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胎盘介导的妊娠并发症中胎儿来源的高甲基化 RASSF1A 浓度的相关性。

Association of fetal-derived hypermethylated RASSF1A concentration in placenta-mediated pregnancy complications.

机构信息

Laboratory of Medical Genetics, Cheil General Hospital and Women's Healthcare Center, Seoul, Republic of Korea.

出版信息

Placenta. 2013 Jan;34(1):57-61. doi: 10.1016/j.placenta.2012.11.001. Epub 2012 Nov 24.

DOI:10.1016/j.placenta.2012.11.001
PMID:23187089
Abstract

OBJECTIVES

To assess whether fetal-derived hypermethylated RASSF1A concentrations in maternal plasma during pregnancy are altered in pregnancies associated with placental dysfunction manifested by intrauterine growth restriction (IUGR), preeclampsia (PE), or placental previa (PP) and whether this alteration can be detected in susceptible subjects before the onset of clinical disease.

METHODS

We performed a real-time quantitative polymerase chain reaction to quantify RASSF1A concentrations before and after methylation-sensitive restriction digestion in maternal plasma at 7-41 gestational weeks of normal pregnancies (n = 161), IUGR (n = 43), PE (n = 22), PP (n = 14) and non-pregnant women (n = 20).

RESULTS

A positive correlation was observed between fetal-derived hypermethylated RASSF1A concentration and gestational age for all study groups (r = 0.624, p < 0.001 for IUGR; r = 0.381, p = 0.042 for PE; r = 0.697, p < 0.001 for PP; r = 0.560, p < 0.001 for controls). The concentration of hypermethylated RASSF1A was relatively high at 7-14 gestational weeks in all patient groups. Hypermethylated RASSF1A concentration at 15-28 weeks was significantly higher in patients who subsequently developed IUGR (p = 0.002), PE (p < 0.001) or PP (p < 0.001) than in controls.

CONCLUSION

We first demonstrated increased concentration of fetal-derived hypermethylated RASSF1A sequences according to advancing gestation and before the onset of the clinical manifestation of pregnancy complications secondary to placental dysfunction, such as IUGR, PE and PP. Hypermethylated RASSF1A in maternal plasma may be useful as a potential biomarker to detect placental-mediated pregnancy complications, regardless of fetal gender and polymorphism.

摘要

目的

评估胎儿来源的 RASSF1A 在妊娠妇女血浆中的高甲基化浓度是否在与胎盘功能障碍相关的妊娠中发生改变,这些妊娠表现为宫内生长受限(IUGR)、子痫前期(PE)或前置胎盘(PP),以及这种改变是否可以在临床疾病发作前在易感受试者中检测到。

方法

我们在正常妊娠(n=161)、IUGR(n=43)、PE(n=22)、PP(n=14)和未怀孕妇女(n=20)的 7-41 孕周时,使用实时定量聚合酶链反应对母血浆中的 RASSF1A 浓度进行定量,该定量在甲基化敏感的酶切前后进行。

结果

对于所有研究组,胎儿来源的高甲基化 RASSF1A 浓度与胎龄呈正相关(IUGR:r=0.624,p<0.001;PE:r=0.381,p=0.042;PP:r=0.697,p<0.001;对照组:r=0.560,p<0.001)。在所有患者组中,高甲基化 RASSF1A 的浓度在 7-14 孕周时相对较高。在随后发生 IUGR(p=0.002)、PE(p<0.001)或 PP(p<0.001)的患者中,15-28 周的高甲基化 RASSF1A 浓度显著高于对照组。

结论

我们首次证明,根据妊娠的进展,在与胎盘功能障碍相关的妊娠并发症(如 IUGR、PE 和 PP)的临床表现出现之前,胎儿来源的高甲基化 RASSF1A 序列的浓度会增加。母体血浆中的高甲基化 RASSF1A 可能是一种有用的潜在生物标志物,可用于检测胎盘介导的妊娠并发症,而与胎儿性别和多态性无关。

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