Asadi, Nasrin; Vafaei, Homeira; Hessami, Kamaran; Darabi, Mohammad Hasan; Kasraeian, Maryam; Faraji, Azam; Alavi, Azin; Abdi, Nazanin; Gissuei, Atena; Roozmeh, Shohre; Bazrafshan, Khadije; Gharibpour, Fereshteh

doi:10.1111/jog.15180

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Title: Vaginal misoprostol and intravenous oxytocin for success of termination in the second‐trimester intrauterine fetal demise: A randomized controlled clinical trial.
Authors: Asadi, Nasrin; Vafaei, Homeira; Hessami, Kamaran; Darabi, Mohammad Hasan; Kasraeian, Maryam; Faraji, Azam; Alavi, Azin; Abdi, Nazanin; Gissuei, Atena; Roozmeh, Shohre; Bazrafshan, Khadije; Gharibpour, Fereshteh
Abstract: Aim: To compare the success rate of vaginal misoprostol versus intravenous (IV) oxytocin in termination of pregnancy in the second trimester intrauterine fetal death (IUFD). Methods: This was an open‐label randomized controlled study for 106 women with second trimester IUFD. Patients were randomly divided into two groups: women given vaginal misoprostol (400 mcg every 6 h up to 48 h) versus those given IV oxytocin (starting with 50 units up to a maximum of 300 units). When the first‐line treatment (as mentioned above) failed, treatment methods were replaced with each other. When the second‐line treatment failed, the patients underwent dilation and evacuation. Results: The first‐line treatment yielded the successful rate of 88.7% versus 73.7% for misoprostol versus oxytocin, respectively (p = 0.047). Among those with first‐line treatment failure, the second‐line treatment yielded success rate of 85.7% versus 83.3% for misoprostol versus oxytocin (p = 0.891). The mean duration of induction to delivery in women with successful response to first‐line treatment was 28.72 and 20.55 h after initially receiving misoprostol versus oxytocin, respectively (p < 0.001). While during second‐line treatment, this mean interval was not significantly different among those with misoprostol versus oxytocin (p = 0.128). No severe adverse events were observed. Conclusion: Vaginal misoprostol was associated with higher termination rate than oxytocin without adverse events when used as the first‐line treatment. Both methods yielded the same success rate when used as the second‐line treatment.
Subjects: OXYTOCIN; INTRAVENOUS therapy; DILATATION & curettage; ABORTION; TREATMENT effectiveness; RANDOMIZED controlled trials; PERINATAL death; MISOPROSTOL; VAGINAL medication; SECOND trimester of pregnancy; STATISTICAL sampling
Publication: Journal of Obstetrics & Gynaecology Research, 2022, Vol 48, Issue 4, p966
ISSN: 1341-8076
Publication type: Academic Journal
DOI: 10.1111/jog.15180

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Vaginal misoprostol and intravenous oxytocin for success of termination in the second‐trimester intrauterine fetal demise: A randomized controlled clinical trial.

Asadi, Nasrin; Vafaei, Homeira; Hessami, Kamaran; Darabi, Mohammad Hasan; Kasraeian, Maryam; Faraji, Azam; Alavi, Azin; Abdi, Nazanin; Gissuei, Atena; Roozmeh, Shohre; Bazrafshan, Khadije; Gharibpour, Fereshteh

OXYTOCIN; INTRAVENOUS therapy; DILATATION & curettage; ABORTION; TREATMENT effectiveness; RANDOMIZED controlled trials; PERINATAL death; MISOPROSTOL; VAGINAL medication; SECOND trimester of pregnancy; STATISTICAL sampling

Journal of Obstetrics & Gynaecology Research, 2022, Vol 48, Issue 4, p966

1341-8076

Academic Journal

10.1111/jog.15180