Applications of Noninvasive Prenatal Testing for Subchromosomal Copy Number Variations Using Cell-Free DNA

Abstract Background Noninvasive prenatal testing (NIPT) has been wildly used to screen for common aneuplodies. In recent years, the test has been expanded to detect rare autosomal aneuploidies (RATs) and copy number variations (CNVs). This study was performed to investigate the performance of expanded noninvasive prenatal testing (expanded NIPT) in screening for common trisomies, sex chromosomal aneuploidies (SCAs), rare autosomal aneuploidies (RATs), and copy number variations (CNVs) and parental willingness for invasive prenatal diagnosis in a Chinese prenatal diagnosis center. Methods A total of 24,702 pregnant women were retrospectively analyzed at the Women and Children’s Hospital from January 2013 to April 2019, among which expanded NIPT had been successfully conducted in 24,702 pregnant women. The high-risk expanded NIPT results were validated by karyotype analysis and chromosomal microarray analysis. All the tested pregnant women were followed up for pregnancy outcomes. Results Of the 24,702 cases, successful follow-up was conducted in 98.77% (401/446) of cases with common trisomies and SCAs, 91.95% (80/87) of RAT and CNV cases, and 76.25% (18,429/24,169) of cases with low-risk screening results. The sensitivity of expanded NIPT was 100% (95% confidence interval[CI], 97.38–100%), 96.67%(95%CI, 82.78–99.92%), and 100%(95%CI, 66.37–100.00%), and the specificity was 99.92%(95%CI, 99.87–99.96%), 99.96%(95%CI, 99.91–99.98%), and 99.88% (95%CI, 99.82–99.93%) for the detection of trisomies 21, 18, and 13, respectively. Expanded NIPT detected 45,X, 47,XXX, 47,XXY, XYY syndrome, RATs, and CNVs with positive predictive values of 25.49%, 75%, 94.12%, 76.19%, 6.45%, and 50%, respectively. The women carrying fetuses with Trisomy 21/Trisomy 18/Trisomy 13 underwent invasive prenatal diagnosis and terminated their pregnancies at higher rates than those at high risk for SCAs, RATs, and CNVs. Conclusions Our study demonstrates that the expanded NIPT detects fetal trisomies 21, 18, and 13 with high sensitivity and specificity. The accuracy of detecting SCAs, RATs, and CNVs is still relatively poor and needs to be improved. With a high-risk expanded NIPT result, the women at high risk for common trisomies are more likely to undergo invasive prenatal diagnosis procedures and terminate their pregnancies than those with unusual chromosome abnormalities.

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A novel decision tree model based on chromosome imbalances in cell-free DNA and CA-125 in the differential diagnosis of ovarian cancer

The International Journal of Biological Markers ◽

10.1177/1724600821992356 ◽

2021 ◽

pp. 172460082199235

Author(s):

Weina Zhang ◽

Yu-min Zhang ◽

Yuan Gao ◽

Shengmiao Zhang ◽

Weixin Chu ◽

...

Keyword(s):

Ovarian Cancer ◽

Differential Diagnosis ◽

Decision Tree ◽

Copy Number ◽

Malignant Tumors ◽

Copy Number Variations ◽

Ca 125 ◽

Benign Tumors ◽

Cell Free Dna ◽

Free Dna

Objective: CA-125 is widely used as biomarker of ovarian cancer. However, CA-125 suffers low accuracy. We developed a hybrid analytical model, the Ovarian Cancer Decision Tree (OCDT), employing a two-layer decision tree, which considers genetic alteration information from cell-free DNA along with CA-125 value to distinguish malignant tumors from benign tumors. Methods: We consider major copy number alterations at whole chromosome and chromosome-arm level as the main feature of our detection model. Fifty-eight patients diagnosed with malignant tumors, 66 with borderline tumors, and 10 with benign tumors were enrolled. Results: Genetic analysis revealed significant arm-level imbalances in most malignant tumors, especially in high-grade serous cancers in which 12 chromosome arms with significant aneuploidy ( P<0.01) were identified, including 7 arms with significant gains and 5 with significant losses. The area under receiver operating characteristic curve (AUC) was 0.8985 for copy number variations analysis, compared to 0.8751 of CA125. The OCDT was generated with a cancerous score (CScore) threshold of 5.18 for the first level, and a CA-125 value of 103.1 for the second level. Our most optimized OCDT model achieved an AUC of 0.975. Conclusions: The results suggested that genetic variations extracted from cfDNA can be combined with CA-125, and together improved the differential diagnosis of malignant from benign ovarian tumors. The model would aid in the pre-operative assessment of women with adnexal masses. Future clinical trials need to be conducted to further evaluate the value of CScore in clinical settings and search for the optimal threshold for malignancy detection.

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Reliable noninvasive prenatal testing by massively parallel sequencing of circulating cell-free DNA from maternal plasma processed up to 24h after venipuncture

Clinical Biochemistry ◽

10.1016/j.clinbiochem.2013.07.020 ◽

2013 ◽

Vol 46 (18) ◽

pp. 1783-1786 ◽

Cited By ~ 11

Author(s):

Karen Buysse ◽

Lean Beulen ◽

Ingrid Gomes ◽

Christian Gilissen ◽

Chantal Keesmaat ◽

...

Keyword(s):

Massively Parallel Sequencing ◽

Prenatal Testing ◽

Maternal Plasma ◽

Massively Parallel ◽

Noninvasive Prenatal Testing ◽

Cell Free Dna ◽

Parallel Sequencing ◽

Free Dna ◽

Circulating Cell Free Dna

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Cost-Effectiveness of Cell-Free DNA-Based Noninvasive Prenatal Testing: Summary of Evidence and Challenges

Noninvasive Prenatal Testing (NIPT) ◽

10.1016/b978-0-12-814189-2.00016-5 ◽

2018 ◽

pp. 269-285

Author(s):

Stephen Morris ◽

Caroline S. Clarke ◽

Emma Hudson

Keyword(s):

Cost Effectiveness ◽

Prenatal Testing ◽

Noninvasive Prenatal Testing ◽

Cell Free Dna ◽

Free Dna

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Noninvasive Prenatal Testing by Cell-Free DNA: Technology, Biology, Clinical Utility, and Limitations

Human Reproductive and Prenatal Genetics ◽

10.1016/b978-0-12-813570-9.00028-0 ◽

2019 ◽

pp. 627-652

Author(s):

Francesca Romana Grati ◽

Komal Bajaj ◽

Giuseppe Simoni ◽

Federico Maggi ◽

Susan J. Gross ◽

...

Keyword(s):

Clinical Utility ◽

Prenatal Testing ◽

Noninvasive Prenatal Testing ◽

Cell Free Dna ◽

Free Dna ◽

Dna Technology

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Nonreportable rates and cell‐free DNA profiles in noninvasive prenatal testing among women with heparin treatment

Prenatal Diagnosis ◽

10.1002/pd.5695 ◽

2020 ◽

Vol 40 (7) ◽

pp. 838-845

Author(s):

Noriyuki Nakamura ◽

Aiko Sasaki ◽

Masashi Mikami ◽

Miyuki Nishiyama ◽

Rina Akaishi ◽

...

Keyword(s):

Prenatal Testing ◽

Noninvasive Prenatal Testing ◽

Cell Free Dna ◽

Free Dna ◽

Heparin Treatment ◽

Dna Profiles

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An online tool for fetal fraction prediction based on direct size distribution analysis of maternal cell-free DNA

BioTechniques ◽

10.2144/btn-2020-0143 ◽

2020 ◽

Author(s):

Luca Bedon ◽

Josef Vuch ◽

Simeone Dal Monego ◽

Germana Meroni ◽

Vanna Pecile ◽

...

Keyword(s):

Size Distribution ◽

Prenatal Testing ◽

Distribution Analysis ◽

Blood Draw ◽

Noninvasive Prenatal Testing ◽

Cell Free Dna ◽

Maternal Cell ◽

Fetal Dna ◽

Free Dna ◽

Fetal Fraction

The discovery of circulating fetal DNA in the plasma of pregnant women has greatly promoted advances in noninvasive prenatal testing. Screening performance is enhanced with higher fetal fraction and analysis of samples whose fetal DNA fraction is lower than 4% are unreliable. Although current approaches to fetal fraction measurement are accurate, most of them are expensive and time consuming. Here we present a simple and cost-effective solution that provides a quick and reasonably accurate fetal fraction by directly evaluating the size distribution of circulating DNA fragments in the extracted maternal cell-free DNA. The presented approach could be useful in the presequencing stage of noninvasive prenatal testing to evaluate whether the sample is suitable for the test or a repeat blood draw is recommended.

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