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首页> 外文期刊>Annals of the New York Academy of Sciences >Fetal Nucleic Acids in Maternal Body Fluids: An Update
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Fetal Nucleic Acids in Maternal Body Fluids: An Update

机译:母体液中的胎儿核酸:最新进展

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摘要

Our laboratory continues to be actively involved in the development of new biomarkers for prenatal diagnosis using maternal blood and amniotic fluid. We have also developed a mouse model that demonstrates that cell-free fetal (cff) DNA is detectable in the pregnant maternal mouse. In human maternal plasma and serum we have analyzed factors that are important in the clinical interpretation of cff DNA levels. Maternal race, parity, and type of conception (natural or assisted) do not affect cff DNA levels, but maternal weight does. We have also analyzed the relationship between placental volume, using a three-dimensionsal ultrasound examination, and cff DNA levels. Surprisingly, there is no association between these values. Finally, we are using specific disease models (such as congenital diaphragmatic hernia and twin-to-twin transfusion) to understand the effects of gestational age and specific pathology on fetal gene expression by analyzing cell-free mRNA levels in maternal plasma. In the amniotic fluid we have focused on improvements in recovery of cff DNA and mRNA. By optimizing recovery we have made some interesting observations about differences in fetal DNA between blood and amniotic fluid. In addition, we have successfully hybridized cff DNA in amniotic fluid to DNA microarrays, permitting assessment of fetal molecular karyotype. We also have preliminary data on fetal gene expression in amniotic fluid. Finally, we remain actively involved in promoting noninvasive prenatal testing in the United States, such as encouraging the use of fetal DNA for fetal rhesus D assessment. On the other hand, we are cautious and concerned about the accuracy of "at-home" kits for fetal gender detection.
机译:我们的实验室继续积极参与使用孕妇血液和羊水进行产前诊断的新生物标记物的开发。我们还开发了一种小鼠模型,该模型证明在孕妇母鼠中可检测到无细胞胎儿(cff)DNA。在人类孕妇血浆和血清中,我们分析了对cff DNA水平的临床解释很重要的因素。孕产妇的种族,性别和受孕类型(自然的或辅助的)不会影响cff DNA的水平,但孕产妇的体重会影响。我们还使用三维扫描检查了胎盘体积与cff DNA水平之间的关系。令人惊讶的是,这些值之间没有关联。最后,我们使用特定的疾病模型(例如先天性diaphragm疝和双胎输血)通过分析母体血浆中无细胞的mRNA水平来了解胎龄和特定病理对胎儿基因表达的影响。在羊水中,我们致力于改善cff DNA和mRNA的回收率。通过优化恢复,我们对血液和羊水之间胎儿DNA的差异做了一些有趣的观察。此外,我们已经成功地将羊水中的cff DNA与DNA微阵列杂交,从而可以评估胎儿分子核型。我们也有关于羊水中胎儿基因表达的初步数据。最后,我们仍在美国积极参与促进无创性产前检查,例如鼓励使用胎儿DNA进行胎儿恒河猴D评估。另一方面,我们对胎儿性别检测“在家”工具包的准确性持谨慎和关注的态度。

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