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首页> 外文期刊>Molecular diagnosis & therapy >Circulating Nucleic Acids in Maternal Plasma and Serum in Pregnancy Complications: Are They Really Useful in Clinical Practice? A Systematic Review
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Circulating Nucleic Acids in Maternal Plasma and Serum in Pregnancy Complications: Are They Really Useful in Clinical Practice? A Systematic Review

机译:孕妇血浆和血清循环核酸在妊娠并发症中:它们在临床实践中真正有用吗? 系统评价

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摘要

Objective A systematic review was carried out to summarize the available evidence to assess whether circulating nucleic acids in maternal plasma and serum (CNAPS) have the potential to serve as extra and independent markers for the prediction and/or progression monitoring of the most common and severe complications of pregnancy, including preeclampsia, intrauterine growth restriction, preterm delivery, morbidly adherent placenta, gestational diabetes, antiphospholipid syndrome, threatened abortion, intrahepatic cholestasis of pregnancy, and hyperemesis gravidarum. Method A comprehensive literature search of the MEDLINE (PubMed), EMBASE, and ISI Web of Knowledge databases was conducted to identify relevant studies that included amounts of CNAPS in the abovementioned pregnancy complications. Results Eighty-three studies met the eligibility criteria. The vast majority of studies were conducted on the quantity of total circulating cell free DNA (cfDNA) and cell free fetal DNA (cffDNA), and some were conducted on messenger RNA (mRNA) species. A few studies have instead evaluated the cell free DNA fetal fraction (cfDNAff), but only in a limited number of pregnancy complications. Despite the growing interest and the abundance of the papers available, little information is available for other new CNAPS, including microRNA (miRNA), long noncoding RNA (lncRNA), mitochondrial DNA (mtDNA), and circular RNA. Conclusion Due to the heterogeneity of the populations enrolled, the scarcity of the studies that adjusted the CNAPS values for possible confounding factors, and the difficulty in interpreting the published data, no conclusion regarding the statistical robustness and clinical relevance of the data can be made at present. If assayed at the third trimester, the CNAPS have, however, shown better performance, and could be used in populations already at risk of developing complications as suggested by the presence of other clinical features. Other CNAPS, including miRNA, are under investigation, especially for the screening of gestational diabetes mellitus, but no data about their clinical utility are available. Circulating DNA (cfDNA, cffDNA, and cfDNAff) and mRNA have not been properly evaluated yet, especially in patients asymptomatic early in pregnancy but who developed complications later, perhaps because of the high cost of these techniques and the availability of other predictors of pregnancy complications (biochemical, biophysical, and ultrasound markers). Therefore, from the analysis of the data, the positive predictive value is not available. As regards the new CNAPS, including miRNA, there are still no sufficient data to understand if they can be promising markers for pregnancy complications monitoring and screening, since CNAPS are statistically weak and expensive. It is reasonable to currently conclude that the use of the CNAPS in clinical practice is not recommended.
机译:目的进行系统审查,以总结可用证据,以评估母体血浆和血清(CNAPS)中是否具有潜在的额外和独立标记,用于预测和/或进展监测最常见和严重的预测和/或进展监测怀孕的并发症,包括预口兰,宫内生长限制,早产,病因粘附胎盘,妊娠期糖尿病,抗磷脂综合征,威胁堕胎,妊娠肝内胆汁淤积,和高血压妊娠。方法进行了综合文献搜索了知识数据库的Medline(PubMed),Embase和ISI网站,以确定相关的研究,包括上述妊娠并发症中的CNAP。结果八十三项研究达到了资格标准。在总循环间无菌DNA(CFDNA)和无细胞胎儿DNA(CFFDNA)的量上进行了绝大多数研究,有些研究在信使RNA(mRNA)物种上进行。少数研究已经评估了无细胞DNA胎儿级分(CFDNAFF),而是仅在有限数量的妊娠并发症中。尽管兴趣越来越多,但可用的论文的丰富性,但其他新的CNAP,包括MicroRNA(miRNA),长的非编码RNA(LNCRNA),线粒体DNA(MTDNA)和圆形RNA。结论由于群体的异质性,调整CNAPS值对于可能的混淆因素的研究的稀缺性,以及解释公布数据的困难,没有关于数据的统计稳健性和临床相关性的结论展示。如果在第三个三个月进行测定,则CNAPS具有更好的性能,并且可以用于已经有可能在存在其他临床特征的情况下表达并发症的风险的群体中。其他CNAPS,包括miRNA,特别是对妊娠期糖尿病的筛查,但没有关于其临床效用的数据。尚未适当评估循环DNA(CFDNA,CFFDNA和CFDNAFF)和mRNA,特别是在怀孕早期的患者中,但是由于这些技术的高成本和妊娠并发症的其他预测因子的高成本以及其他预测因子的高成本而言,也许是在妊娠早期的患者中。 (生物化学,生物物理和超声标记)。因此,从数据的分析中,阳性预测值不可用。关于新的CNAPS,包括miRNA,仍然没有足够的数据来了解妊娠并发症监测和筛查的有前途的标志,因为CNAPS在统计上弱和昂贵。目前得出结论是合理的,即不建议使用CNAP在临床实践中的使用。

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