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Review
. 2024 Apr;230(4):381-389.
doi: 10.1016/j.ajog.2023.11.1240. Epub 2023 Nov 25.

Placental, maternal, fetal, and technical origins of false-positive cell-free DNA screening results

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Free article
Review

Placental, maternal, fetal, and technical origins of false-positive cell-free DNA screening results

Yvette Raymond et al. Am J Obstet Gynecol. 2024 Apr.
Free article

Abstract

The introduction of noninvasive prenatal testing has resulted in substantial reductions to previously accepted false-positive rates of prenatal screening. Despite this, the possibility of false-positive results remains a challenging consideration in clinical practice, particularly considering the increasing uptake of genome-wide noninvasive prenatal testing, and the subsequent increased proportion of high-risk results attributable to various biological events besides fetal aneuploidy. Confined placental mosaicism, whereby chromosome anomalies exclusively affect the placenta, is perhaps the most widely accepted cause of false-positive noninvasive prenatal testing. There remains, however, a substantial degree of ambiguity in the literature pertaining to the clinical ramifications of confined placental mosaicism and its potential association with placental insufficiency, and consequentially adverse pregnancy outcomes including fetal growth restriction. Other causes of false-positive noninvasive prenatal testing include vanishing twin syndrome, in which the cell-free DNA from a demised aneuploidy-affected twin triggers a high-risk result, technical failures, and maternal origins of abnormal cell-free DNA such as uterine fibroids or unrecognized mosaicisms. Most concerningly, maternal malignancies are also a documented cause of false-positive screening results. In this review, we compile what is currently known about the various causes of false-positive noninvasive prenatal testing.

Keywords: cancer in pregnancy; cell-free DNA screening; confined placental mosaicism; genome-wide screening; maternal malignancy; noninvasive prenatal testing; placental insufficiency; prenatal screening; rare autosomal trisomy; segmental copy number variation; uterine fibroids; vanishing twin syndrome.

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