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孕晚期生长速度减慢与出生体重正常胎儿的胎盘功能不全有关:一项前瞻性队列研究。

Reduced growth velocity across the third trimester is associated with placental insufficiency in fetuses born at a normal birthweight: a prospective cohort study.

作者信息

MacDonald Teresa M, Hui Lisa, Tong Stephen, Robinson Alice J, Dane Kirsten M, Middleton Anna L, Walker Susan P

机构信息

Mercy Perinatal, Mercy Hospital for Women, Melbourne, Australia.

Department of Obstetrics and Gynaecology, University of Melbourne, Melbourne, Australia.

出版信息

BMC Med. 2017 Aug 31;15(1):164. doi: 10.1186/s12916-017-0928-z.

Abstract

BACKGROUND

While being small-for-gestational-age due to placental insufficiency is a major risk factor for stillbirth, 50% of stillbirths occur in appropriate-for-gestational-age (AGA, > 10th centile) fetuses. AGA fetuses are plausibly also at risk of stillbirth if placental insufficiency is present. Such fetuses may be expected to demonstrate declining growth trajectory across pregnancy, although they do not fall below the 10th centile before birth. We investigated whether reduced growth velocity in AGA fetuses is associated with antenatal, intrapartum and neonatal indicators of placental insufficiency.

METHODS

We performed a prospective cohort study of 308 nulliparous women who subsequently gave birth to AGA infants. Ultrasound was utilised at 28 and 36 weeks' gestation to determine estimated fetal weight (EFW) and abdominal circumference (AC). We correlated relative EFW and AC growth velocities with three clinical indicators of placental insufficiency, namely (1) fetal cerebroplacental ratio (CPR; CPR < 5th centile reflects placental resistance, and blood flow redistribution to the brain - a fetal response to hypoxia); (2) neonatal acidosis after the hypoxic challenge of labour (umbilical artery (UA) pH < 7.15 at birth); and (3) low neonatal body fat percentage (BF%, measured by air displacement plethysmography) reflecting reduced nutritional reserve in utero.

RESULTS

For each one centile reduction in EFW growth velocity between 28 and 36 weeks' gestation, there was a 2.4% increase in the odds of cerebral redistribution (CPR < 5th centile, odds ratio (OR) (95% confidence interval) = 1.024 (1.005-1.042), P = 0.012) and neonatal acidosis (UA pH < 7.15, OR = 1.024 (1.003-1.046), P = 0.023), and a 3.3% increase in the odds of low BF% (OR = 1.033 (1.001-1.067), P = 0.047). A decline in EFW of > 30 centiles between 28 and 36 weeks (compared to greater relative growth) was associated with cerebral redistribution (CPR < 5th centile relative risk (RR) = 2.80 (1.25-6.25), P = 0.026), and a decline of > 35 centiles was associated with neonatal acidosis (UA pH < 7.15 RR = 3.51 (1.40-8.77), P = 0.030). Similar associations were identified between low AC growth velocity and clinical indicators of placental insufficiency.

CONCLUSIONS

Reduced growth velocity between 28 and 36 weeks' gestation among fetuses born AGA is associated with antenatal, intrapartum and neonatal indicators of placental insufficiency. These fetuses potentially represent an important unrecognised cohort at increased risk of stillbirth and may warrant more intensive antenatal surveillance.

摘要

背景

虽然因胎盘功能不全导致小于胎龄是死产的主要危险因素,但50%的死产发生在适于胎龄(AGA,>第10百分位数)的胎儿中。如果存在胎盘功能不全,AGA胎儿也可能有死产风险。尽管这些胎儿在出生前未低于第10百分位数,但预计其在整个孕期的生长轨迹会下降。我们调查了AGA胎儿生长速度降低是否与胎盘功能不全的产前、产时及新生儿指标相关。

方法

我们对308名随后分娩出AGA婴儿的初产妇进行了一项前瞻性队列研究。在妊娠28周和36周时使用超声来确定估计胎儿体重(EFW)和腹围(AC)。我们将相对EFW和AC生长速度与胎盘功能不全的三个临床指标进行了关联,即(1)胎儿脑胎盘比(CPR;CPR<第5百分位数反映胎盘阻力以及血流重新分布至脑部——胎儿对缺氧的反应);(2)产时缺氧挑战后的新生儿酸中毒(出生时脐动脉(UA)pH<7.15);以及(3)低新生儿体脂百分比(BF%,通过空气置换体积描记法测量),反映子宫内营养储备减少。

结果

在妊娠28周和36周之间,EFW生长速度每降低一个百分位数,脑血流重新分布(CPR<第5百分位数,比值比(OR)(95%置信区间)=1.024(1.005 - 1.042),P = 0.012)和新生儿酸中毒(UA pH<7.15,OR = 1.024(1.003 - 1.046),P = 0.023)的几率增加2.4%,低BF%的几率增加3.3%(OR = 1.033(1.001 - 1.067),P = 0.047)。妊娠28周和36周之间EFW下降>30个百分位数(与相对生长较大相比)与脑血流重新分布相关(CPR<第5百分位数相对危险度(RR)=2.80(1.25 - 6.25),P = 0.026),下降>35个百分位数与新生儿酸中毒相关(UA pH<7.15 RR = 3.51(1.40 - 8.77),P = 0.030)。在低AC生长速度与胎盘功能不全的临床指标之间也发现了类似的关联。

结论

AGA出生胎儿在妊娠28周和36周之间生长速度降低与胎盘功能不全的产前、产时及新生儿指标相关。这些胎儿可能代表一个重要的未被认识的队列,其死产风险增加,可能需要更强化的产前监测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f60/5577811/686bc91fa493/12916_2017_928_Fig1_HTML.jpg

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