MicroRNA biomarkers for early detection of embryonic malformations in pregnancy.

Xuezheng Li, Zhiyong Zhao
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引用次数: 6

Abstract

Congenital birth defects, manifested in newborn infants, are formed during early embryogenesis. Targeted and individualized interventions to prevent birth defects require early detection of risk and signs of developmental abnormalities. Current diagnosis of structural anomalies largely relies on ultrasonography, which can only detect abnormities after their formation in fetuses. Biomolecules, mainly proteins, in maternal blood have been used as indicators of fetal anomalies; however, they lack adequate sensitivity for detecting embryonic malformations. Recently, cell-free microRNAs (miRNAs) have been found in blood and evaluated as biomarkers for diseases. Expression of certain miRNAs in maternal plasma has been shown to be correlated with birth defects in infants. Although their reliability and sensitivity remain to be validated, miRNAs, which can be amplified and sequenced, are potentially sensitive and specific biomarkers for early embryonic dysmorphogenesis.

Abstract Image

早期检测妊娠期胚胎畸形的MicroRNA生物标志物。
先天性出生缺陷,表现在新生儿,形成于早期胚胎发生。预防出生缺陷的针对性和个体化干预需要及早发现发育异常的风险和迹象。目前结构异常的诊断主要依赖于超声检查,超声检查只能在胎儿形成后发现异常。母亲血液中的生物分子(主要是蛋白质)已被用作胎儿异常的指标;然而,它们在检测胚胎畸形方面缺乏足够的灵敏度。近年来,在血液中发现了无细胞microRNAs (miRNAs),并被评价为疾病的生物标志物。母体血浆中某些mirna的表达已被证明与婴儿出生缺陷相关。虽然它们的可靠性和敏感性仍有待验证,但mirna可以扩增和测序,是早期胚胎畸形发生的潜在敏感和特异性生物标志物。
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