Dodd Jodie M, Crowther Caroline A
School of Paediatrics and Reproductive Health, Discipline of Obstetrics and Gynaecology, The University of Adelaide, Women's and Children's Hospital, 72 King William Road, Adelaide, South Australia, Australia, 5006.
Cochrane Database Syst Rev. 2010 Apr 14;2010(4):CD004901. doi: 10.1002/14651858.CD004901.pub2.
A woman may need to give birth prior to the spontaneous onset of labour in situations where the fetus has died in utero (also called a stillbirth), or for the termination of pregnancy where the fetus, if born alive would not survive or would have a permanent handicap. Misoprostol is a prostaglandin medication that can be used to induce labour in these situations.
To compare the benefits and harms of misoprostol to induce labour to terminate pregnancy in the second and third trimester for women with a fetal anomaly or after intrauterine fetal death when compared with other methods of induction of labour.
We searched the Cochrane Pregnancy and Childbirth Group's Trials Register (November 2009).
Randomised controlled trials comparing misoprostol with placebo or no treatment, or any other method of induction of labour, for women undergoing induction of labour to terminate pregnancy in the second and third trimester following an intrauterine fetal death or for fetal anomalies.
Both authors independently assessed trial quality and extracted data.
We included 38 studies (3679 women).Nine studies included pregnancies after intrauterine deaths, five studies included termination of pregnancies because of fetal anomalies when the fetus was still alive and the rest (24) presented the pooled data for intrauterine deaths, fetal anomalies and social reasons.When compared with agents that have traditionally been used to induce labour in this setting (for example, gemeprost, prostaglandin E(2) and prostaglandin F(2alpha)), vaginal misoprostol is as effective in ensuring vaginal birth within 24 hours, with a similar induction to birth interval. Vaginal misoprostol is associated with a reduction in the occurrence of maternal gastrointestinal side effects such as nausea, vomiting and diarrhoea when compared with other prostaglandin preparations. While the different treatments involving various prostaglandin preparations appear comparable for the reported outcomes, the information available regarding rare maternal complications, such as uterine rupture, is limited.
AUTHORS' CONCLUSIONS: The use of vaginal misoprostol in the termination of second and third trimester of pregnancy is as effective as other prostaglandin preparations (including cervagem, prostaglandin E(2) and prostaglandin F(2alpha)), and more effective than oral administration of misoprostol. However, important information regarding maternal safety, and in particular the occurrence of rare outcomes such as uterine rupture, remains limited. Future research efforts should be directed towards determining the optimal dose and frequency of administration, with particular attention to standardised reporting of all relevant outcomes and assessment of rare adverse events. Further information is required about the use of sublingual misoprostol in this setting.
在胎儿死于子宫内(也称为死产)的情况下,或者在胎儿如果存活出生后无法存活或会有永久性残疾而需要终止妊娠的情况下,女性可能需要在自然分娩开始前分娩。米索前列醇是一种前列腺素药物,可用于在这些情况下引产。
与其他引产方法相比,比较米索前列醇引产在妊娠中期和晚期终止妊娠的益处和危害,这些情况包括胎儿异常或宫内胎儿死亡后的引产。
我们检索了Cochrane妊娠与分娩组试验注册库(2009年11月)。
随机对照试验,比较米索前列醇与安慰剂或不治疗,或任何其他引产方法,用于在宫内胎儿死亡后或因胎儿异常而在妊娠中期和晚期引产以终止妊娠的女性。
两位作者独立评估试验质量并提取数据。
我们纳入了38项研究(3679名女性)。9项研究纳入了宫内死亡后的妊娠,5项研究纳入了因胎儿异常而终止妊娠(此时胎儿仍存活)的情况,其余24项研究呈现了宫内死亡、胎儿异常和社会原因的汇总数据。与传统上用于这种情况下引产的药物(如吉美前列素、前列腺素E2和前列腺素F2α)相比,阴道用米索前列醇在确保24小时内阴道分娩方面同样有效,引产至分娩间隔相似。与其他前列腺素制剂相比,阴道用米索前列醇可降低母体胃肠道副作用如恶心、呕吐和腹泻的发生率。虽然涉及各种前列腺素制剂的不同治疗方法在报告的结果方面似乎相当,但关于罕见母体并发症(如子宫破裂)的可用信息有限。
在妊娠中期和晚期终止妊娠时使用阴道用米索前列醇与其他前列腺素制剂(包括卡孕栓、前列腺素E2和前列腺素F2α)同样有效,且比口服米索前列醇更有效。然而,关于母体安全性的重要信息,特别是罕见结局(如子宫破裂)的发生情况,仍然有限。未来的研究应致力于确定最佳剂量和给药频率,尤其要注意所有相关结局的标准化报告以及罕见不良事件的评估。关于舌下含服米索前列醇在这种情况下的使用还需要更多信息。