Souter V L, Nyberg D A
Center for Perinatal Studies, University of Washington Medical Center, Seattle, USA.
J Ultrasound Med. 2001 Jul;20(7):775-90. doi: 10.7863/jum.2001.20.7.775.
Screening for fetal aneuploidy is now possible during the first trimester using sonographic and biochemical markers. The aim of this review was to summarize the efficacy and use of nuchal translucency in screening for fetal aneuploidy, especially fetal Down syndrome, and other anomalies.
We reviewed available literature regarding first-trimester screening. This includes more than 16 studies of nuchal translucency as a marker for fetal aneuploidy published since 1995.
Although early studies showed wide variation in detection of fetal Down syndrome when using nuchal translucency, more recent studies showed sensitivities of approximately 70% to 80%, for a 5% false-positive rate. Increased nuchal translucency has also been found to be a marker for other aneuploidies, including trisomy 18, trisomy 13, and Turner syndrome. Maternal serum biochemical screening can be used as a test for aneuploidy during the first trimester The 2 maternal serum markers that appear to be most useful in the late first trimester are the free beta subunit of human chorionic gonadotropin and pregnancy-associated plasma protein A. Together with maternal age, these markers yield a detection rate for trisomy 21 of approximately 60%, for a 5% false-positive rate. Because sonographic and biochemical markers appear to be largely independent, their combined risk results in improved detection rates compared with either method alone. As a result, the combination of nuchal translucency, biochemical markers, and maternal age has achieved a detection rate of approximately 85%, for a 5% false-positive level for detection of trisomy 21. A newly proposed "integrated" approach using a panel of first- and second-trimester markers suggests that further improvement in the screening performance is possible. A number of questions regarding first-trimester screening remain. We address some of these questions: is first-trimester screening more effective than second-trimester screening? How to account for intrauterine lethality? Is earlier diagnosis important, and will it be accepted by patients? Is first-trimester screening cost-effective? How should first-trimester screening be interpreted with second-trimester tests?
Despite encouraging data and general enthusiasm for first-trimester screening for fetal Down syndrome and other aneuploidies, a number of questions remain about its implementation in the United States. Multicenter studies currently under way should help answer some of these questions.
目前在孕早期利用超声和生化标志物筛查胎儿非整倍体已成为可能。本综述的目的是总结颈部透明带厚度在筛查胎儿非整倍体,尤其是胎儿唐氏综合征及其他异常情况中的有效性及应用。
我们回顾了关于孕早期筛查的现有文献。这包括自1995年以来发表的16项以上将颈部透明带厚度作为胎儿非整倍体标志物的研究。
尽管早期研究显示使用颈部透明带厚度检测胎儿唐氏综合征时差异较大,但近期研究表明,在假阳性率为5%时,敏感性约为70%至80%。颈部透明带厚度增加也被发现是其他非整倍体的标志物,包括18三体、13三体和特纳综合征。孕早期可将母体血清生化筛查用作非整倍体检测方法。孕早期晚期最有用的两种母体血清标志物是人绒毛膜促性腺激素游离β亚基和妊娠相关血浆蛋白A。结合孕妇年龄,这些标志物对21三体的检测率约为60%,假阳性率为5%。由于超声和生化标志物在很大程度上似乎相互独立,与单独使用任何一种方法相比,它们的联合风险可提高检测率。因此,颈部透明带厚度、生化标志物和孕妇年龄相结合,对21三体的检测率达到了约85%,假阳性水平为5%。一种新提出的使用孕早期和孕中期标志物组合的“整合”方法表明筛查性能可能会进一步提高。关于孕早期筛查仍有一些问题。我们讨论其中一些问题:孕早期筛查比孕中期筛查更有效吗?如何考虑宫内致死率?早期诊断重要吗,患者会接受吗?孕早期筛查具有成本效益吗?孕早期筛查结果应如何与孕中期检测结果一起解读?
尽管有令人鼓舞的数据以及对孕早期筛查胎儿唐氏综合征和其他非整倍体普遍热情高涨,但在美国其实施仍存在许多问题。目前正在进行的多中心研究应有助于回答其中一些问题。
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