excess of 10,000 women would need to be studied.
five minutes (RR 1.27, 95% CI 0.85 to 1.92, n = 2974, five trials) and It is also important to note that, although the BPP is used in
overall incidence of caesarean section (RR 1.18, 95% CI 0.90 to 1.54, clinical practice to assess fetal wellbeing at premature gestations,
n = 2239, four trials). most trials, with the exception of Lewis 1999 (n = 135), included
participants with pregnancies of 36 weeks' gestation or more.
The following a priori defined outcomes were reported in individual Furthermore, the impact of the BPP at premature gestations, on
trials and consequently, comparable data were not available for intervention rates, length of hospitalisation, serious short-term and
meta-analysis; however, we found no differences between the long-term neonatal morbidity and parental satisfaction requires
groups for incidence of admission to the neonatal intensive care further evaluation.
unit (NICU) (RR 0.20, 95% CI 0.01 to 4.15, n = 145, P = 0.30), presence
of meconium at birth (RR 1.45, 95% CI 0.79 to 2.64, n = 145, P = 0.23) The increase in the rate of induction of labour observed in the small
(Alfirevic 1995) and birthweight less than 10th centile (RR 0.71, 95% trial by Alfirevic and Walkinshaw (Alfirevic 1995) highlights the need
CI 0.32 to 1.56, n = 652, P = 0.39) (Platt 1985). for careful evaluation of the impact of different fetal monitoring
policies on a much wider range of relevant outcomes. The observed
There were significant differences between the groups (favouring increase in this outcome in this study was thought by the authors
conventional monitoring) in length of stay for the neonate in the to be caused by the difference in the type of test used to assess
NICU (SMD 0.20 95% CI 0.09 to 0.30, n = 1442, two trials). However, amniotic fluid volume in two groups (amniotic fluid index in the BPP
the data are skewed due to the length of stay associated with group (experimental) and maximum pool depth in the MBPP group
prematurity in the Lewis 1999 trial and are therefore unreliable. (control)) rather than by the BPP itself. The amniotic fluid index was
Women in the BPP group were also more likely to have labour more frequently abnormal than maximum pool depth leading to
induced (RR 1.45, 95% CI 1.04 to 2.03, n = 145, one trial, P = 0.03), increased intervention in the BPP group.
in particular for an abnormal BPP test result (RR 2.58, 95% CI 1.39
to 4.78, n =145, P = 0.003). The Lewis 1999 trial (n = 135) found that It is regrettable that since the introduction of the BPP in the 1980s,
neither the BPP nor daily CTG demonstrated good sensitivity for and following reports of observational studies of tens of thousands
predicting infectious complications following preterm prelabour of pregnancies, less than 3000 women have been enrolled into
rupture of membranes. randomised trials.
No reported data were available for analysis for the following AUTHORS' CONCLUSIONS
outcomes: acidemia, transient tachypnoea of the newborn, hypoxic
ischaemic encephalopathy, multi-organ compromise, cognitive Implications for practice
impairment or disability, incidence of antenatal admissions,
incidence of fetal blood sampling, and length of postnatal hospital There is insufficient evidence from randomised trials to support
stay. the biophysical profile (BPP) as a test of fetal wellbeing in high-
risk pregnancies. Although the number of participating women was
Sensitivity analysis (high-quality trials) relatively small (n = 280), combined data from the two high-quality
trials Alfirevic 1995 and Lewis 1999 suggest an increase in the risk
There was no significant difference in Apgar scores less than seven of caesarean section in the BPP group. In addition, the increase in
at five minutes between the groups (outcome 02.01, RR 1.37, 95% the rate of induction of labour in the Alfirevic 1995 trial highlights
CI 0.63 to 3.01, n = 280, two trials). However, it would appear that the need for careful evaluation of the impact of the BPP on a
the risk of having a caesarean section was influenced by the quality wide range of relevant maternal and neonatal outcomes. However,
of the trials (outcome 02.02). In the two high-quality trials (Alfirevic additional data are required to reach any definite conclusion about
1995; Lewis 1999) the caesarean section rate in the BPP group was the benefit or otherwise of the BPP in high-risk pregnancies, as
higher than women who had a CTG or CTG and MBPP (RR) 1.60, 95% the total number of women included in this meta-analysis remains
CI 1.05 to 2.44, n = 280, interaction test P = 0.03. small at 2964. Consequently, careful evaluation of the impact of
the BPP on intervention rates, in premature gestations, on serious
DISCUSSION short-term and long-term neonatal morbidity is required.
The main reason for the introduction of the biophysical profile [Note: The three citations in the awaiting classification section of
(BPP) into clinical practice was the belief that it would identify the review may alter the conclusions of the review once assessed.]
REFERENCES
References to studies included in this review James 2001 {published data only}
Alfirevic 1995 {published data only} James C, George SS, Gaunekar N, Seshadri L. Management of
prolonged pregnancy: a randomized trial of induction of labour
Alfirevic Z, Walkinshaw SA. A randomised controlled trial of
and antepartum foetal monitoring. National Medical Journal of
simple compared with complex antenatal fetal monitoring
India 2001;14(5):270-3.
after 42 weeks of gestation. British Journal of Obstetrics and
Gynaecology 1995;102:638-43. Kamel 1999 {published data only}
Lewis 1999 {published data only} Kamel HS, Makhlouf AM, Youssef AA. Simplified biophysical
profile: an antepartum fetal screening test. Gynecologic and
* Lewis DF, Adair CD, Weeks JW, Barrilleaux PS, Edwards MS,
Obstetric Investigation 1999;47(4):223-8.
Garite TJ. A randomized clinical trial of daily nonstress testing
versus biophysical profile in the management of preterm Magann 2003 {published data only}
premature rupture of membranes. American Journal of
Magann E, Doherty D, Field K, Chauhan S, Muffley P, Morrison J.
Obstetrics and Gynecology 1999;181:1495-9.
Biophysical profile with amniotic fluid volume assessment: a
Lewis DF, Adair CD, Weeks JW, Barrilleaux PS, Edwards MS, randomized controlled trial of the amniotic fluid index versus
Garite TJ. A randomized clinical trial of nonstress test single deepest pocket [abstract]. American Journal of Obstetrics
versus biophysical profile in preterm premature rupture of and Gynecology 2003;189(6):S179.
membranes. American Journal of Obstetrics and Gynecology
Magann EF, Doherty DA, Field K, Chauhan SP, Muffley PE,
1998;178(1 Pt 2):S197.
Morrison JC. Biophysical profile with amniotic fluid volume
Manning 1984 {published data only} assessments. Obstetrics & Gynecology 2004;104(1):5-10.
Manning FA, Lange IR, Morrison I, Harman CR. Fetal biophysical Ott 1998 {published data only}
profile score and the nonstress test: a comparative trial.
Ott WJ, Mora G, Arias F, Sunderji S, Sheldon G. Comparison
Obstetrics & Gynecology 1984;64:326-31.
of the modified biophysical profile to a "new" biophysical
Nageotte 1994 {published data only} profile incorporating the middle cerebral artery to umbilical
artery velocity flow systolic/diastolic ratio. American Journal of
Nageotte MP, Towers CV, Asrat T, Freeman RK. Perinatal
Obstetrics and Gynecology 1998;178(6):1346-53.
outcome with the modified biophysical profile. American
Journal of Obstetrics and Gynecology 1994;170:1672-6. Tongsong 1999 {published data only}
Platt 1985 {published and unpublished data} Tongsong T, Piyamongkol W, Anantachote A, Pulphutapong K.
The rapid biophysical profile for assessment of fetal well-
Platt LD, Walla CA, Paul RH, Trujillo ME, Loesser CV, Jacobs ND,
being. Journal of Obstetrics and Gynaecology Research
et al. A prospective trial of the fetal biophysical profile
1999;25(6):431-6.
vs the nonstress test in the management of high-risk
pregnancies. American Journal of Obstetrics and Gynecology Tyrrell 1990 {published data only}
1985;153(6):624-33.
Tyrrell SN, Lilford RJ, MacDonald H, Nelson E, Porter J,
Gupta JK. Randomized comparison of routine vs highly
References to studies excluded from this review selective use of Doppler ultrasound and biophysical scoring to
investigate high risk pregnancies. British Journal of Obstetrics
Chauhan 2004 {published data only} and Gynaecology 1990;10:909-16.
Chauhan SP, Doherty DD, Magann EF, Cahanding F, Moreno F,
Klausen JH. Amniotic fluid index vs single deepest pocket
technique during modified biophysical profile: a randomized References to studies awaiting assessment
clinical trial. American Journal of Obstetrics and Gynecology Jamal 2007 {published data only}
2004;191(2):661-6.
Jamal A, Marsoosi V, Eslamian L, Noori K. A prospective trial
Habek 2001 {published data only} of the fetal biophysical profile versus modified biophysical
profile in the management of high risk pregnancies. Acta Medica
Habek D, Hodek B, Herman R, Maticevic A, Jugovic D,
Iranica 2007; Vol. 45, issue 3:204-8.
Habek J, et al. Modified fetal biophysical profile in the
assessment of perinatal outcome. Zentralblatt fur Gynakologie Lien 1994 {published data only}
2001;123(7):411-7.
Lien JM, Nageotte MP, Towers CV, de Veciana M, Toohey JS.
Jamal 2005 {published data only} Intrauterine growth retardation: contraction stress test or
biophysical profile?. American Journal of Obstetrics and
Jamal A. A prospective trial of the fetal biophysical vs
Gynecology 1994;170:316.
the modified biophysical in the management of high-risk
pregnancies. Ultrasound in Obstetrics & Gynecology 2005;26:444.
Participants 145 women with uncomplicated singleton post-term pregnancies (= or > 42 weeks); 72 women were
randomised to BPP and 73 to simple monitoring.
Interventions Complex (BPP) versus simple fetal monitoring (CTG and amniotic fluid measurement) twice weekly.
Experimental group: complex BPP: FM, FT, FBM and computerised CTG instead of standard CTG, amni-
otic fluid assessment using AFI technique
Control group: CTG and ultrasound measurement of the maximum pool depth twice weekly.
If monitoring was normal, labour was induced at 43 weeks. Abnormal monitoring was an indication for
induction of labour as soon as possible.
Alfirevic 1995 (Continued)
Notes
Risk of bias
Lewis 1999
Methods Randomisation: random-number tables.
Notes
Risk of bias
Manning 1984
Methods Randomisation: coin flip.
Participants 735 high-risk women referred with the diagnosis other than suspected IUGR, ie hypertension (27%),
post-term (22%), diabetes (15%), previous stillbirth (7%), decreased fetal movements (4%), antepartum
haemorrhage (4%), premature labour (3%), Rh disease (1%). 360 women were assigned to a non-stress
test and 375 to a BPP. Mean gestational age 36.2 weeks.
Outcomes Perinatal deaths (> 500 gr, > 20 weeks' gestation, < 28 days of neonatal life).
Apgar < 7 after 5 minutes.
Notes
Manning 1984 (Continued)
Risk of bias
Nageotte 1994
Methods Randomisation: not stated.
Participants 1307 women referred for antepartum fetal surveillance who had abnormal 'modified' BPP (CTG with
sound stimulation and the amniotic fluid index); 628 were randomised to a contraction stress test and
679 to a BPP.
Insulin-dependent women were excluded. Mean gestational age 40.1 weeks.
Interventions All women were monitored with twice weekly MBPP (CTG and amniotic fluid assessment using AFI tech-
nique). Women with abnormal results were randomised into backup BPP or contraction stress test. Ex-
perimental group: full BPP as a back-up test.
Control group: contraction stress test as a back-up test.
Notes
Risk of bias
Platt 1985
Methods Quasi-randomisation using sequential numbers (even/odd).
Participants 642 women with high-risk pregnancies, ie post-term (41%), IUGR (13%), diabetes (12%), decreased fetal
movements (7%), hypertension (12%), previous stillbirth (3%). 279 women were randomised to a BPP
and 373 to the control group. Mean gestational age 39 weeks.
Platt 1985 (Continued)
Notes
Risk of bias
Chauhan 2004 This randomised study compared (i) MBPP (CTG and sonographic estimation of amniotic fluid) or
(ii) determination of the presence or absence of a 2x1-cm single deepest pocket.
Habek 2001 Non-randomised trial; included pregnant women with a singleton pregnancy in the 28th to 42nd
week of gestation with clinically and ultrasonically verified fetal growth retardation and evaluation
of the variables of the BPP for prediction of perinatal outcome.
Jamal 2005 This randomised trial did not include antenatal CTG. 2 randomised groups received (i) BPP or (ii)
MBPP.
James 2001 This randomised study of low-risk women (287 days' gestation) compared (i) induction of labour
with (ii) antenatal monitoring (daily fetal movement counting and BPP alternate days).
Kamel 1999 This non-randomised trial included 2 groups of high-risk women comparing (i) BPP and fetal
acoustic stimulation and (ii) BPP and antenatal CTG.
Magann 2003 This randomised study compared (i) AFI or (ii) the SDP technique to estimate the adequacy of am-
niotic fluid volume during a BPP along with the other components of the test in predicting an ad-
verse pregnancy outcome. Conclusion: the AFI offers no advantage in the detection of adverse out-
comes to the SDP when assessed with the other components of the BPP.
Ott 1998 Does not meet the criteria for this review.
Tongsong 1999 Non-randomised trial; compared 2 groups (i) antenatal CTG with (ii) the rapid BPP which includes
estimation of the AFI and SPFM to predict intrapartum fetal distress in high-risk pregnancies.
Tyrrell 1990 This randomised study of high-risk women compared 2 groups (i) routine BPP with (ii) umbilical
and uteroplacental artery doppler velocity waveforms for obstetric intervention rates and short-
term neonatal morbidity.
DATA AND ANALYSES
Comparison 1. Biophysical profile versus conventional fetal monitoring (CTG)
1 Perinatal deaths including major 4 2839 Risk Ratio (M-H, Fixed, 95% CI) 1.33 [0.60, 2.98]
malformations
2 Apgar score < 7 at or after 5 min- 5 2974 Risk Ratio (M-H, Fixed, 95% CI) 1.27 [0.85, 1.92]
utes (all infants included)
3 Admission to neonatal intensive 1 145 Risk Ratio (M-H, Fixed, 95% CI) 0.20 [0.01, 4.15]
care unit
4 Length of stay in neonatal inten- 2 1442 Std. Mean Difference (IV, Fixed, 95% CI) 0.20 [0.09, 0.30]
sive care unit
5 Birthweight < 10th centile 1 652 Risk Ratio (M-H, Fixed, 95% CI) 0.71 [0.32, 1.56]
6 Meconium 1 145 Risk Ratio (M-H, Fixed, 95% CI) 1.45 [0.79, 2.64]
7 Respiratory distress syndrome 1 135 Risk Ratio (M-H, Fixed, 95% CI) 1.72 [0.97, 3.04]
8 Induction for abnormal fetal as- 1 145 Risk Ratio (M-H, Fixed, 95% CI) 2.58 [1.39, 4.78]
sessment (biophysical profile or car-
diotocograph)
9 Caesarean section 4 2239 Risk Ratio (M-H, Fixed, 95% CI) 1.18 [0.90, 1.54]
10 Caesarean section for fetal dis- 2 1452 Risk Ratio (M-H, Fixed, 95% CI) 1.18 [0.83, 1.68]
tress
11 Caesarean section for intra- 2 1959 Risk Ratio (M-H, Fixed, 95% CI) 1.03 [0.74, 1.42]
partum fetal distress
12 Induction of labour 1 145 Risk Ratio (M-H, Fixed, 95% CI) 1.45 [1.04, 2.03]
Analysis 1.1. Comparison 1 Biophysical profile versus conventional fetal
monitoring (CTG), Outcome 1 Perinatal deaths including major malformations.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 1/72 0/73 4.84% 3.04[0.13,73.44]
Manning 1984 4/375 4/360 39.77% 0.96[0.24,3.81]
Nageotte 1994 5/679 3/628 30.37% 1.54[0.37,6.42]
Platt 1985 3/279 3/373 25.02% 1.34[0.27,6.57]
Analysis 1.2. Comparison 1 Biophysical profile versus conventional fetal monitoring
(CTG), Outcome 2 Apgar score < 7 at or after 5 minutes (all infants included).
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 1/72 0/73 1.29% 3.04[0.13,73.44]
Lewis 1999 11/66 9/69 22.83% 1.28[0.57,2.88]
Manning 1984 17/375 15/360 39.72% 1.09[0.55,2.15]
Nageotte 1994 11/679 6/628 16.18% 1.7[0.63,4.56]
Platt 1985 8/279 9/373 19.99% 1.19[0.46,3.04]
Total (95% CI) 1471 1503 100% 1.27[0.85,1.92]
Total events: 48 (BPP), 39 (CTG)
Heterogeneity: Tau2=0; Chi2=0.84, df=4(P=0.93); I2=0%
Test for overall effect: Z=1.16(P=0.25)
Analysis 1.3. Comparison 1 Biophysical profile versus conventional fetal
monitoring (CTG), Outcome 3 Admission to neonatal intensive care unit.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 0/72 2/73 100% 0.2[0.01,4.15]
Total (95% CI) 72 73 100% 0.2[0.01,4.15]
Total events: 0 (BPP), 2 (CTG)
Heterogeneity: Not applicable
Test for overall effect: Z=1.04(P=0.3)
Analysis 1.4. Comparison 1 Biophysical profile versus conventional fetal
monitoring (CTG), Outcome 4 Length of stay in neonatal intensive care unit.
Study or subgroup BPP CTG Std. Mean Difference Weight Std. Mean Difference
N Mean(SD) N Mean(SD) Fixed, 95% CI Fixed, 95% CI
Lewis 1999 66 33.8 (39.6) 69 28.2 (25.4) 9.38% 0.17[-0.17,0.51]
Nageotte 1994 679 5.2 (11.2) 628 3.4 (5.9) 90.62% 0.2[0.09,0.31]
Study or subgroup BPP CTG Std. Mean Difference Weight Std. Mean Difference
N Mean(SD) N Mean(SD) Fixed, 95% CI Fixed, 95% CI
Total *** 745 697 100% 0.2[0.09,0.3]
Heterogeneity: Tau2=0; Chi2=0.03, df=1(P=0.87); I2=0%
Test for overall effect: Z=3.71(P=0)
Analysis 1.5. Comparison 1 Biophysical profile versus conventional
fetal monitoring (CTG), Outcome 5 Birthweight < 10th centile.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Platt 1985 9/279 17/373 100% 0.71[0.32,1.56]
Total (95% CI) 279 373 100% 0.71[0.32,1.56]
Total events: 9 (BPP), 17 (CTG)
Heterogeneity: Not applicable
Test for overall effect: Z=0.85(P=0.39)
Analysis 1.6. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG), Outcome 6 Meconium.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 20/72 14/73 100% 1.45[0.79,2.64]
Total (95% CI) 72 73 100% 1.45[0.79,2.64]
Total events: 20 (BPP), 14 (CTG)
Heterogeneity: Not applicable
Test for overall effect: Z=1.21(P=0.23)
Analysis 1.7. Comparison 1 Biophysical profile versus conventional
fetal monitoring (CTG), Outcome 7 Respiratory distress syndrome.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Lewis 1999 23/66 14/69 100% 1.72[0.97,3.04]
Total (95% CI) 66 69 100% 1.72[0.97,3.04]
Total events: 23 (BPP), 14 (CTG)
Heterogeneity: Not applicable
Test for overall effect: Z=1.85(P=0.06)
Analysis 1.8. Comparison 1 Biophysical profile versus conventional fetal monitoring (CTG),
Outcome 8 Induction for abnormal fetal assessment (biophysical profile or cardiotocograph).
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 28/72 11/73 100% 2.58[1.39,4.78]
Total (95% CI) 72 73 100% 2.58[1.39,4.78]
Total events: 28 (BPP), 11 (CTG)
Heterogeneity: Not applicable
Test for overall effect: Z=3.01(P=0)
Analysis 1.9. Comparison 1 Biophysical profile versus
conventional fetal monitoring (CTG), Outcome 9 Caesarean section.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 13/72 7/73 7.92% 1.88[0.8,4.45]
Lewis 1999 21/66 14/69 15.6% 1.57[0.87,2.82]
Nageotte 1994 55/679 44/628 52.1% 1.16[0.79,1.69]
Platt 1985 14/279 25/373 24.38% 0.75[0.4,1.41]
Total (95% CI) 1096 1143 100% 1.18[0.9,1.54]
Total events: 103 (BPP), 90 (CTG)
Heterogeneity: Tau2=0; Chi2=4.02, df=3(P=0.26); I2=25.41%
Test for overall effect: Z=1.2(P=0.23)
Analysis 1.10. Comparison 1 Biophysical profile versus conventional
fetal monitoring (CTG), Outcome 10 Caesarean section for fetal distress.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 8/72 6/73 11.53% 1.35[0.49,3.7]
Nageotte 1994 55/679 44/628 88.47% 1.16[0.79,1.69]
Total (95% CI) 751 701 100% 1.18[0.83,1.68]
Total events: 63 (BPP), 50 (CTG)
Heterogeneity: Tau2=0; Chi2=0.08, df=1(P=0.78); I2=0%
Test for overall effect: Z=0.9(P=0.37)
Analysis 1.12. Comparison 1 Biophysical profile versus conventional
fetal monitoring (CTG), Outcome 12 Induction of labour.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 43/72 30/73 100% 1.45[1.04,2.03]
Total (95% CI) 72 73 100% 1.45[1.04,2.03]
Total events: 43 (BPP), 30 (CTG)
Heterogeneity: Not applicable
Test for overall effect: Z=2.19(P=0.03)
Comparison 2. Biophysical profile versus conventional monitoring (CTG) - high-quality trials
1 Apgar score < 7 at or after 5 minutes 2 280 Risk Ratio (M-H, Fixed, 95% CI) 1.37 [0.63, 3.01]
2 Caesarean section 2 280 Risk Ratio (M-H, Fixed, 95% CI) 1.60 [1.05, 2.44]
Analysis 2.1. Comparison 2 Biophysical profile versus conventional monitoring
(CTG) - high-quality trials, Outcome 1 Apgar score < 7 at or after 5 minutes.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 1/72 0/73 5.34% 3.04[0.13,73.44]
Lewis 1999 11/66 9/69 94.66% 1.28[0.57,2.88]
Total (95% CI) 138 142 100% 1.37[0.63,3.01]
Total events: 12 (BPP), 9 (CTG)
Analysis 2.2. Comparison 2 Biophysical profile versus conventional
monitoring (CTG) - high-quality trials, Outcome 2 Caesarean section.
Study or subgroup BPP CTG Risk Ratio Weight Risk Ratio
n/N n/N M-H, Fixed, 95% CI M-H, Fixed, 95% CI
Alfirevic 1995 21/72 13/73 48.54% 1.64[0.89,3.02]
Lewis 1999 21/66 14/69 51.46% 1.57[0.87,2.82]
Total (95% CI) 138 142 100% 1.6[1.05,2.44]
Total events: 42 (BPP), 27 (CTG)
Heterogeneity: Tau2=0; Chi2=0.01, df=1(P=0.92); I2=0%
Test for overall effect: Z=2.18(P=0.03)
APPENDICES
1. biophysical profil$.af.
2. randomized controlled trial.pt.
3. exp Randomized Controlled Trials/
4. exp Random Allocation/
5. exp Double-Blind Method/
6. exp single-blind method/
7. clinical trial.pt.
8. exp Clinical Trials/
9. (clin$ adj25 trial$).tw.
10.((singl$ or doubl$ or trebl$ ot tripl$) adj25 (blind$ or mask$)).tw.
11.exp Placebos/
12.placebo$.tw.
13.random$.tw.
14.exp Research Design/
15.comparative study/
16.exp Evaluation Studies/
17.exp Follow-Up Studies/
18.exp Prospective Studies/
19.or/ 2-18
20.1 and 19
CINAHL
2. clinical trial.pt.
3. (clinic$ adj trial$1).tw.
4. (((singl$ or doubl$ or treb$ or tripl$) adj blind$3) or mask$3).tw.
5. randomi?ed control$ trial$.tw.
6. exp Random Assignment/
7. random$ allocat$.tw.
8. placebo$.tw.
9. exp Quantitative Studies/
10.random$ allocat$.tw.
11.exp Placebos/
12.or/1-11
13.biophysical profil$.af.
14.13 and 12
EMBASE
1. randomization/
2. double blind procedure/
3. crossover procedure/
4. intermethod comparison/
5. single blind procedure/
6. clinical study/
7. controlled study/
8. randomized controlled trial/
9. (clin$ adj2 trial$).tw.
10.((singl$ or doubl$ or trebl$ or tripl$) adj2 (blind$ or mask$)).tw.
11.exp clinical trial/
12.placebo/
13.placebo$.tw.
14.random$.tw.
15.comparison/
16.follow up/
17.evaluation.mp. and follow up/
18."evaluation and follow up"/
19.prospective study/
20.major clinical study/
21.(control$ or prospectiv$ or volunteer$).tw.
22.1 or 2 or 3 or 4 or 5 or 6 or 7 or 8 or 9 or 10 or 11 or 12 or 13 or 14 or 15 or 16 or
23.17 or 18 or 19 or 20 or 21 or 22
24.23 biophysical profil$.af. and 22
WHAT'S NEW
Date Event Description
10 January 2012 Amended Search updated. One report added to Studies awaiting classifica-
tion (Jamal 2007)
HISTORY
Protocol first published: Issue 2, 1996
Review first published: Issue 2, 1996
Date Event Description
CONTRIBUTIONS OF AUTHORS
The original review was conceived by ZA.
JL and DD updated the methods section and BF updated the background.
JL and BF extracted and entered the data for analysis independently.
JL ran the analyses and drafted the results; however, all authors contributed to each section of the final review.
DECLARATIONS OF INTEREST
Zarko Alfirevic is the first author of one of the randomised trials included in this review.
SOURCES OF SUPPORT
Internal sources
• The University of Liverpool, UK.
External sources
• No sources of support supplied
INDEX TERMS