胎盘输血对母亲的影响。

Arpitha Chiruvolu, Emily Estes, Karen C Stanzo, Sujata Desai, Brandon C Cornelius
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引用次数: 3

摘要

目的:虽然有充分的证据支持新生儿延迟脐带夹紧(DCC),但与DCC相关的产妇结局数据相对较少。此外,结果,如产后出血(PPH),大多报道了无并发症的足月阴道分娩。本研究的目的是介绍两个主要的产妇结局,PPH的发病率和红细胞压积的变化,在复杂的早产和足月剖宫产的分娩前后。研究设计:自2013年8月在我们的分娩医院以分步方式实施胎盘输血过程以来,前瞻性地收集产妇数据。这些关于单胎极早产、中度早产、极早产双胎妊娠、晚期早产和足月剖宫产合并DCC或脐带挤奶(UCM)的数据与分别采用立即脐带夹紧(ICC)分娩的回顾性队列进行了比较。结果:与非常早产的单胎分娩相比,ICC组和DCC组PPH的发生率相似(2.3% vs. 1.7%)。分娩前后平均红细胞压积变化(3.06±1.32∶3.47±1.52)无显著差异。45 s DCC组与60 s DCC组比较,PPH发生率(1.7% vs. 4.8%)和分娩前后红细胞压积变化(3.47±1.52 vs. 4.32±1.88)无显著差异。当比较回顾性ICC队列和前瞻性DCC队列延迟60 s极早产双胎分娩时,两组均未观察到PPH。分娩前后平均红细胞比容变化(5.5±3.3 vs. 5.8±3.9)无显著差异。当比较妊娠32°至346周的中度和早期晚期早产时,产前和产后PPH发生率(0.9% vs. 0%)或红细胞压积变化(4.2±2.3 vs. 4.8±2.9)之间没有差异。与晚期早产儿(妊娠35°和366周)相比,PPH的发生率(13% vs. 11.4%)或分娩前后平均红细胞压积变化(5.0±3.0 vs. 5.1±2.8)无显著差异。在剖宫产足月分娩中,回顾性ICC组PPH发生率为2.2%,前瞻性UCM组为1.4%。分娩前后平均红细胞压积变化无差异(5.9±3.7 vs. 6.2±2.8)。结论:DCC或UCM与极早产单胎、中度早产、极早产双胎、晚期早产和足月剖宫产分娩前后PPH风险增加或母体红细胞压积显著变化无关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The effects of placental transfusion on mothers.

Objective: While there is ample evidence supporting delayed cord clamping (DCC) in neonates, the data on the maternal outcomes related to DCC are relatively sparse. Moreover, the outcomes, such as postpartum hemorrhage (PPH), were mostly reported for uncomplicated term vaginal deliveries. The objective of this study was to present the two primary maternal outcomes, incidence of PPH and change in hematocrit pre- and post-delivery in complex situations of preterm deliveries and term cesarean sections.

Study design: Maternal data were collected prospectively since the placental transfusion process was implemented in a step-wise fashion in our delivery hospitals, starting August, 2013. These data on very preterm singleton, moderate preterm, very preterm twin gestation, late preterm deliveries and term cesarean sections with DCC or umbilical cord milking (UCM) were compared with respective retrospective cohorts of deliveries in which immediate cord clamping (ICC) was performed.

Results: Comparing very preterm singleton deliveries, the incidence of PPH was similar between the ICC and DCC groups (2.3% vs. 1.7%). There was no significant difference in mean hematocrit change pre- and postdelivery (3.06 ± 1.32 vs. 3.47 ± 1.52). When 45 s DCC cohort was compared with 60 s DCC cohort, there were no significant differences in the incidence of PPH (1.7% vs. 4.8%) or the hematocrit change pre- and postdelivery (3.47 ± 1.52 vs. 4.32 ± 1.88). PPH was not observed in either group when comparing retrospective ICC cohort with prospective DCC cohort with 60 s delay in very preterm twin gestation deliveries. There was no significant difference between the mean hematocrit change pre- and postdelivery (5.5 ± 3.3 vs. 5.8 ± 3.9). When moderate and early late preterm deliveries between 32° to 346 weeks of gestation were compared, there were no differences between the incidence of PPH (0.9% vs. 0%) or hematocrit change pre- and postdelivery (4.2 ± 2.3 vs. 4.8 ± 2.9). Comparing late preterm deliveries between 35° and 366 weeks of gestation, there was no significant difference in the incidence of PPH (13% vs. 11.4%) or the mean hematocrit change pre- and postdelivery (5.0 ± 3.0 vs. 5.1 ± 2.8). In term cesarean deliveries, the incidence of PPH was 2.2% in the retrospective ICC group and 1.4% in the prospective UCM group. There was no difference in mean hematocrit change pre- and postdelivery (5.9 ± 3.7 vs. 6.2 ± 2.8).

Conclusion: DCC or UCM was not associated with the increased risk for PPH or significant change in maternal hematocrit pre- and postdelivery in very preterm singleton, moderate preterm, very preterm twin gestation, late preterm deliveries and term cesarean sections.

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