Intramuscular versus intravenous prophylactic oxytocin for postpartum hemorrhage after vaginal delivery: a randomized controlled study

Dağdeviren, Hediye; Cengiz, Hüseyin; Heydarova, Ulkar; Çaypınar, Sema Süzen; Kanawati, Ammar; Guven, E.S. dag; Ekin, Murat

doi:10.1007/s00404-016-4060-7

Cited by 17 publications

(24 citation statements)

References 15 publications

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“…Blinding of the clinicians, participants, and researchers was not mentioned and no difference was found in measured blood loss or PPH 27. The other study compared oxytocin 10 IU intravenous at 1 mL/min with oxytocin 10 IU intramuscularly 28. Birth attendants and participants were not blinded but the research team who performed the measurement of blood loss were blinded.…”

Section: Discussionmentioning

confidence: 99%

Intramuscular versus intravenous oxytocin to prevent postpartum haemorrhage at vaginal delivery: randomised controlled trial

Adnan

Conlan-Trant

McCormick

et al. 2018

BMJ

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ObjectiveTo determine whether intravenous oxytocin is more effective than intramuscular oxytocin at preventing postpartum haemorrhage at vaginal delivery.DesignDouble blind placebo controlled randomised trial.SettingUniversity affiliated maternity unit in the Republic of Ireland.Participants1075 women aged 18 years or older, at term with a singleton pregnancy who were aiming for a vaginal delivery with an actively managed third stage of labour.InterventionsWomen were allocated to an intravenous bolus of oxytocin (10 IU in 1 mL given slowly over one minute) and placebo intramuscular injection (1 mL 0.9% saline) or an intramuscular bolus of oxytocin (10 IU in 1 mL) and placebo intravenous injection (1 mL 0.9% saline given slowly over one minute) at vaginal delivery. Allocation was by a secure web based randomisation service with masking of participants and clinicians to the trial intervention.Main outcome measuresThe primary outcome was postpartum haemorrhage (PPH, measured blood loss ≥500 mL). Secondary outcomes were severe PPH (measured blood loss ≥1000 mL), need for blood transfusion, admission to a high dependency unit, and side effects to oxytocin.ResultsBetween 4 January 2016 and 13 December 2017, 1075 women were randomised and 1035 (96.3%) included in the primary and secondary analyses (517 in the intravenous oxytocin group and 518 in the intramuscular oxytocin group). The incidence of PPH was not significantly lower in the intravenous group (18.8%, 97/517) compared with intramuscular group (23.2%, 120/518): adjusted odds ratio 0.75 (95% confidence interval 0.55 to 1.03). The incidence of severe PPH, however, was significantly lower in the intravenous group (4.6%, 24/517) compared with intramuscular group (8.1%, 42/518): 0.54 (0.32 to 0.91) as was the need for blood transfusion (1.5% v 4.4%, 0.31, 0.13 to 0.70) and admission to a high dependency unit (1.7% v 3.7%, 0.44, 0.20 to 0.98). The number needed to treat to prevent one case of severe PPH was 29 (95% confidence interval 16 to 201) and to prevent one case of blood transfusion was 35 (20 to 121). The incidence of side effects to oxytocin was not increased in the intravenous group compared with intramuscular group (4.1% v 5.2%, 0.75, 0.42 to 1.35).ConclusionIntravenous oxytocin for the third stage of labour results in less frequent severe PPH, blood transfusion, and admission to a high dependency unit than intramuscular oxytocin, and without excess side effects.Trial registrationCurrent Controlled Trials ISRCTN14718882.

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Section: Discussionmentioning

confidence: 99%

Intramuscular versus intravenous oxytocin to prevent postpartum haemorrhage at vaginal delivery: randomised controlled trial

Adnan

Conlan-Trant

McCormick

et al. 2018

BMJ

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“…Four trials were considered to have an unclear risk of selection bias as the methods to describe adequate random sequence generation were not reported or inadequately described [14,15,28,42]. There was an unclear risk for five trials [19,28,29,35,39] concerning allocation concealment as it was not reported appropriately. The Diop 2016 [11] and Raghavan 2015 [21] trials were cluster randomised trials meaning allocation would have been known in advance so were judged to be high risk for inadequate allocation concealment.…”

Section: Risk Of Bias Of Included Trialsmentioning

confidence: 99%

“…Detection bias showed similar results with 50% of trials deemed low risk, 17% unclear and 33% high risk. The large number of trials judged to be unclear or high risk for performance and detection bias were commonly due to difficult blinding participants and personnel to interventions due to the differences in administration [11,16,19,21,22,31,32,35,39,41,42,44], unclear reporting of methods [28,29] and a likelihood that blinding could be broken [18,20]. The Deneux-Tharaux 2013 [32] and Groot 1996 [44] trials were judged to be high risk of performance bias but low and unclear risk of detection bias, respectively, due to the use of objective measurements for the primary outcome.…”

Section: Risk Of Bias Of Included Trialsmentioning

confidence: 99%

“…Grade 1 included 11 trials and had a random effects pooled proportion of 0.10 (95% CI = 0.042 to 0.18), with high heterogeneity (p < 0.0001; I 2 = 99.1%; 95% CI = 98.9 to 99.2%) (Additional file 2: Figure S1) [12, 13, 17-19, 21, 22, 26, 28, 38, 44]. Grade 2 included four trials and had a random effects pooled proportion of 0.15 (95% CI = 0.067 to 0.26), with high heterogeneity (p < 0.0001; I 2 of 96.6%; 95% CI = 94.6 to 97.7%) (Additional file 2: Figure S2) [16,24,35,41]. Grade 3 included two trials and had a random effects pooled proportion of 0.14 (95% CI = 0.095 to 0.18), with medium heterogeneity (p = 0.07; I 2 = 69.6%) (Additional file 2: Figure S3) [29,42].…”

Section: Primary Outcomes Proportion Analysis For Minor Pph Gradesmentioning

confidence: 99%

“…Grade 1 [12,13,18,26,38,44]. Grade 2 included three trials and had a random pooled proportion of 0.033 (95% CI 0.012 to 0.063), with high heterogeneity (p = 0.004; I 2 = 81.9%; 95%CI = 0 to 92.3%) (Additional file 3: Figure S2) [16,35,41]. Grade 3 included one trial with a proportion of 0.020 (95% CI = 0.014 to 0.027) (Additional file 3: Figure S3) [42].…”

Section: Proportion Analysis For Major Pph Gradesmentioning

confidence: 99%

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Postpartum haemorrhage (PPH) rates in randomized trials of PPH prophylactic interventions and the effect of underlying participant PPH risk: a meta-analysis

Hawker

Weeks

2020

BMC Pregnancy Childbirth

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Background: Postpartum haemorrhage (PPH) remains a leading cause of maternal mortality. Many trials assessing interventions to prevent PPH base their data on low risk women. It is important to consider the impact data collection methods may have on these results. This review aims to assess trials of PPH prophylaxis by grading trials according to the degree of risk status of the population enrolled in these trials and identify differences in the PPH rates of low risk and high risk populations. Methods: Systematic review and meta-analysis using a random-effects model. Trials were identified through CENTRAL. Trials were assessed for eligibility then graded according to antenatal risk factors and method of birth into five grades. The main outcomes were overall trial rate of minor PPH (blood loss ≥500 ml) and major PPH (> 1000 ml) and method of determining blood loss (estimated/measured).

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Intramuscular versus intravenous prophylactic oxytocin for the third stage of labour

Oladapo

Okusanya

Ábalos

2018

Cochrane Database of Systematic Reviews

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Intramuscular versus intravenous prophylactic oxytocin for postpartum hemorrhage after vaginal delivery: a randomized controlled study

Abstract: Using oxytocin by intravenous and intramuscular route has a similar efficacy and adverse effects.

Cited by 17 publications

References 15 publications

Intramuscular versus intravenous oxytocin to prevent postpartum haemorrhage at vaginal delivery: randomised controlled trial

Intramuscular versus intravenous oxytocin to prevent postpartum haemorrhage at vaginal delivery: randomised controlled trial

Postpartum haemorrhage (PPH) rates in randomized trials of PPH prophylactic interventions and the effect of underlying participant PPH risk: a meta-analysis

Intramuscular versus intravenous prophylactic oxytocin for the third stage of labour

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