班达尔阿巴斯市一项病例对照研究:妊娠期胎儿心室回声灶与胎儿染色体异常之间的相关性

Mazyar Rastegar, Shahrokh Rajaei, Negin Yazdian Anari, Seyyed Mohammad Hashemi, Amir Entezar Baghiatallah, Arezoo Ghazalgoo, Sholes Namazi, Saman Soltani Moghadam, M. Aleali, M. Keivanlou, Ehsan Amini-Salehi
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引用次数: 0

摘要

心室回声灶是一些胎儿心脏内的小结构。这些小区域是位于乳头肌附近的胎儿心室回声增高所致。有报道称这些病灶与胎儿染色体异常有关。考虑到染色体异常是产前死亡的主要原因,本研究旨在确定胎儿回声灶作为染色体异常标志物的价值。 一名经验丰富的心脏病专家对 149 名怀孕后三个月的孕妇进行了胎儿超声心动图检查。其中 75 例报告有阳性回声灶,74 例报告无回声灶。随后,对包括 21、18 和 13 三体在内的三种染色体异常进行了检查。这些个体的信息,包括胎龄和回声灶,均已记录在案。 根据本研究的结果,7 名婴儿(4.7%)患有 21 三体综合征,4 名婴儿(2.7%)患有 13 三体综合征,6 名婴儿(4.1%)患有 18 三体综合征。出现阳性和阴性回声病灶的孕妇的平均孕龄分别为(21.07±3.23)岁和(21.03±3.09)岁。未发现心室回声灶与 21、18 或 13 三体症有明显关系。 本研究表明,回声灶的存在与染色体三体之间无明显关系。这一发现表明,当出现心内回声灶时,尤其是在高风险胎儿中,需要进行额外的检查来确认染色体异常。此外,没有回声灶并不能排除染色体疾病。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Correlation between fetal ventricular echogenic foci in pregnancy and fetus chromosomal anomaly, a case-control study in bandar abbas city
Ventricular echogenic foci are small structures within the hearts of some fetuses. These small areas result from increased echogenicity in the ventricles of fetuses located near the papillary muscles. An association between these foci and chromosomal abnormalities in fetuses has been reported. Considering that chromosomal abnormalities are a major cause of prenatal death, this study aimed to determine the value of fetal echogenic foci as markers for chromosomal abnormalities. Fetal echocardiography was performed by an experienced cardiologist on 149 pregnant women in the second trimester. Of these, 75 were reported to have positive echogenic foci, and 74 were reported to have no echogenic foci. Subsequently, the three chromosomal anomalies including trisomies 21, 18, and 13 were examined. The information of the individuals, including gestational age and echogenic foci, was recorded. Based on the findings of the present study, seven infants (4.7%) had trisomy 21, four infants (2.7%) had trisomy 13, and six infants (4.1%) had trisomy 18. The mean gestational age of pregnant women with positive and negative echogenic foci was 21.07±3.23 and 21.03±3.09, respectively. No significant relationship was found between ventricular echogenic foci and trisomy 21, 18, or 13. The present study suggests no significant relation between the presence of echogenic foci and chromosomal trisomies. This finding indicates that additional tests are required to confirm chromosomal abnormalities when echogenic intracardiac foci are present, especially in high-risk fetuses. Moreover, the absence of echogenic focus does not rule out chromosomal disorders.
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