Relevance of Invasive Testing in Era of Non-Invasive Testing for Prenatal Chromosomal Abnormalities

Abhijeet Kumar, M. Dey, D. Arora
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引用次数: 1

Abstract

Prenatal screening for chromosomal abnormalities has two components i.e. prenatal screening (maternal serum screening and cell-free fetal DNA screening) and prenatal diagnosis (chorionic villus sampling, amniocentesis, and cordocentesis). Prenatal testing in the past decade is evolving towards non-invasive methods to determine the chromosome abnormality disorders in the fetus without incurring the risk of miscarriage. Conventional tools for prenatal screening included maternal age, maternal serum markers, ultrasound marker (nuchal thickness), and their combinations. With the increased risk of screening test patients were offered diagnostic tests (chorionic villus sampling, amniocentesis, and cordocentesis). After the availability of noninvasive prenatal tests for commercial use in 2011, a great marketing drive is there to establish it as a master tool for prenatal testing. However various society guidelines i.e. ACOG, RCOG, and ISUOG have clearly stated that cell-free fetal DNA based noninvasive prenatal tests is a screening test, not a diagnostic test. In the succeeding paragraph, we will review current trends in the field of cell-free fetal DNA noninvasive prenatal tests and the relevance of invasive testing in the context of noninvasive prenatal tests. Noninvasive prenatal tests does not entirely replace invasive prenatal testing procedures. Positive noninvasive prenatal tests findings must be confirmed by diagnostic tests based on an invasive sample source, mainly chorionic villus sampling or amniocentesis due to false positive and false negative reports of cell-free fetal DNA based tests. Continuing research and development efforts are focused on overriding noninvasive prenatal tests limitations. Recent studies show that procedure-associated risks in the case of prenatal invasive testing are very low as compared to previous studies. Prenatal invasive testing will remain as the backbone of prenatal diagnostic testing until the limitation of noninvasive prenatal tests is overcome.
在无创产前染色体异常检测时代侵入性检测的相关性
产前染色体异常筛查有两个组成部分,即产前筛查(母体血清筛查和无细胞胎儿DNA筛查)和产前诊断(绒毛膜绒毛取样、羊膜穿刺术和脐带穿刺术)。在过去的十年中,产前检测正朝着非侵入性的方法发展,以确定胎儿的染色体异常疾病,而不会产生流产的风险。产前筛查的常规工具包括母亲年龄、母亲血清标志物、超声标志物(颈厚)及其组合。随着筛查试验风险的增加,为患者提供诊断试验(绒毛膜绒毛取样、羊膜穿刺术和脐带穿刺术)。自2011年无创产前检测可用于商业用途以来,一股巨大的营销动力将其确立为产前检测的主要工具。然而,各种社会指南,如ACOG、RCOG和ISUOG都明确指出,基于无细胞胎儿DNA的无创产前检查是一种筛查试验,而不是诊断试验。在接下来的段落中,我们将回顾无细胞胎儿DNA无创产前检测领域的当前趋势,以及在无创产前检测背景下侵入性检测的相关性。无创产前检查并不能完全取代有创产前检查程序。由于无细胞胎儿DNA检测的假阳性和假阴性报告,必须通过基于侵入性样本来源的诊断测试(主要是绒毛膜绒毛取样或羊膜穿刺术)来证实非侵入性产前检查的阳性结果。持续的研究和开发工作的重点是克服无创产前检查的局限性。最近的研究表明,与以前的研究相比,产前侵入性检查的程序相关风险非常低。在克服无创产前检查的局限性之前,产前侵入性检查仍将是产前诊断检查的支柱。
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