Factors predisposing to perinatal death related to uterine rupture during attempted vaginal birth after caesarean section: retrospective cohort study

doi:10.1136/bmj.38160.634352.55

BMJ 2004;329:375 (14 August), doi:10.1136/bmj.38160.634352.55 (published 19 July 2004)

Paper

Factors predisposing to perinatal death related to uterine rupture during attempted vaginal birth after caesarean section: retrospective cohort study

Gordon C S Smith, professor¹, Jill P Pell, consultant², Dharmintra Pasupathy, specialist registrar³, Richard Dobbie, senior statistician⁴

¹ Department of Obstetrics and Gynaecology, Cambridge University, Cambridge CB2 2QQ, ² Department of Public Health, Greater Glasgow NHS Board, Glasgow G3 8YU, ³ Departments of Obstetrics and Gynaecology, Addenbrooke's NHS Trust, Cambridge CB2 2SW, ⁴ Information and Statistics Division, Common Services Agency, Edinburgh EH5 3SE

Correspondence to: G C S Smith gcss2{at}cam.ac.uk

Abstract

Objective To determine the factors associated with an increasedrisk of perinatal death related to uterine rupture during attemptedvaginal birth after caesarean section.

Design Population based retrospective cohort study.

Setting Data from the linked Scottish Morbidity Record and Stillbirthand Infant Death Survey of births in Scotland, 1985-98.

Participants All women with one previous caesarean deliverywho gave birth to a singleton infant at term by a means otherthan planned repeat caesarean section (n = 35 854).

Main outcome measures All intrapartum uterine rupture and uterinerupture resulting in perinatal death (that is, death of thefetus or neonate).

Results The overall proportion of vaginal births was 74.2% andof uterine rupture was 0.35%. The risk of intrapartum uterinerupture was higher among women who had not previously givenbirth vaginally (adjusted odds ratio 2.5, 95% confidence interval1.6 to 3.9, P < 0.001) and those whose labour was inducedwith prostaglandin (2.9, 2.0 to 4.3, P < 0.001). Both factorswere also associated with an increased risk of perinatal deathdue to uterine rupture. Delivery in a hospital with < 3000births a year did not increase the overall risk of uterine rupture(1.1, 0.8 to 1.5, P = 0.67). However, the risk of perinataldeath due to uterine rupture was significantly higher in hospitalswith < 3000 births a year (one per 1300 births) than in hospitalswith $≥$ 3000 births a year (one per 4700; 3.4, 1.0 to 14.3, P= 0.04).

Conclusion Women who have not previously given birth vaginallyand those whose labour is induced with prostaglandin are atincreased risk of uterine rupture when attempting vaginal birthafter caesarean section. The risk of consequent death of theinfant is higher in units with lower annual numbers of births.

Introduction

Uterine rupture during attempted vaginal birth after a previouscaesarean section is a rare event that affects about one in200 women,¹ and consequent death of the infant is even rarer,affecting about one per 2000.² Analysis of the factors determiningperinatal death due to uterine rupture therefore requires datafrom large numbers of women. Most large scale databases of birthslack detailed information on the cause of perinatal death andthe obstetric characteristics of the population. Consequently,we know of no reports of the risk factors for perinatal deathdue to uterine rupture during attempted vaginal birth afterprevious caesarean section. We linked national registries ofpregnancy discharge data and perinatal death to determine thefactors associated with this event.

Methods

The inclusion criteria for the study were that a woman had previouslyhad one caesarean section and was delivered in her current pregnancyby a means other than planned caesarean section. We excludedwomen with more than one previous caesarean, those with multiplegestations, those delivering before 37 weeks' gestation, andthose delivering beyond 43 weeks' gestation. We also excludedcases in which the infant died from causes other than intrapartumuterine rupture.

Data sources—The Scottish Morbidity Record (SMR2) collectsinformation on clinical and demographic characteristics andoutcomes for all patients discharged from Scottish maternityhospitals. The register is subjected to regular quality assurancechecks and has been > 99% complete since the late 1970s.³The register collects both specific obstetric data and up tosix ICD-9 (international classification of diseases, ninth revision)or ICD-10 (10th revision) diagnostic codes relating to the admission.In 1996-7 a quality assurance analysis comparing 1414 recordswith the clinical notes showed that the register was free fromsignificant errors in > 98% of records in all the specificfields used in the present analysis. Exceptions were postcode(94.0%), height (96.2%), estimated gestation (94.4%), and methodof induction of labour (93.6%). The previous caesarean sectionfield was 99.7% accurate. ICD diagnostic codes were found tobe 80-90% accurate for the first four diagnoses and 70-80% accuratefor the remainder (Jim Chalmers, personal communication). SMR2records were linked to records from the Scottish Stillbirthand Infant Death Survey. This national register routinely classifiesall perinatal deaths in Scotland. Coding of the cause of deathis performed by a single medically qualified individual, andthe survey is described in detail elsewhere.⁴

Definitions—We defined trial of labour as a singletondelivery at term by a means other than planned caesarean sectionin women with only one previous caesarean delivery. The definitionof perinatal death due to uterine rupture was that the obstetriccause of death was coded as "mechanical" under the modifiedWigglesworth classification⁵ and that the ICD-9 diagnostic codefor intrapartum uterine rupture (665.1) was listed under thespecific diagnoses. Intrapartum uterine ruptures that did notresult in perinatal death were identified with ICD-9 and ICD-10diagnostic codes 665.1 and O711, respectively, from the diagnosticfields in the SMR2 record related to hospital discharge afterdelivery. Hospital throughput was defined as the total numberof births recorded in the SMR2 database for the given hospitalover the given year. Hospital throughput was categorised intoabove or below the median (3000 births). Other maternal characteristicswere defined as previously described.²

Statistical analyses—We summarised continuous variableswith medians and interquartile ranges and used the Mann-WhitneyU test for comparisons between groups and Fisher's exact testfor univariate comparisons of dichotomous data. P values forall hypothesis tests were two sided. Multivariate analysis wasperformed using logistic regression analysis. The significanceof interaction terms was assessed with the likelihood ratiotest. The goodness of fit of models was assessed with the Hosmerand Lemeshow test based on tenths of probability.⁶ Because ofthe rarity of the event we used exact logistic regression tomodel the risk of perinatal death due to uterine rupture.⁷ Whenwe treated annual number of births as a continuous variablein the exact model, we rounded it to the nearest 50 to makethe model computationally feasible. All statistical analyseswere performed with the Stata software package version 8.2 (StataCorp,College Station, TX), except for exact logistic regression,which was performed with LogXact version 5.0 (Cytel SoftwareCorporation, Cambridge, MA).

Results

There were 871 283 SMR2 birth records for Scotland for 1985-98.In total 39 729 (4.6%) women had had one previous caesareandelivery and were delivered by a means other than planned caesareansection. There were 452 (1.1%) multiple births, 3462 (8.7%)births outside the range of 37-43 weeks' gestation, and 543(1.4%) perinatal deaths due to causes other than intrapartumuterine rupture. We excluded a further 32 (< 0.1%) recordsbecause the women were documented as being primigravid, despitehaving had a previous caesarean delivery. We therefore excluded3875 (9.8%) records (some cases were excluded in more than onecategory), leaving a study group of 35 854. We compared thedemographic and obstetric characteristics of the study groupaccording to whether there was a perinatal death due to uterinerupture (table 1).

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Table 1 Maternal demographic and obstetric characteristics in relation to perinatal death due to uterine rupture. Figures are numbers (percentages) unless stated otherwise

There was no association between the annual number of deliveriesand the risk of emergency caesarean delivery (odds ratio 1.00,95% confidence interval 0.98 to 1.01, P = 0.58) or uterine ruptureoverall (0.98, 0.86 to 1.11, P = 0.70), but there was a significantnegative association with the risk of perinatal death due touterine rupture (0.68, 0.46 to 0.99, P = 0.04) (figure).

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Proportions of emergency caesarean section, all uterine rupture, and perinatal death due to uterine rupture, in relation to size of hospital

On univariate analysis, with the 35 854 women who attemptedvaginal birth as the denominator, the risk of uterine rupturewas higher in women who had not previously given birth vaginallyand in women who had been induced with prostaglandin but notwith other methods of induction (table 2). Though delivery ina hospital with < 3000 births a year was not associated withthe risk of uterine rupture overall, the other associationsremained highly significant in multivariate analysis and thepoint estimates were similar (table 3). There were enough uterineruptures for us to test the goodness of fit of the model andto examine interactions between the variables. The goodnessof fit was adequate (P > 0.05), and there were no significantfirst order interactions between any of the variables with eachother or with the year of birth.

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Table 2 Univariate obstetric associations with uterine rupture and perinatal death due to uterine rupture. Figures are numbers (percentages) unless stated otherwise

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Table 3 Multivariate analysis (with odds ratios and 95% confidence intervals) of risk of uterine rupture and perinatal death due to uterine rupture

The risk of perinatal death due to uterine rupture was alsohigher in women who had not previously given birth vaginallyand in women who had been induced with prostaglandins but notwith other methods of induction (table 2). However, in addition,delivery in a hospital with < 3000 births a year was associatedwith a significantly increased risk of perinatal death due touterine rupture. The risk of perinatal death was about one in1300 in hospitals with < 3000 births a year and one in 4700in hospitals with $≥$ 3000 births a year. Because of the smallnumber of deaths caused by uterine rupture, significance wasgenerally attenuated in multivariate analysis (table 3). However,the point estimates were similar to those from the univariateanalysis, indicating that the associations seen in univariateanalysis were not due to confounding by the factors includedin the model. There were too few events for us to assess goodnessof fit or first order interactions.

Among the 124 cases of uterine rupture, there were 17 (13.7%)intrapartum stillbirths or neonatal deaths. There were 63 uterineruptures in hospitals delivering < 3000 women per year and13 (20.6%) resulted in perinatal death. In hospitals delivering $≥$ 3000 women a year there were 61 uterine ruptures and four (6.6%)resulted in perinatal death (P=0.03). Among women with uterinerupture, the relative risk of perinatal death in a hospitalwith < 3000 births a year was about threefold (table 4).

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Table 4 Factors associated with perinatal death among women with documented uterine rupture. Figures are numbers (percentages) unless stated otherwise

When we confined the analysis to births $≥$ 40 weeks' gestation,the risk of uterine rupture was significantly associated withno previous vaginal birth (odds ratio 2.0, 95% confidence interval1.2 to 3.4, P = 0.009) and induction of labour with prostaglandin(2.2, 1.4 to 3.5, P = 0.001). Formal tests of interaction betweeneach of these variables and gestation $≥$ 40 weeks showed thatthe strength of the associations did not significantly differbefore and after 40 weeks (P = 0.2 and 0.3, respectively). Amongthe 22 170 births $≥$ 40 weeks' gestation, there were seven deathsout of 10 602 births in hospitals with < 3000 births a yearand one death out of 11 568 births in hospitals with $≥$ 3000 birthsa year (P=0.02).

Of the 12 633 women who had previously given birth vaginally,1499 (11.8%) were induced with prostaglandin compared with 2976of the 20 215 (12.8%) women who had not done so (P = 0.006).We used a logistic regression model to estimate the absoluterisk of uterine rupture (including cases in which the infantsurvived and cases in which the infant died) in relation todifferent combinations of parity and induction of labour withprostaglandin in relation to 1998 rates. Among women who hadnot previously given birth vaginally, the risk of uterine rupturewithout induction of labour with prostaglandin was one in 210and with induction of labour with prostaglandin was one in 71.Among women with a previous vaginal birth, the risk of uterinerupture without induction of labour with prostaglandin was onein 514 and with induction of labour with prostaglandin was onein 175.

Discussion

We found that after a previous caesarean section women who hadnot previously given birth vaginally and those who had labourinduced with prostaglandin were at increased risk of uterinerupture. The same two factors were associated with the riskof perinatal death due to uterine rupture. In contrast, deliveringin a hospital with low throughput was not associated with uterinerupture overall but was associated with an increased risk ofperinatal death due to uterine rupture. We found that uterinerupture was three times more likely to result in death of theinfant if the delivery took place in a hospital with < 3000births a year. Confining trials of labour to larger obstetricunits may therefore reduce the risk of perinatal death associatedwith uterine rupture during a trial of labour.

The finding that units with high throughput had lower ratesof perinatal death due to uterine rupture is plausible. Hospitalswith greater throughput are more likely to have resident obstetric,anaesthetic, and neonatal services as well as a dedicated obstetricoperating theatre. These factors would allow a faster responseto fetal distress due to uterine rupture, which in turn wouldallow more rapid delivery and resuscitation of the neonate.We did not have information on the structure of services ateach unit over the period of study. However, the factors arelikely to be highly correlated and interdependent. A unit withno resident obstetric or anaesthetic cover is unlikely to havea dedicated obstetric operating theatre or a resident experiencedneonatologist. Therefore, even if these data were available,it would be extremely difficult to determine the independentcontributions of each of these factors in reducing the riskof death. Therefore, the total number of births is a usefulcomposite measure of the level of support and has the pragmaticadvantage of being easy to define.

Study strengths and weaknesses
Previous large scale analyses of the factors determining uterinerupture could not reliably distinguish between asymptomaticdehiscence of the previous caesarean section scar and clinicallysignificant, symptomatic uterine rupture.^1
8
9 The failure todefine the event may lead to ascertainment bias. As asymptomaticdehiscence of the scar will generally be identified during asubsequent caesarean section, there will be increased ascertainmentof uterine rupture for any exposure that is associated withan increased risk of caesarean delivery. As we were able tostudy perinatal death due to uterine rupture, this allowed usto identify catastrophic rupture that would be ascertained irrespectiveof the mode of delivery. We conclude that the associations betweenuterine rupture and no previous vaginal birth and inductionof labour with prostaglandin are unlikely to be explained byascertainment bias. Previous studies have suggested that theprotective effect of a previous vaginal birth is observed whetherit preceded or followed the first caesarean delivery.¹⁰

Findings are comparable with previous studies
The estimates of absolute risk in the present analysis are comparablewith those from previous studies. The overall rate of successfulvaginal delivery of 74.2% is similar to the generally quotedoverall figure of 75%.¹¹ The overall rate of uterine ruptureof 0.35% is consistent with that reported in a previous largescale Swiss study.⁹ The overall risk of perinatal death dueto uterine rupture (one in 2100) is similar to the one in 2600reported in a study from Washington State, USA.¹ The risk amonglarge obstetric units (one per 4700) is similar to a case seriesfrom a large obstetric centre in California (one per 4200).¹²Although the total number of perinatal deaths in our study wasrelatively small (17), this is almost three times more thanreported in a recent meta-analysis of all previous studies.¹³Guise et al commented that the risk of death in Scotland, ascited from our previous report,² was 10 times higher than reportedin other studies.¹³ However, the figure they quoted was forperinatal death due to all causes related to delivery. The absoluterisk of death due to uterine rupture in our previous study (4.5per 10 000) was similar to the overall risk in our current analysis.Both fall within the 95% confidence intervals of the meta-analysis.We believe that the current data give the best estimate of theabsolute risk of perinatal death among women attempting vaginalbirth after caesarean.

A previous population based study had shown an association betweeninduction of labour with prostaglandin and uterine rupture.¹This finding led the American College of Obstetricians and Gynecologiststo recommend avoidance of prostaglandin in women with a previouscaesarean section. However, the number of women was small (366)and this was less than 2% of the study population. In the presentstudy, we had data on 4475 women who had labour induced withprostaglandin, which was 12.5% of our cohort. Our analyses confirmedthat induction of labour with prostaglandin, but not other methods,was independently associated with an increased risk of uterinerupture, including catastrophic rupture leading to perinataldeath. It remains to be determined whether this is due to aspecific pharmacological effect or whether the use of prostaglandinis merely a marker for a woman with an unfavourable cervix.

We defined trial of labour as any woman who had a single previouscaesarean birth who was delivered at term by a means other thanplanned caesarean section. The cohort studied probably includessome women who were due for planned repeat caesarean sectionbut attended in early labour, had an emergency caesarean delivery,and did not truly attempt vaginal birth. However, women deliveringat or after 40 weeks are unlikely to have requested plannedrepeat caesarean section. We found that the nature and strengthof associations in the present study were similar when we confinedanalyses to births at or after 40 weeks' gestation, and misclassificationof attempted vaginal birth is unlikely to have significantlyaffected our results.

Conclusion
In summary, we have shown that the risk of uterine rupture isincreased among women who have not previously given birth vaginallyand those undergoing induction of labour with prostaglandin.Our data show that the risk of consequent death of the infantis lower in obstetric units with higher throughput. Althoughother interpretations could be made, we believe the most plausibleexplanation for these findings is that the facilities generallyavailable at larger obstetric units reduce the risk of perinataldeath in the event of uterine rupture. The same is probablytrue of other obstetric emergencies. Perinatal deaths could,therefore, potentially be reduced by confining high risk birthsto large obstetric units or by providing additional facilitiesat smaller units.

What is already known on this topic

Attempting vaginal birthafter previous caesarean section (VBAC) carried the risk ofuterine rupture, which may result in perinatal death

No studiesto date have examined the factors associated with perinataldeath due to uterine rupture during attempted VBAC

No studiesto date have examined the organisation of health care and therisk of perinatal death due to uterine rupture during attemptedVBAC

What this study adds

For women attempting VBAC, no previousvaginal birth and induction of labour with prostaglandin wereassociated with uterine rupture resulting in perinatal death

Therisk of perinatal death due to uterine rupture was greater inhospitals with lower annual numbers of deliveries

Contributors: GCSS had the original idea. DP reviewed previouspublications. GCSS and DP undertook the statistical analysesand wrote the initial draft. RD performed the record linkage.GCSS, JPP, and DP agreed the study design, interpreted the results,and revised the original draft. All authors approved the finalversion. GCSS is the guarantor.

Funding: None.

Competing interests: None declared.

Ethical approval: Not required.

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(Accepted 3 June 2004)

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Perinatal death is more likely in women with previous caesareans if labour is induced with prostaglandin
BMJ 2004 329: 0. [Full Text]

Vaginal delivery after caesarean section: Jeanne-Marie Guise
BMJ 2004 329: 359-360. [Extract] [Full Text] [PDF]

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Smith, G. C.S., Pell, J. P., Kaplan, D. L., Gagnon, D. E., Muri, J. H., Shah, P. S., Landon, M. B., Leindecker, S., Spong, C. Y. (2005). Outcomes Associated with a Trial of Labor after Prior Cesarean Delivery. NEJM 352: 1718-1720 [Full text]
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