推导和评估性别特异性胎儿生长标准。

Nathan R Blue, Amanda A Allshouse, Sarah Heerboth, William Grobman, Brian Mercer, Anthony Shanks, Julia M Bregand-White, Hyagriv Simhan, Uma M Reddy, George Saade, Samuel Parry, Robert M Silver
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引用次数: 0

摘要

目的:根据胎儿的性别特异性生长状况,得出规定性的胎儿性别特异性生长标准,并评估临床管理和结果:这是对无子宫妊娠结局研究(Nulliparous Pregnancy Outcomes Study:nuMoM2b)的二次分析。该研究是一项前瞻性观察性研究,研究对象是来自美国八个中心的10038名无妊娠期妇女,她们分别在14-20周和22-29周接受了超声波检查,并在分娩后确定了结果。我们从中选择了一个嵌套队列中的低风险参与者(排除了那些患有慢性高血压、妊娠前糖尿病、疑似非整倍体和早产的患者),利用超声和出生时的胎儿体重得出了一个性别特异性的预期胎儿生长方程。我们比较了性别特异性标准和性别中性(Hadlock)标准之间体重第 90 百分位数(胎龄偏大 [LGA])比率的男女差异。然后,我们使用完整的未入选队列,根据性别特异性 SGA 和 LGA 状态评估了结果和临床管理:总体而言,低风险巢式队列中的 7280 名婴儿被用于推导性别特异性方程,其中胎儿性别被列为方程截距。性别中性标准诊断出的 SGA 多见于女性新生儿(21% 对 13%,p = .23;LGA:13% 对 13%,p = .58)。为了接近未经筛选的人群,我们的次要目标(N = 8339)纳入了最初因发育异常风险因素而被排除在外的 1059 名参与者。在这个未经筛选的队列中,按性别中性标准被归类为 SGA 的 1498 名新生儿中,有 39% (95% CI 37.0-42.0%)按性别特异性标准被重新归类为适合胎龄 (AGA)。与两种方法都认为是 AGA 的新生儿相比,这些被重新分类的新生儿尽管发病风险较低(女性)或发病风险相当(男性),但却更有可能因生长受限而分娩。在按性别中性标准被认为是AGA的6485名新生儿中,有737名(11.4%,95% CI 10.6-12.2%)按性别特异性标准被重新分类为LGA。这些被重新分类的新生儿因胎位下降停止而进行剖宫产、因宫口扩张停止而进行剖宫产以及肩难产的比例均高于两种方法均被视为 AGA 的新生儿。结论:结论:Hadlock 性别中立标准会造成出生时 SGA 和 LGA 的性别差异。结论:Hadlock性别中性标准会造成出生时SGA和LGA的性别差异,而我们的性别特异性标准则解决了这些差异,并有可能提高生长病理学风险分层的准确性。
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Derivation and assessment of a sex-specific fetal growth standard.

Purpose: To derive a prescriptive sex-specific fetal growth standard and assess clinical management and outcomes according to sex-specific growth status.

Materials and methods: This was a secondary analysis of the Nulliparous Pregnancy Outcomes Study: Monitoring Mothers-to-Be (nuMoM2b), a prospective observational study of 10,038 nulliparas from eight U.S. centers who underwent ultrasounds at 14-20 and 22-29 weeks with outcomes ascertained after delivery. From these, we selected a nested cohort of lower risk participants (excluded those with chronic hypertension, pre-gestational diabetes, suspected aneuploidy, and preterm delivery) to derive a sex-specific equation for expected fetal growth using fetal weights by ultrasound and at birth. We compared the male-female discrepancy in the rate of weight <10th (small for gestational age [SGA]) and >90th (large for gestational age [LGA]) percentiles between the sex-specific and sex-neutral (Hadlock) standards. Using the full unselected cohort, we then assessed outcomes and clinical management according to sex-specific SGA and LGA status.

Results: Overall, 7280 infants in the lower risk nested cohort were used to derive a sex-specific equation with fetal sex included as an equation intercept. The sex-neutral standard diagnosed SGA more often in female newborns (21% vs. 13%, p < .001) and LGA more often in male newborns (5% vs. 3%, p < .001). The sex-specific standard resolved these disparities (SGA: 9% vs. 10%, p = .23; LGA: 13% vs. 13%, p = .58). To approximate an unselected population, 1059 participants initially excluded for risk factors for abnormal growth were then included for our secondary objective (N = 8339). In this unselected cohort, 39% (95% CI 37.0-42.0%) of the 1498 newborns classified as SGA by the sex-neutral standard were reclassified as appropriate for gestational age (AGA) by the sex-specific standard. These reclassified newborns were more likely to be delivered for growth restriction despite having lower risk of morbidity (females) or comparable risk of morbidity (males) compared to newborns considered AGA by both methods. Of the 6485 newborns considered AGA by the sex-neutral standard, 737 (11.4%, 95% CI 10.6-12.2%) were reclassified as LGA by the sex-specific standard. These reclassified newborns had higher rates of cesarean for arrest of descent, cesarean for arrest of dilation, and shoulder dystocia than newborns considered AGA by both methods. None were reclassified from LGA to AGA by the sex-specific standard.

Conclusion: The Hadlock sex-neutral standard generates sex disparities in SGA and LGA at birth. Our sex-specific standard resolves these disparities and has the potential to improve accuracy of growth pathology risk stratification.

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