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30-33 孕周母血清胎盘生长因子、妊娠相关血浆蛋白-A 和游离β-人绒毛膜促性腺激素预测子痫前期的价值。

Maternal serum placental growth factor, pregnancy-associated plasma protein-a and free β-human chorionic gonadotrophin at 30-33 weeks in the prediction of pre-eclampsia.

机构信息

Harris Birthright Research Centre of Fetal Medicine, King's College Hospital, London, UK.

出版信息

Fetal Diagn Ther. 2013;33(3):164-72. doi: 10.1159/000345090. Epub 2013 Feb 20.

DOI:10.1159/000345090
PMID:23445908
Abstract

OBJECTIVE

To investigate the potential value of maternal serum concentrations of free β-human chorionic gonadotrophin (β-hCG), pregnancy-associated plasma protein-A (PAPP-A) and placental growth factor (PlGF) at 30-33 weeks of gestation in the prediction of pre-eclampsia (PE) developing at or after 34 weeks.

METHODS

Serum free β-hCG, PAPP-A and PlGF were measured at 11-13 and at 30-33 weeks of gestation in a case-control study of 50 cases that developed PE at or after 34 weeks and 250 unaffected controls. The measured concentration of metabolites was converted into multiples of the unaffected median (MoM) and the MoM values in the PE and control groups were compared.

RESULTS

At 11-13 weeks, serum PlGF and PAPP-A, but not free β-hCG, were significantly lower in the PE group than in the controls (0.824, 0.748 and 0.857 vs. 1.000 MoM). At 30-33 weeks in the PE group, PlGF was reduced (0.356 MoM), free β-hCG was increased (1.750 MoM), but PAPP-A was not significantly different (0.991 MoM) from control (1.000 MoM). In screening for PE at 30-33 weeks by a combination of maternal characteristics and serum PlGF, the estimated detection rates, at a false-positive rate of 10%, of intermediate PE (requiring delivery at 34-37 weeks) and late PE (with delivery after 37 weeks) were 85.7 and 52.8%, respectively. The performance of screening was not improved by the addition of free β-hCG or the free β-hCG/PlGF ratio.

CONCLUSION

Screening by maternal characteristics and serum PlGF at 30-33 weeks could identify most pregnancies that will subsequently develop PE.

摘要

目的

探讨孕 30-33 周时母体血清游离β-人绒毛膜促性腺激素(β-hCG)、妊娠相关血浆蛋白-A(PAPP-A)和胎盘生长因子(PlGF)浓度对预测 34 周及以后发生子痫前期(PE)的潜在价值。

方法

采用病例对照研究,对 50 例 34 周及以后发生的 PE 患者和 250 例未受影响的对照组在 11-13 周和 30-33 周时进行血清游离β-hCG、PAPP-A 和 PlGF 检测。将代谢物的测量浓度转换为未受影响中位数的倍数(MoM),并比较 PE 组和对照组的 MoM 值。

结果

在 11-13 周时,PE 组血清 PlGF 和 PAPP-A 水平显著低于对照组(0.824、0.748 和 0.857 比 1.000 MoM),但游离β-hCG 水平无显著差异(0.857 比 1.000 MoM)。在 30-33 周时,PE 组 PlGF 水平降低(0.356 MoM),游离β-hCG 水平升高(1.750 MoM),但 PAPP-A 水平与对照组(1.000 MoM)无显著差异(0.991 MoM)。在孕 30-33 周时,结合母体特征和血清 PlGF 筛查 PE,假阳性率为 10%时,中孕期 PE(需要在 34-37 周分娩)和晚孕期 PE(37 周后分娩)的估计检出率分别为 85.7%和 52.8%。添加游离β-hCG 或游离β-hCG/PlGF 比值并不能提高筛查的效果。

结论

孕 30-33 周时,通过母体特征和血清 PlGF 筛查可以识别出大多数随后会发生 PE 的妊娠。

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