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妊娠期糖尿病、缺铁性贫血和妊娠期高血压孕妇母血中胎儿DNA的定量分析。

Quantitative analysis of fetal DNA in maternal plasma in gestational diabetes mellitus, iron deficiency anemia and gestational hypertension pregnancies.

作者信息

Zamanpoor Mansour, Rosli Rozita, Yazid Mohd Nazri, Husain Zaheed, Nordin Norshariza, Thilakavathy Karuppiah

机构信息

Genetic Medicine Research Centre, Faculty of Medicine and Health Sciences, Universiti Putra Malaysia, Selangor, Malaysia.

出版信息

J Matern Fetal Neonatal Med. 2013 Jul;26(10):960-6. doi: 10.3109/14767058.2013.766710. Epub 2013 Feb 20.

Abstract

OBJECTIVE

To quantify circulating fetal DNA (fDNA) levels in the second and third trimesters of normal healthy pregnant individuals and pregnant women with the following clinical conditions: gestational diabetes mellitus (GDM), iron deficiency anemia and gestational hypertension (GHT).

METHODS

The SRY gene located on the Y chromosome was used as a unique fetal marker. The fDNA was extracted from maternal plasma and the SRY gene concentrations were measured by quantitative real-time polymerase chain reaction (PCR) amplification using TaqMan dual labeled probe system.

RESULTS

No significant differences were observed in the mean fDNA concentration between normal and GDM pregnancy samples (p > 0.05) and also between normal and anemic pregnancy samples (p > 0.05) in both trimesters, but significant differences were observed between the third trimester normal and GHT pregnancy samples (p = 0.001). GDM and iron deficiency anemia do not affect the levels of fDNA in maternal plasma while GHT significantly elevates the levels of fDNA in maternal plasma.

CONCLUSIONS

Increased amount of circulating fDNA in maternal plasma could be used for early identification of adverse pregnancies. GDM and anemia do not affect the levels of fDNA in maternal plasma while GHT significantly elevates the levels of fDNA in maternal plasma. Hence, the elevated fDNA values could be used as a potential screening marker in pregnancies complicated with GHT but not with GDM and iron deficiency anemia.

摘要

目的

量化正常健康孕妇以及患有以下临床病症的孕妇(妊娠期糖尿病(GDM)、缺铁性贫血和妊娠高血压(GHT))在妊娠中期和晚期的循环胎儿DNA(fDNA)水平。

方法

将位于Y染色体上的SRY基因用作独特的胎儿标志物。从母血浆中提取fDNA,并使用TaqMan双标记探针系统通过定量实时聚合酶链反应(PCR)扩增来测量SRY基因浓度。

结果

在两个孕期中,正常妊娠样本与GDM妊娠样本之间(p>0.05)以及正常妊娠样本与贫血妊娠样本之间(p>0.05)的平均fDNA浓度均未观察到显著差异,但在妊娠晚期正常妊娠样本与GHT妊娠样本之间观察到显著差异(p = 0.001)。GDM和缺铁性贫血不影响母血浆中fDNA的水平,而GHT会显著提高母血浆中fDNA的水平。

结论

母血浆中循环fDNA量的增加可用于不良妊娠的早期识别。GDM和贫血不影响母血浆中fDNA的水平,而GHT会显著提高母血浆中fDNA的水平。因此,fDNA值升高可作为妊娠合并GHT而非GDM和缺铁性贫血的潜在筛查标志物。

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