Developing and validating noninvasive prenatal testing for de novo autosomal dominant monogenic diseases in Vietnam.

Nhi Hoang Nguyen ,Minh-Duy Phan ,Lisa Truong ,Diem-Tuyet Thi Hoang,Vanessa Tran ,Lan-Anh Thi Luong ,My-Ngoc Ba Nguyen ,Minh‐Trung Nguyen ,Phuoc-Loc Doan ,Nhat Thang Tran ,Kim-Phuong Doan ,My-Nhi Ba Nguyen ,Sautina Vo ,Quang Thanh Le ,Thanh-Thanh Thi Nguyen ,Vu Quoc Huy Nguyen ,Viet-Thang Ho ,Hoai-Nghia Nguyen ,Uyen Vu Tran ,Huyen-Trang Thi Tran ,Hung-Sang Tang ,Duc-Tam Lam ,Thị Minh Thi Hà ,Linh Dinh ,Kim-Van Thi Tran ,Duy-Anh Nguyen ,Chi-Thuong Bui ,Sonny Tran ,Canh-Chuong Nguyen ,Van Thong Nguyen,Y-Thanh Lu ,Martin Tran ,Dinh-Kiet Truong ,Phuong Thi-Mai Cao ,Thu Huong Nhut Trinh ,Danh-Cuong Tran ,Thanh-Thuy Thi ,An Q Dinh ,Hong-Thinh Le ,Hoa Giang

doi:10.2217/pme-2023-0076

Abstract

Background: Over 60% of single-gene diseases in newborns are autosomal dominant variants. Noninvasive prenatal testing for monogenic conditions (NIPT-SGG) is cost-effective and timesaving, but not widely applied. This study introduces and validates NIPT-SGG in detecting 25 monogenic conditions. Methods: NIPT-SGG with a 30-gene panel applied next-generation sequencing and trio assays to confirm de novo variants. Diagnostic tests confirmed NIPT-detected cases. Results: Among 93 pregnancies with ultrasound findings, 11(11.8%) fetuses were screened and diagnosed with monogenic diseases, mostly with Noonan syndrome. NIPT-SGG determined >99.99% of actual positive and negative cases, confirmed by diagnostic tests. No false-negatives or false-positives were reported. Conclusion: NIPT-SGG effectively identifies the fetuses affected with monogenic diseases, which is a promisingly safe and timely antenatal screening option for high-risk pregnancies.

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