Prevention of fetal growth retardation with low-dose aspirin: findings of the EPREDA trial
- PMID: 1675315
- DOI: 10.1016/0140-6736(91)93124-r
Prevention of fetal growth retardation with low-dose aspirin: findings of the EPREDA trial
Abstract
The efficacy of low-dose aspirin in preventing fetal growth retardation was tested in a randomised, placebo-controlled, double-blind trial. A secondary aim was to find out whether dipyridamole improves the efficacy of aspirin. 323 women at 15-18 weeks' amenorrhoea were selected at twenty-five participating centres on the basis of fetal growth retardation and/or fetal death or abruptio placentae in at least one previous pregnancy. They were randomly allocated to groups receiving placebo, 150 mg/day aspirin, or 150 mg/day aspirin plus 225 mg/day dipyridamole, for the remainder of the pregnancy. In the first phase of the trial all actively treated patients (n = 156) were compared with the placebo group (n = 73). Mean birthweight was significantly higher in the treated than in the placebo group (2751 [SD 670] vs 2526 [848] g; difference 225 g [95% CI 129-321 g], p = 0.029) and the frequency of fetal growth retardation in the placebo group was twice that in the treated group (19 [26%] vs 20 [13%]; p less than 0.02). The frequencies of stillbirth (4 [5%] vs 2 [1%]) and abruptio placentae (6 [8%] vs 7 [5%]) were also higher in the placebo than in the treated group. The benefits of aspirin treatment were greater in patients with two or more previous poor outcomes than in those with only one. In the second analysis, of aspirin only (n = 127) vs aspirin plus dipyridamole (n = 119), no significant differences were found. There was no excess of maternal or neonatal side-effects in the aspirin-treated patients.
Comment in
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Low-dose aspirin and nulliparae.Lancet. 1991 Aug 3;338(8762):324. doi: 10.1016/0140-6736(91)90471-z. Lancet. 1991. PMID: 1677150 Clinical Trial. No abstract available.
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Low-dose aspirin during pregnancy.Lancet. 1991 Aug 31;338(8766):579. doi: 10.1016/0140-6736(91)91152-k. Lancet. 1991. PMID: 1678840 No abstract available.
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