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6 三体综合征的产前诊断挽救导致父源 UPD6 及新的胎盘发现。

Prenatal diagnosis of trisomy 6 rescue resulting in paternal UPD6 with novel placental findings.

机构信息

Department of Pathology, University of Pittsburgh Medical Center, Pennsylvania, USA.

出版信息

Am J Med Genet A. 2011 Aug;155A(8):1996-2002. doi: 10.1002/ajmg.a.34106. Epub 2011 Jul 7.

Abstract

Uniparental disomy (UPD) is defined by the inheritance of both copies of a chromosome pair from one single parent. Although 23 cases of paternal UPD6 have been reported earlier, the occurrence of trisomy 6 rescue with paternal UPD6 has not been previously reported. The phenotype of paternal UPD6 results from biallelic expression of the maternally imprinted, paternally expressed ZAC and HYMAI genes, and includes transient neonatal diabetes mellitus (TNDM), intra-uterine growth restriction (IUGR), macroglossia, and minor anomalies. Trisomy rescue has been proposed as a pathogenic mechanism leading to UPD of other chromosomes. We report on the first case of a prenatally diagnosed infant with UPD6 and describe the clinical, cytogenetic, molecular, and novel placental findings in a female infant with paternal UPD6. Low-level trisomy 6 and paternal UPD6 were prenatally diagnosed through amniocentesis. After birth trisomy 6 was documented in the placenta but was not found in three different cell lines from the infant. The placenta was small with a peculiar pattern of vascular proliferation. Our results of trisomy 6 cells predominantly present in the placenta and only in low levels in the amniotic fluid suggest that the distribution and proportion of trisomic and diploid UPD cells contribute to the variability of fetal and placental phenotypes.

摘要

单亲二体(UPD)是指一对染色体的两个拷贝均来自单一亲代的遗传。尽管先前已经报道了 23 例父源 UPD6,但父源 UPD6 伴三体 6 挽救的情况尚未见报道。父源 UPD6 的表型源自母源印记、父源表达的 ZAC 和 HYMAI 基因的双等位基因表达,包括短暂性新生儿糖尿病(TNDM)、宫内生长受限(IUGR)、巨舌和小畸形。三体挽救已被提议为导致其他染色体 UPD 的致病机制。我们报告了首例产前诊断的 UPD6 婴儿,并描述了一例父源 UPD6 女性婴儿的临床、细胞遗传学、分子和新型胎盘发现。通过羊膜穿刺术在产前诊断出低水平的三体 6 和父源 UPD6。出生后,在胎盘上发现了三体 6,但在婴儿的三个不同细胞系中未发现。胎盘较小,血管增殖呈特殊模式。我们关于三体 6 细胞主要存在于胎盘且仅在羊水低水平存在的结果表明,三体和二倍体 UPD 细胞的分布和比例有助于胎儿和胎盘表型的变异性。

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