| Literature DB >> 30076564 |
Hong Yao1, Ya Gao2,3,4, Jia Zhao2,3, Rong Zhang1, Huixin Xu2, Huamei Hu1, Yanmei Luo1, Yuying Yuan5, Meili Fu5, Hongyun Zhang5, Hui Jiang2,3, Wei Wang2,4,5, Huanming Yang2,6, Jian Wang2,6, Zhiqing Liang7, Fang Chen8,9,10.
Abstract
Cell-free DNA (cfDNA) testing for common fetal trisomies (T21, T18, T13) is highly effective. However, the usefulness of cfDNA testing in detecting other chromosomal abnormalities is unclear. We evaluated the performance of cfDNA testing for genome-wide abnormalities, and analyzed the incremental yield by reporting extra abnormalities. We performed genome-wide cfDNA testing in 15,626 consecutive pregnancies prospectively enrolled in this study. cfDNA testing results were reported and counseling was given depending on the presence of extra chromosomal abnormalities. cfDNA testing identified 190 cases (1.2%) of chromosomal abnormalities including 100 common trisomies and 90 additional abnormalities. By expanding the cfDNA reporting range to genome-wide abnormalities, the false positive rate increased to 0.39% (P<0.001) and positive predictive value (PPV) was reduced to 65.58% (P=0.42). However, the detection yield increased from 0.44% to 0.65% (P=0.014), and cfDNA testing detected 38.61% (39/101) additional abnormalities with no ultrasound and biochemical screening findings. cfDNA testing outperformed biochemical screening by showing 60 times higher true positive rate and fewer false negative results. Genome-wide cfDNA testing significantly increased the diagnostic yield by detecting extra abnormalities, especially those without diagnostic indications. Genome-wide cfDNA testing has fewer false positive and false negative results compared with biochemical screening.Entities:
Keywords: PPV; cell-free DNA; chromosomal abnormalities; genome-wide; sensitivity; specificity
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Year: 2018 PMID: 30076564 DOI: 10.1007/s11427-017-9344-7
Source DB: PubMed Journal: Sci China Life Sci ISSN: 1674-7305 Impact factor: 6.038