Clinical application of massively parallel sequencing‐based prenatal noninvasive fetal trisomy test for trisomies 21 and 18 in 11 105 pregnancies with mixed risk factors

Shan Dan(BGI Group (China)), Wei Wang(BGI Group (China)), Jinghui Ren(ShenZhen People’s Hospital), Yali Li(BGI Group (China)), Hua Hu(Army Medical University), Zhengfeng Xu(Nanjing Maternity and Child Health Care Hospital), Tze Kin Lau(Fetal Medicine Foundation), Jianhong Xie(Shenzhen Maternity and Child Healthcare Hospital), Weihua Zhao(Shenzhen Second People's Hospital), Hefeng Huang(Ministry of Education), Jiansheng Xie(Shenzhen Maternity and Child Healthcare Hospital), Luming Sun(Shanghai First Maternity and Infant Hospital), Xiaohong Zhang(BGI Group (China)), Xiaohong Zhang(BGI Group (China)), Weipeng Wang(BGI Group (China)), Shixiu Liao(Henan Provincial People's Hospital), Rong Qiang(Northwest Women's and Children's Hospital), Jiangxia Cao(Peking University), Qiufang Zhang(Peking University), Yulin Zhou(Nanjing Drum Tower Hospital), Haiyan Zhu(Nanfang Hospital), Mei Zhong(Nanfang Hospital), Yi Guo(ShenZhen People’s Hospital), Linhua Lin(Chinese PLA General Hospital), Zhiying Gao(Army Medical University), Hong Yao(BGI Group (China)), Hong‐Yun Zhang(BGI Group (China)), Lijian Zhao(BGI Group (China)), Fuman Jiang(BGI Group (China)), Fang Chen(BGI Group (China)), Hui Jiang(BGI Group (China)), Songgang Li(BGI Group (China)), Yingrui Li(BGI Group (China)), Jun Wang(BGI Group (China)), Jian Wang(BGI Group (China)), Tao Duan(Shanghai First Maternity and Infant Hospital), Yue Su(BGI Group (China)), Xiuqing Zhang(BGI Group (China)), Xiuqing Zhang(BGI Group (China))
Prenatal Diagnosis
November 9, 2012
Cited by 235Open Access
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Abstract

OBJECTIVE: To report the performance of massively parallel sequencing (MPS) based prenatal noninvasive fetal trisomy test based on cell-free DNA sequencing from maternal plasma in a routine clinical setting in China. METHOD: The MPS-based test was offered as a prenatal screening test for trisomies 21 and 18 to pregnant women in 49 medical centers over 2 years. A total of 11,263 participants were recruited and the MPS-based test was performed in 11,105 pregnancies. Fetal outcome data were obtained after the expected date of confinement. RESULTS: One hundred ninety cases were classified as positive, including 143 cases of trisomy 21 and 47 cases of trisomy 18. With the karyotyping results and the feedback of fetal outcome data, we observed one false positive case of trisomy 21, one false positive case of trisomy 18 and no false negative cases, indicating 100% sensitivity and 99.96% specificity for the detection of trisomies 21 and 18. CONCLUSION: Our large-scale multicenter study proved that the MPS-based test is of high sensitivity and specificity in detecting fetal trisomies 21 and 18. The introduction of this screening test into a routine clinical setting could avoid about 98% of invasive prenatal diagnostic procedures.


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