BMC Medical Genomics (Dec 2012)

Noninvasive Fetal Trisomy (NIFTY) test: an advanced noninvasive prenatal diagnosis methodology for fetal autosomal and sex chromosomal aneuploidies

  • Jiang Fuman,
  • Ren Jinghui,
  • Chen Fang,
  • Zhou Yuqiu,
  • Xie Jiansheng,
  • Dan Shan,
  • Su Yue,
  • Xie Jianhong,
  • Yin Baomin,
  • Su Wen,
  • Zhang Huakun,
  • Wang Wei,
  • Chai Xianghua,
  • Lin Linhua,
  • Guo Hui,
  • Li Qiyun,
  • Li Peipei,
  • Yuan Yuying,
  • Pan Xiaoyu,
  • Li Yihan,
  • Liu Lifu,
  • Chen Huifei,
  • Xuan Zhaoling,
  • Chen Shengpei,
  • Zhang Chunlei,
  • Zhang Hongyun,
  • Tian Zhongming,
  • Zhang Zhengyu,
  • Jiang Hui,
  • Zhao Lijian,
  • Zheng Weimou,
  • Li Songgang,
  • Li Yingrui,
  • Wang Jun,
  • Wang Jian,
  • Zhang Xiuqing

DOI
https://doi.org/10.1186/1755-8794-5-57
Journal volume & issue
Vol. 5, no. 1
p. 57

Abstract

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Abstract Background Conventional prenatal screening tests, such as maternal serum tests and ultrasound scan, have limited resolution and accuracy. Methods We developed an advanced noninvasive prenatal diagnosis method based on massively parallel sequencing. The Noninvasive Fetal Trisomy (NIFTY) test, combines an optimized Student’s t-test with a locally weighted polynomial regression and binary hypotheses. We applied the NIFTY test to 903 pregnancies and compared the diagnostic results with those of full karyotyping. Results 16 of 16 trisomy 21, 12 of 12 trisomy 18, two of two trisomy 13, three of four 45, X, one of one XYY and two of two XXY abnormalities were correctly identified. But one false positive case of trisomy 18 and one false negative case of 45, X were observed. The test performed with 100% sensitivity and 99.9% specificity for autosomal aneuploidies and 85.7% sensitivity and 99.9% specificity for sex chromosomal aneuploidies. Compared with three previously reported z-score approaches with/without GC-bias removal and with internal control, the NIFTY test was more accurate and robust for the detection of both autosomal and sex chromosomal aneuploidies in fetuses. Conclusion Our study demonstrates a powerful and reliable methodology for noninvasive prenatal diagnosis.

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