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An Optimized Method for Accurate Fetal Sex Prediction and Sex Chromosome Aneuploidy Detection in Non-Invasive Prenatal Testing

机译:非侵入性产前检查中准确进行胎儿性别预测和性染色体非整倍性检测的优化方法

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摘要

Massively parallel sequencing (MPS) combined with bioinformatic analysis has been widely applied to detect fetal chromosomal aneuploidies such as trisomy 21, 18, 13 and sex chromosome aneuploidies (SCAs) by sequencing cell-free fetal DNA (cffDNA) from maternal plasma, so-called non-invasive prenatal testing (NIPT). However, many technical challenges, such as dependency on correct fetal sex prediction, large variations of chromosome Y measurement and high sensitivity to random reads mapping, may result in higher false negative rate (FNR) and false positive rate (FPR) in fetal sex prediction as well as in SCAs detection. Here, we developed an optimized method to improve the accuracy of the current method by filtering out randomly mapped reads in six specific regions of the Y chromosome. The method reduces the FNR and FPR of fetal sex prediction from nearly 1% to 0.01% and 0.06%, respectively and works robustly under conditions of low fetal DNA concentration (1%) in testing and simulation of 92 samples. The optimized method was further confirmed by large scale testing (1590 samples), suggesting that it is reliable and robust enough for clinical testing.
机译:大规模并行测序(MPS)与生物信息学分析相结合已被广泛应用于通过从母体血浆中对无细胞胎儿DNA(cffDNA)进行测序来检测胎儿染色体非整倍性,如21、18、13三体性染色体和性染色体非整倍性(SCA)。称为非侵入性产前检查(NIPT)。但是,许多技术挑战,例如对正确的胎儿性别预测的依赖,Y染色体测量的较大变化以及对随机读数映射的高度敏感性,可能导致胎儿性别预测中较高的假阴性率(FNR)和假阳性率(FPR)。以及SCA检测中。在这里,我们开发了一种优化方法,通过滤除Y染色体六个特定区域中的随机映射读段来提高当前方法的准确性。该方法将胎儿性别预测的FNR和FPR分别从近1%降低到0.01%和0.06%,并且在92个样本的测试和模拟中在低胎儿DNA浓度(1%)的条件下具有良好的效果。大规模测试(1590个样本)进一步证实了该优化方法的有效性,表明该方法可靠且鲁棒,足以用于临床测试。

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