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1 NIPT data showed recurrent gains and losses in primary m
2 NIPT for fetal aneuploidy screening (chromosomes 13, 18,
3 NIPT profiles from patients with confirmed malignancies
5 NAIT cases will become apparent and accurate NIPT blood group antigen typing results are crucial for
6 used in our standard pipeline for aneuploidy NIPT detected 15/18 (83%) samples with pathogenic rearra
8 results suggest that NGS-based fetal antigen NIPT may identify more fetuses at risk for hemolytic dis
9 ted a next generation sequencing-(NGS) based NIPT assay using quantitative counting template (QCT) te
12 xed with far-larger amounts of maternal DNA, NIPT requires a minimum fraction of the circulating cfDN
19 pregnant women, a low percentage (0.02%) of NIPT results were assessed as indicative of a maternal m
22 ome-wide copy-number changes in the original NIPT samples and in subsequent serial samples from indiv
24 ncers most frequently occurred with the rare NIPT finding of more than 1 aneuploidy detected (7 known
26 g a UK Biobank reference panel and simulated NIPT data, we see accurate imputation of the mother (0.2
31 targeted NIPT, 0.005% malignancy suspicious-NIPT results were reported, in 2/3 patients a malignancy
33 y detection on noninvasive prenatal testing (NIPT) and occult maternal malignancies may explain resul
46 NA fractions and complex genetic variations, NIPT has become essential in managing alloimmunized preg
47 e seen in 23 of 48 patients with genome-wide NIPT, and a malignancy was confirmed in 16 patients (16/
48 lts were reported in 0.03% after genome-wide NIPT, and malignancies confirmed in 16 patients (16/48,