首页> 外文期刊>European journal of medical genetics >Prenatal diagnosis of mosaicism for 11q terminal deletion.
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Prenatal diagnosis of mosaicism for 11q terminal deletion.

机译:产前诊断为11q末端缺失的镶嵌症。

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The phenotype of 11q terminal deletion also known as Jacobsen syndrome is a clinically well known entity whose diagnosis in infancy and childhood is based on clinical examination, hematological and cytogenetic findings. Hematological features in Jacobsen syndrome are very similar to those reported in Paris-Trousseau syndrome (PTS) which is also associated with11q terminal deletion. Karyotype analysis shows a variable terminal deletion from 11q23 sub-band extending to the telomere. Most often in patients with Jacobsen syndrome, this chromosomal deletion is present in all metaphases. We report on the identification of a distal 11q deletion in mosaic (20% of deleted cells) in a fetus ascertained after amniocentesis for maternal serum screening test indicative for Down syndrome. The present case is the third prenatal diagnosis of a mosaic for a distal 11q deletion with the lowest mosaicism rate. The 2D-ultrasound examination and cord blood hematological studies were useful to estimate the prognosis at term, considering the contribution of the mosaicism rate to the phenotypic variability in Jacobsen syndrome. The identification of mosaicism for distal 11q deletion is a very rare event in prenatal diagnosis. This case illustrates the complexity in genetic counselling for prenatally ascertained partial monosomy 11qter in mosaic.
机译:11q末端缺失的表型也称为Jacobsen综合征,是临床上众所周知的实体,其婴儿和儿童期的诊断基于临床检查,血液学和细胞遗传学发现。 Jacobsen综合征的血液学特征与Paris-Trousseau综合征(PTS)报道的血液学特征非常相似,后者也与11q末端缺失有关。核型分析显示从11q23子带延伸至端粒的可变末端缺失。在雅各布森综合症患者中,这种染色体缺失最常见于所有中期。我们报告了羊膜穿刺术确定唐氏综合症的母体血清筛查试验后确定的胎儿中远端11q缺失的镶嵌体(缺失细胞的20%)的鉴定。本例是第三次产前马赛克发生率最低的11q远端缺失马赛克的产前诊断。考虑到镶嵌率对雅各布森症候群表型变异性的贡献,二维超声检查和脐带血血液学研究有助于评估足月的预后。在产前诊断中,远端11q缺失的镶嵌性鉴定是非常罕见的事件。这个案例说明了在产前确定的镶嵌中11qter部分遗传性的遗传咨询的复杂性。

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