Kelly Anthony J, Malik Sidra, Smith Lee, Kavanagh Josephine, Thomas Jane
Department of Obstetrics and Gynaecology, Brighton and Sussex University Hospitals NHS Trust, Royal Sussex County Hospital, Eastern Road, Brighton, UK, BN2 5BE.
Cochrane Database Syst Rev. 2009 Oct 7(4):CD003101. doi: 10.1002/14651858.CD003101.pub2.
Prostaglandins have been used for induction of labour since the 1960s. Initial work focused on prostaglandin F2a as prostaglandin E2 was considered unsuitable for a number of reasons. With the development of alternative routes of administration, comparisons were made between various formulations of vaginal prostaglandins.
To determine the effects of vaginal prostaglandins E2 and F2a for third trimester cervical ripening or induction of labour in comparison with placebo/no treatment or other vaginal prostaglandins (except misoprostol).
We searched the Cochrane Pregnancy and Childbirth Group's Trials Register (May 2009) and bibliographies of relevant papers.
Clinical trials comparing vaginal prostaglandins used for third trimester cervical ripening or labour induction with placebo/no treatment or other methods listed above it on a predefined list of labour induction methods.
We assessed studies and extracted data independently.
Sixty-three (10,441 women) have been included.Vaginal prostaglandin E2 compared with placebo or no treatment reduced the likelihood of vaginal delivery not being achieved within 24 hours (18.1% versus 98.9%, risk ratio (RR) 0.19, 95% confidence interval (CI) 0.14 to 0.25, two trials, 384 women). The risk of the cervix remaining unfavourable or unchanged was reduced (21.6% versus 40.3%, RR 0.46, 95% CI 0.35 to 0.62, five trials, 467 women); and the risk of oxytocin augmentation reduced (35.1% versus 43.8%, RR 0.83, 95% CI 0.73 to 0.94, 12 trials, 1321 women) when PGE2 was compared to placebo. There was no evidence of a difference between caesarean section rates, although the risk of uterine hyperstimulation with fetal heart rate changes was increased (4.4% versus 0.49%, RR 4.14, 95% CI 1.93 to 8.90, 14 trials, 1259 women).PGE2 tablet, gel and pessary appear to be as efficacious as each other and the use of sustained release PGE2 inserts appear to be associated with a reduction in instrumental vaginal delivery rates (9.9 % versus 19.5%, RR 0.51, 95% CI 0.35 to 0.76, NNT 10 (6.7 to 24.0), five trials, 661 women) when compared to vaginal PGE2 gel or tablet.
AUTHORS' CONCLUSIONS: PGE2 increases successful vaginal delivery rates in 24 hours and cervical favourability with no increase in operative delivery rates. Sustained release vaginal PGE2 is superior to vaginal PGE2 gel with respect to some outcomes studied.Further research is needed to assess the best vehicle for delivering vaginal prostaglandins and this should, where possible, include some examination of the cost-analysis.
自20世纪60年代以来,前列腺素一直被用于引产。最初的研究集中在前列腺素F2α,因为前列腺素E2由于多种原因被认为不适用。随着给药途径的发展,人们对各种阴道用前列腺素制剂进行了比较。
与安慰剂/未治疗或其他阴道用前列腺素(米索前列醇除外)相比,确定阴道用前列腺素E2和F2α用于孕晚期宫颈成熟或引产的效果。
我们检索了Cochrane妊娠与分娩组试验注册库(2009年5月)以及相关论文的参考文献。
将用于孕晚期宫颈成熟或引产的阴道用前列腺素与安慰剂/未治疗或在预定义引产方法列表中位于其上方的其他方法进行比较的临床试验。
我们独立评估研究并提取数据。
共纳入63项研究(10441名女性)。与安慰剂或未治疗相比,阴道用前列腺素E2降低了24小时内未实现阴道分娩的可能性(18.1%对98.9%,风险比(RR)0.19,95%置信区间(CI)0.14至0.25,两项试验,384名女性)。宫颈仍未成熟或未改变的风险降低(21.6%对40.3%,RR 0.46,95%CI 0.35至0.62,五项试验,467名女性);与安慰剂相比,当使用前列腺素E2时,催产素增加的风险降低(35.1%对43.8%,RR 0.83,95%CI 0.73至0.94,12项试验,1321名女性)。虽然伴有胎儿心率变化的子宫过度刺激风险增加(4.4%对0.49%,RR 4.14,95%CI 1.93至8.90,14项试验,1259名女性),但剖宫产率没有差异的证据。前列腺素E2片剂凝胶和阴道环似乎彼此疗效相同,与阴道用前列腺素E2凝胶或片剂相比,使用缓释前列腺素E2阴道环似乎与器械助产阴道分娩率降低有关(9.9%对19.5%,RR 0.51,95%CI 0.35至0.76,需治疗人数10(6.7至24.0),五项试验,661名女性)。
前列腺素E2可提高24小时内成功阴道分娩率和宫颈成熟度,且手术分娩率无增加。就所研究的一些结果而言,缓释阴道用前列腺素E2优于阴道用前列腺素E2凝胶。需要进一步研究以评估递送阴道用前列腺素的最佳载体,并且在可能的情况下,这应包括对成本分析的一些考察。
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