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定制的出生体重百分位数与胎盘相关的胎儿生长受限。

Customized birth-weight centiles and placenta-related fetal growth restriction.

机构信息

Department of Obstetrics and Gynecology, University of Toronto, Toronto, Ontario, Canada.

Division of Maternal-Fetal Medicine, Department of Obstetrics and Gynecology, Sunnybrook Health Sciences Centre, Toronto, Ontario, Canada.

出版信息

Ultrasound Obstet Gynecol. 2021 Mar;57(3):409-416. doi: 10.1002/uog.23516.

DOI:10.1002/uog.23516
PMID:33073889
Abstract

OBJECTIVE

The value of using customized birth-weight centiles to improve the diagnostic accuracy for fetal growth restriction (FGR), in comparison with using population-based charts, remains a matter of debate. One potential explanation for the conflicting data is that most studies used measures of perinatal mortality and morbidity as proxies for placenta-mediated FGR, many of which are not specific and may be confounded by other factors such as prematurity. The aim of this study was to compare the diagnostic accuracy of small-for-gestational age (SGA) at birth, defined according to customized vs population-based charts, for associated abnormal placental pathology.

METHODS

This was a secondary analysis of data from a prospective cohort study on risk factors for placenta-mediated complications and abnormal placental pathology in low-risk nulliparous women. All placentae were sent for detailed histopathological examination by two perinatal pathologists. The primary exposure was SGA, defined as birth weight < 10 centile for gestational age using either a customized (SGA ) or a population-based (SGA ) birth-weight reference. The outcomes of interest were one of three types of abnormal placental pathology associated with FGR: maternal vascular malperfusion (MVM), chronic villitis and fetal vascular malperfusion (FVM). Adjusted relative risks (aRR) with 95% CIs were estimated using modified Poisson regression analysis, with adjustment for smoking, body mass index and aspirin treatment.

RESULTS

A total of 857 nulliparous women met the study criteria. The proportions of infants identified as SGA based on the customized and population-based charts were 12.6% (108/857) and 11.4% (98/857), respectively. A diagnosis of SGA using either customized or population-based charts was associated with an increased risk of any placental pathology (aRR, 3.04 (95% CI, 2.29-4.04) and 1.60 (95% CI, 1.10-2.31), respectively) and MVM pathology (aRR, 12.33 (95% CI, 6.60-23.03) and 5.29 (95% CI, 2.87-9.76), respectively). SGA , but not SGA , was also associated with an increased risk for chronic villitis (aRR, 1.85 (95% CI, 1.07-3.18)) and FVM pathology (aRR, 2.48 (95% CI, 1.25-4.93)). SGA had a higher detection rate for any placental pathology (30.3% vs 17.1%; P < 0.001), MVM pathology (63.2% vs 39.5%; P = 0.003) and chronic villitis (20.8% vs 8.3%; P = 0.007) than did SGA , for a similar false-positive rate. This was mainly the result of a higher detection rate for abnormal pathology in the white and East-Asian subgroups and a lower false-positive rate for abnormal pathology in the South-Asian subgroup by SGA than by SGA . In addition, pregnancies in the SGA group, but not those in the SGA group, were more likely to be complicated by preterm birth and a low 5-min Apgar score than were the corresponding non-SGA group.

CONCLUSION

These findings suggest that customized birth-weight centiles may be superior to population-based birth-weight centiles in detecting FGR that is due to underlying placental disease. © 2020 International Society of Ultrasound in Obstetrics and Gynecology.

摘要

目的

使用定制的出生体重百分位数来提高胎儿生长受限(FGR)的诊断准确性,与使用基于人群的图表相比,其价值仍存在争议。数据冲突的一个潜在解释是,大多数研究使用围产期死亡率和发病率作为胎盘介导的 FGR 的替代指标,但其中许多指标并不具体,可能会受到早产等其他因素的干扰。本研究旨在比较根据定制和基于人群的图表定义的出生时小于胎龄儿(SGA)与相关异常胎盘病理的诊断准确性。

方法

这是一项对低危初产妇胎盘介导并发症和异常胎盘病理危险因素的前瞻性队列研究数据的二次分析。所有胎盘均由两名围产病理学家进行详细的组织病理学检查。主要暴露是 SGA,定义为使用定制(SGA )或基于人群的(SGA )出生体重参考值时出生体重<胎龄第 10 百分位。感兴趣的结局是与 FGR 相关的三种异常胎盘病理之一:母体血管灌注不良(MVM)、慢性绒毛膜炎和胎儿血管灌注不良(FVM)。使用修正泊松回归分析,调整吸烟、体重指数和阿司匹林治疗,估计调整后的相对风险(aRR)及其 95%可信区间。

结果

共有 857 名初产妇符合研究标准。根据定制和基于人群的图表,婴儿被诊断为 SGA 的比例分别为 12.6%(108/857)和 11.4%(98/857)。使用定制或基于人群的图表诊断 SGA 与任何胎盘病理(aRR,3.04(95%CI,2.29-4.04)和 1.60(95%CI,1.10-2.31))和 MVM 病理(aRR,12.33(95%CI,6.60-23.03)和 5.29(95%CI,2.87-9.76))的风险增加相关。SGA 而不是 SGA 也与慢性绒毛膜炎(aRR,1.85(95%CI,1.07-3.18))和 FVM 病理(aRR,2.48(95%CI,1.25-4.93))的风险增加相关。SGA 比 SGA 有更高的任何胎盘病理(30.3%比 17.1%;P<0.001)、MVM 病理(63.2%比 39.5%;P=0.003)和慢性绒毛膜炎(20.8%比 8.3%;P=0.007)的检出率,而假阳性率相似。这主要是由于 SGA 比 SGA 检测到白人和东亚亚组的异常病理的检出率更高,而南亚亚组的异常病理的假阳性率更低。此外,与相应的非 SGA 组相比,SGA 组的妊娠更可能因早产和低 5 分钟 Apgar 评分而复杂化。

结论

这些发现表明,与基于人群的出生体重百分位数相比,定制的出生体重百分位数可能更有助于检测由潜在胎盘疾病引起的 FGR。

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