Leung H H Y, Papastefanou I, Chen Y, Nguyen-Hoang L, Nguyen D-A, Dinh L T, Pooh R K, Shiozaki A, Zheng M, Hu Y, Wu Y, Kusuma A, Yapan P, Gosavi A, Sekizawa A, Luewan S, Chang T-Y, Chaiyasit N, Nanthakomon T, Liu H, Shaw S W, Leung W C, Mohamad A S, Aguilar A, Lau S L, Lee N M W, Lin J, Sahota D S, Chong M K C, Poon L C
Department of Obstetrics and Gynaecology, Prince of Wales Hospital, The Chinese University of Hong Kong, Hong Kong, SAR, China.
Department of Women and Children's Health, School of Life Course and Population Sciences, Faculty of Life Sciences & Medicine, King's College London, London, UK.
Ultrasound Obstet Gynecol. 2025 Jul;66(1):24-32. doi: 10.1002/uog.29255. Epub 2025 Jun 2.
To investigate the impact of aspirin administration on the incidence of preterm birth, according to the type of delivery and gestational age at preterm birth, and to examine the hypothesis that aspirin delays preterm delivery.
This was a secondary analysis of a multicenter stepped-wedge cluster randomized trial of a first-trimester screen-and-prevent strategy for preterm pre-eclampsia (PE), which included 18 maternity/diagnostic units in 10 regions across Asia between 1 August 2019 and 28 February 2022. Women deemed to be at high risk for preterm PE according to a Bayes' theorem-based triple test, i.e. those with an adjusted risk for preterm PE of ≥ 1 in 100, received low-dose aspirin from < 16 weeks until 36 weeks' gestation. Outcome measures were the incidence of early preterm birth (24 + 0 to 31 + 6 weeks' gestation) and late preterm birth (32 + 0 to 36 + 6 weeks). The treatment effect of aspirin on the rate of preterm birth, stratified by gestational age at birth, type of delivery and presence of pregnancy complications, was estimated by computing the relative risks (RR) between the aspirin and non-aspirin groups with their 95% CIs. A shift model was designed to evaluate the effect of aspirin on preterm birth, based on the hypothesis that aspirin delays a preterm birth to a more advanced gestational age.
In the randomized trial, 42 897/48 647 women accepted screening for preterm PE. Following exclusions, 10 294 and 27 965 women were included in the non-intervention and intervention phases, respectively. Of the 4688 women at high risk for preterm PE, 2909 (62.05%) received aspirin in the trial. Aspirin was associated with a 42% reduction in the risk of early preterm birth (adjusted relative risk (aRR), 0.577 (95% CI, 0.380-0.852)), and there was a significant upward trend in the rate of late preterm birth accordingly (test for trend, P < 0.01). Similar findings were observed for iatrogenic preterm birth and pregnancies with a small-for-gestational-age neonate. Additionally, aspirin was associated with a 60% reduction in the risk of iatrogenic early preterm birth in pregnancies with PE (aRR, 0.398 (95% CI, 0.192-0.788)). However, aspirin did not have a significant effect on iatrogenic late preterm birth in pregnancies with PE. Aspirin significantly delayed early preterm birth, with the effect decreasing by 0.26 (95% credibility interval, -0.40 to -0.05) weeks for each week of advancing gestation. At 24 weeks, aspirin delayed delivery by 3.63 weeks, while at 37 weeks, the delay was only 0.25 weeks.
This secondary explanatory analysis found that early administration of aspirin could effectively reduce the risk of early preterm birth in women at high risk for preterm PE. While the reasons for preterm birth are often multifactorial, this study provides greater insight into the relationship between aspirin and different types of preterm birth at different gestational ages. Our findings support the hypothesis that aspirin helps to prevent preterm birth by delaying the timing of delivery, with a greater impact observed for deliveries that would have occurred at an earlier gestational age had aspirin not been administered. © 2025 The Author(s). Ultrasound in Obstetrics & Gynecology published by John Wiley & Sons Ltd on behalf of International Society of Ultrasound in Obstetrics and Gynecology.
根据分娩类型和早产时的孕周,研究阿司匹林给药对早产发生率的影响,并检验阿司匹林可延迟早产这一假设。
这是一项对多中心阶梯楔形整群随机试验的二次分析,该试验针对早发型子痫前期(PE)的孕早期筛查与预防策略,于2019年8月1日至2022年2月28日期间在亚洲10个地区的18个产科/诊断单位进行。根据基于贝叶斯定理的三联检测被认为早产PE高危的女性,即早产PE校正风险≥1/100的女性,从妊娠<16周开始至妊娠36周接受低剂量阿司匹林治疗。观察指标为早期早产(妊娠24⁺⁰至31⁺⁶周)和晚期早产(妊娠32⁺⁰至36⁺⁶周)的发生率。通过计算阿司匹林组和非阿司匹林组之间的相对风险(RR)及其95%可信区间,评估阿司匹林对早产率的治疗效果,按出生孕周、分娩类型和妊娠并发症的存在进行分层。基于阿司匹林将早产延迟至更晚期孕周的假设,设计了一个移位模型来评估阿司匹林对早产的影响。
在随机试验中,42897/48647名女性接受了早产PE筛查。排除后,分别有10294名和27965名女性纳入非干预期和干预期。在4688名早产PE高危女性中,2909名(62.05%)在试验中接受了阿司匹林治疗。阿司匹林使早期早产风险降低42%(校正相对风险(aRR),0.577(95%可信区间,0.380 - 0.852)),相应地晚期早产率有显著上升趋势(趋势检验,P<0.01)。对于医源性早产和小于胎龄儿的妊娠也观察到类似结果。此外,阿司匹林使PE妊娠中医源性早期早产风险降低60%(aRR,0.398(95%可信区间,0.192 - 0.788))。然而,阿司匹林对PE妊娠中医源性晚期早产没有显著影响。阿司匹林显著延迟了早期早产,随着孕周增加,每周延迟效果降低0.26(95%可信区间,-0.40至-0.05)周。在24周时,阿司匹林使分娩延迟3.63周,而在37周时,延迟仅0.25周。
这项二次解释性分析发现,早期给予阿司匹林可有效降低早产PE高危女性的早期早产风险。虽然早产原因通常是多因素的,但本研究更深入地洞察了阿司匹林与不同孕周不同类型早产之间的关系。我们的研究结果支持阿司匹林通过延迟分娩时间有助于预防早产这一假设,对于如果未服用阿司匹林会在更早孕周发生的分娩,观察到的影响更大。©2025作者。《妇产科超声》由约翰·威利父子有限公司代表国际妇产科超声学会出版。
