Effectiveness and safety of the oxytocin antagonist atosiban versus beta‐adrenergic agonists in the treatment of preterm labour

医学 生育力抑制剂 催产素 催产素 不利影响 利托君 特布他林 人口 胎龄 沙丁胺醇 麻醉 产科 妊娠期 怀孕 内科学 早产 遗传学 环境卫生 哮喘 生物
作者
J.M. Moutquin,D. Cabrol,Nicholas M. Fisk,A. H. MacLennan,Karel Maršál,Jaron Rabinovici
出处
期刊:Bjog: An International Journal Of Obstetrics And Gynaecology [Wiley]
卷期号:108 (2): 133-142 被引量:230
标识
DOI:10.1111/j.1471-0528.2001.00043.x
摘要

Objective To compare the effectiveness and safety of the oxytocin antagonist atosiban with conventional beta‐adrenergic agonist (beta‐agonist) therapy in the treatment of preterm labour. Design Three multinational, multicentre, double‐blind, randomised, controlled trials. Setting Hospitals in Australia, Canada, Czech Republic, Denmark, France, Israel, Sweden, and the UK. Population Women diagnosed with preterm labour at 23–33 completed weeks of gestation. Methods Seven hundred and forty‐two women were randomised; 733 received atosiban ( n =363; intravenous (iv) bolus dose of 6.75 mg, then 300 μg/minute iv. for 3h and 100 μg/min iv thereafter) or beta‐agonist ( n =379; ritodrine, salbutamol or terbutaline iv; dose titrated) for at least 18h and up to 48 hours. Uterine contraction rate, cervical dilatation and effacement were used to assess progression of labour. An all patients treated analysis, using the Cochran‐Mantel‐Haenszel test, was performed. Main outcome measures Tocolytic effectiveness was assessed in terms of the number of women undelivered after 48 hours and seven days. Safety was assessed in terms of maternal side effects and neonatal morbidity. Results There were no significant differences between atosiban and β ‐agonists in delaying delivery for 48h (88.1% vs 88.9%; P =0.99) or seven days (79.7% versus 77.6%; P =0.28). Tocolytic effectiveness was also similar in terms of mean [SD] gestational age at delivery (35.8 [3.9] weeks vs 35.5 [4.1] weeks) and mean [SD] birthweight (2491 [813] g versus 2461 [831] g). Maternal side effects, particularly cardiovascular adverse events (8.3% vs 81.2%, P < 0.001 ), were reported more frequently in women given β ‐agonists, resulting in more treatment discontinuations due to side effects (1.1% vs 15.4%, P =0.0001). No statistical differences in neonatal/infant outcomes were observed with either study medication. Conclusions In the largest study of tocolytic therapy to date, atosiban was comparable in clinical effectiveness to conventional beta‐agonist therapy, but was associated with fewer maternal cardiovascular side effects. We conclude that atosiban has clinical advantages over current tocolytic therapy.
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