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使用游离胎儿 DNA 和 RNA 于母体外周血中进行非侵入性性染色体异常检测:最新进展与未来展望。

Non-invasive aneuploidy detection using free fetal DNA and RNA in maternal plasma: recent progress and future possibilities.

机构信息

Department of Obstetrics/Gynaecology, VU University Medical Center, De Boelelaan 1117, 1081 HV Amsterdam, The Netherlands.

出版信息

Hum Reprod Update. 2011 May-Jun;17(3):372-82. doi: 10.1093/humupd/dmq054. Epub 2010 Nov 12.

DOI:10.1093/humupd/dmq054
PMID:21076134
Abstract

BACKGROUND

Cell-free fetal DNA (cff DNA) and RNA can be detected in maternal plasma and used for non-invasive prenatal diagnostics. Recent technical advances have led to a drastic change in the clinical applicability and potential uses of free fetal DNA and RNA. This review summarizes the latest clinical developments in non-invasive prenatal diagnosis in the context of the latest technical developments.

METHODS

We searched PubMed with the search terms 'prenatal', 'non-invasive', 'fetal DNA', 'mRNA' and cross-referenced them with 'diagnostics', 'microRNA', 'aneuploidy', 'trisomy' and 'placenta'. We also searched the reference list of the articles identified by this search strategy.

RESULTS

Genome-wide methods have been, or can be, successfully applied on total DNA (DNA-seq), methylated DNA immunoprecipitation (with tiling array), microRNA (Megaplex) and total RNA (RNA-seq). Chromosome- or gene-specific assays have been successively applied on placenta RNA (allele ratio) or DNA multiplex ligation-dependent probe amplification (MLPA). These methods are reviewed for their merits and pitfalls with consideration of the placental biology. For the purpose of clarity, the technical and clinical characteristics are limited to non-invasive prenatal detection of chromosomal aneuploidies, with emphasis on trisomy 21.

CONCLUSIONS

The technical advances for non-invasive aneuploidy tests based on cff DNA and placental mRNA in maternal plasma have been enormous. Multimarker assays including genome-wide approaches with the option of qualitative information on variation (polymorphism or mutation) besides quantitative information are the preferred methods of choice. The time for population-based, double blind, large-scale clinical cohort trials has come.

摘要

背景

游离胎儿 DNA(cff DNA)和 RNA 可从母体血浆中检测到,可用于非侵入性产前诊断。最近的技术进步导致游离胎儿 DNA 和 RNA 的临床适用性和潜在用途发生了重大变化。本综述总结了在最新技术进展背景下非侵入性产前诊断的最新临床进展。

方法

我们使用术语“产前”、“非侵入性”、“胎儿 DNA”、“mRNA”在 PubMed 中进行检索,并与“诊断”、“microRNA”、“非整倍体”、“三体性”和“胎盘”交叉引用。我们还搜索了通过这种搜索策略确定的文章的参考文献列表。

结果

全基因组方法已成功应用于总 DNA(DNA-seq)、甲基化 DNA 免疫沉淀(带有平铺阵列)、microRNA(Megaplex)和总 RNA(RNA-seq)。染色体或基因特异性检测已成功应用于胎盘 RNA(等位基因比)或 DNA 多重连接依赖性探针扩增(MLPA)。考虑到胎盘生物学,我们对这些方法的优缺点进行了回顾。为了清晰起见,技术和临床特征仅限于非侵入性产前染色体非整倍体检测,重点是 21 三体。

结论

基于母体血浆中游离胎儿 DNA 和胎盘 mRNA 的非侵袭性非整倍体检测的技术进步是巨大的。多标记物检测包括全基因组方法,除了定量信息外,还具有变异(多态性或突变)的定性信息,是首选的方法。进行基于人群的、双盲的、大规模临床队列试验的时机已经成熟。

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