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Size-based molecular diagnostics using plasma DNA for noninvasive prenatal testing

三体 大规模并行测序 DNA 非整倍体 生物 胎儿游离DNA 产前诊断 分子生物学 胎儿 DNA测序 21号染色体 遗传学 染色体 怀孕 基因
作者
Stephanie C Y Yu,K.C. Allen Chan,Yama W. L. Zheng,Peiyong Jiang,Gary J. W. Liao,Hao Sun,Ranjit Akolekar,Tak Yeung Leung,Attie T. J. I. Go,J. M. G. van Vugt,Ryoko Minekawa,Cees B.M. Oudejans,K. H. Nicolaides,Rossa W. K. Chiu,Y. M. Dennis Lo
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [Proceedings of the National Academy of Sciences]
卷期号:111 (23): 8583-8588 被引量:259
标识
DOI:10.1073/pnas.1406103111
摘要

Noninvasive prenatal testing using fetal DNA in maternal plasma is an actively researched area. The current generation of tests using massively parallel sequencing is based on counting plasma DNA sequences originating from different genomic regions. In this study, we explored a different approach that is based on the use of DNA fragment size as a diagnostic parameter. This approach is dependent on the fact that circulating fetal DNA molecules are generally shorter than the corresponding maternal DNA molecules. First, we performed plasma DNA size analysis using paired-end massively parallel sequencing and microchip-based capillary electrophoresis. We demonstrated that the fetal DNA fraction in maternal plasma could be deduced from the overall size distribution of maternal plasma DNA. The fetal DNA fraction is a critical parameter affecting the accuracy of noninvasive prenatal testing using maternal plasma DNA. Second, we showed that fetal chromosomal aneuploidy could be detected by observing an aberrant proportion of short fragments from an aneuploid chromosome in the paired-end sequencing data. Using this approach, we detected fetal trisomy 21 and trisomy 18 with 100% sensitivity (T21: 36/36; T18: 27/27) and 100% specificity (non-T21: 88/88; non-T18: 97/97). For trisomy 13, the sensitivity and specificity were 95.2% (20/21) and 99% (102/103), respectively. For monosomy X, the sensitivity and specificity were both 100% (10/10 and 8/8). Thus, this study establishes the principle of size-based molecular diagnostics using plasma DNA. This approach has potential applications beyond noninvasive prenatal testing to areas such as oncology and transplantation monitoring.
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