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早孕期基于生物标志物和母体外周血游离胎儿 DNA 的唐氏综合征 contingent 筛查。

First-trimester contingent screening for trisomy 21 by biomarkers and maternal blood cell-free DNA testing.

机构信息

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

出版信息

Ultrasound Obstet Gynecol. 2013 Jul;42(1):41-50. doi: 10.1002/uog.12511. Epub 2013 Jun 7.

DOI:10.1002/uog.12511
PMID:23744626
Abstract

OBJECTIVE

To define risk cut-offs with corresponding detection rates (DR) and false-positive rates (FPR) in screening for trisomy 21 using maternal age and combinations of first-trimester biomarkers in order to determine which women should undergo contingent maternal blood cell-free (cf) DNA testing.

METHODS

From singleton pregnancies undergoing screening for aneuploidies at three UK hospitals between March 2006 and May 2012, we analyzed prospectively collected data on the following biomarkers: fetal nuchal translucency thickness (NT) and ductus venosus pulsatility index for veins (DV-PIV) at 11 + 0 to 13 + 6 weeks' gestation and serum free β-human chorionic gonadotropin (β-hCG), pregnancy-associated plasma protein-A (PAPP-A), placental growth factor (PlGF) and alpha-fetoprotein (AFP) at 8 + 0 to 13 + 6 weeks. Estimates of risk cut-offs, DRs and FPRs were derived for combinations of biomarkers and these were used to define the best strategy for contingent cfDNA testing.

RESULTS

In contingent screening, detection of 98% of fetuses with trisomy 21 at an overall invasive testing rate < 0.5% can be potentially achieved by offering cfDNA testing to about 36%, 21% and 11% of cases identified by first-line screening using the combined test alone, using the combined test with the addition of serum PlGF and AFP and using the combined test with the addition of PlGF, AFP and DV-PIV, respectively.

CONCLUSIONS

Effective first-trimester screening for trisomy 21, with DR of 98% and invasive testing rate < 0.5%, can be potentially achieved by contingent screening incorporating biomarkers and cfDNA testing.

摘要

目的

通过使用母体年龄和孕早期生物标志物组合来定义唐氏综合征 21 三体筛查的风险截止值及其相应的检出率(DR)和假阳性率(FPR),以确定哪些女性应进行有条件的母体无细胞游离(cf)DNA 检测。

方法

我们对 2006 年 3 月至 2012 年 5 月期间在英国三家医院进行的非整倍体筛查的单胎妊娠进行了前瞻性分析,收集了以下生物标志物的前瞻性数据:胎儿颈项透明层厚度(NT)和静脉导管搏动指数(DV-PIV)在 11+0 至 13+6 孕周以及血清游离人绒毛膜促性腺激素-β(β-hCG)、妊娠相关血浆蛋白-A(PAPP-A)、胎盘生长因子(PlGF)和甲胎蛋白(AFP)在 8+0 至 13+6 孕周。我们对生物标志物组合的风险截止值、DR 和 FPR 进行了估计,并将其用于定义有条件 cfDNA 检测的最佳策略。

结果

在有条件筛查中,通过仅使用联合检测、联合检测加血清 PlGF 和 AFP 以及联合检测加 PlGF、AFP 和 DV-PIV,分别向 36%、21%和 11%的病例提供 cfDNA 检测,可潜在地实现以总体侵入性检测率<0.5%检测出 98%唐氏综合征 21 三体胎儿的目标。

结论

通过整合生物标志物和 cfDNA 检测的有条件筛查,可能实现有效的孕早期唐氏综合征 21 三体筛查,其 DR 为 98%,侵入性检测率<0.5%。

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