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利用母体血浆 DNA 的大规模平行测序进行无创性产前检测:从分子核型分析到胎儿全基因组测序。

Non-invasive prenatal testing using massively parallel sequencing of maternal plasma DNA: from molecular karyotyping to fetal whole-genome sequencing.

机构信息

Li Ka Shing Institute of Health Sciences and Department of Chemical Pathology, The Chinese University of Hong Kong, Prince of Wales Hospital, Shatin, New Territories, Hong Kong SAR, China.

出版信息

Reprod Biomed Online. 2013 Dec;27(6):593-8. doi: 10.1016/j.rbmo.2013.08.008. Epub 2013 Sep 7.

Abstract

The discovery of cell-free fetal DNA in maternal plasma in 1997 has stimulated a rapid development of non-invasive prenatal testing. The recent advent of massively parallel sequencing has allowed the analysis of circulating cell-free fetal DNA to be performed with unprecedented sensitivity and precision. Fetal trisomies 21, 18 and 13 are now robustly detectable in maternal plasma and such analyses have been available clinically since 2011. Fetal genome-wide molecular karyotyping and whole-genome sequencing have now been demonstrated in a number of proof-of-concept studies. Genome-wide and targeted sequencing of maternal plasma has been shown to allow the non-invasive prenatal testing of β-thalassaemia and can potentially be generalized to other monogenic diseases. It is thus expected that plasma DNA-based non-invasive prenatal testing will play an increasingly important role in future obstetric care. It is thus timely and important that the ethical, social and legal issues of non-invasive prenatal testing be discussed actively by all parties involved in prenatal care.

摘要

1997 年,科学家在母体血浆中发现了游离的胎儿 DNA,这一发现极大地推动了非侵入性产前检测技术的发展。近年来,高通量测序技术的出现使得分析循环游离胎儿 DNA 的灵敏度和精确度达到了前所未有的水平。目前,母体血浆中可可靠地检测到胎儿 21、18 和 13 三体,自 2011 年以来,这些分析方法已在临床上得到应用。在一些概念验证研究中已经证明了胎儿全基因组分子核型分析和全基因组测序。全基因组和靶向测序的母体血浆已经被证明可以进行非侵入性产前检测β-地中海贫血,并有可能推广到其他单基因疾病。因此,基于血浆 DNA 的非侵入性产前检测预计将在未来的产科护理中发挥越来越重要的作用。因此,积极讨论非侵入性产前检测的伦理、社会和法律问题是非常及时和重要的,这涉及到所有参与产前保健的各方。

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