PLAGL1 epimutation and bladder exstrophy: Coincidence or concurrent etiology?

Q Medicine

Birth defects research. Part A, Clinical and molecular teratology Pub Date : 2016-05-25 DOI:10.1002/bdra.23521

Julia Kolarova, Susanne Bens, Ole Ammerpohl, Alina C. Hilger, Rong Zhang, Heiko Reutter, Reiner Siebert

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引用次数: 2

Abstract

Background

The bladder exstrophy-epispadias complex (BEEC) is characterized by a spectrum of genitourinary malformations. Both classical bladder exstrophy and the most severe phenotype, exstrophy of the cloaca, display omphaloceles, a cardinal anomaly of some disorders caused by altered imprinting. Therefore, we hypothesized that BEEC in some patients could occur on the basis of an undiagnosed imprinting disorder. Such altered imprinting is associated with changes in the parent-of-origin-specific DNA methylation.

Methods

We analyzed the DNA methylation of 54 imprinted loci in 23 selected patients with different BEEC subtypes (epispadias n = 1, classical bladder exstrophy n = 10, exstrophy of the cloaca n = 12) using the Infinium HumanMethylation450 BeadChip. A total of 471,722 not imprinted autosomal CpG loci and 891 imprinted CpG loci were investigated. Findings were corroborated by methylation-specific-multiplex ligation-dependent probe amplification (MS-MLPA) and microsatellite analysis.

Results

No significant differences in the DNA methylation of the not imprinted and imprinted CpG were observed depending on subtype of BEEC. Nevertheless, in 1 of the 23 patients who displayed a classical bladder exstrophy, we detected hypomethylation of the imprinted PLAGL1 locus in chromosome 6q24. We verified this hypomethylation by MS-MLPA and showed further the methylation loss to be caused most likely by a mosaic epimutation.

Conclusion

Considering that it is highly unlikely to detect a PLAGL1 epimutation among 23 individuals given the low incidence of this alteration in the population, our observations further support a link between BEEC and imprinting disorders. Birth Defects Research (Part A) 106:724–728, 2016. © 2016 Wiley Periodicals, Inc.

查看原文本刊更多论文

PLAGL1脱位和膀胱外翻:是巧合还是同时的病因?

背景:膀胱外翻-上尿道复合体(BEEC)以一系列泌尿生殖系统畸形为特征。典型的膀胱外翻和最严重的表现型，泄殖腔外翻，都表现出脐膨出，这是一些由印记改变引起的疾病的主要异常。因此，我们假设一些患者的BEEC可能发生在未确诊的印迹障碍的基础上。这种改变的印记与父母起源特异性DNA甲基化的变化有关。方法采用Infinium HumanMethylation450芯片，对23例不同BEEC亚型患者(1例尿道外翻、10例膀胱外翻、12例泄殖腔外翻)的54个印迹位点进行DNA甲基化分析。共研究了471,722个非印迹常染色体CpG位点和891个印迹CpG位点。研究结果通过甲基化特异性多重连接依赖探针扩增(MS-MLPA)和微卫星分析得到证实。结果在不同的BEEC亚型中，未印迹和印迹CpG的DNA甲基化没有显著差异。然而，在23例典型膀胱外翻患者中的1例中，我们检测到6q24染色体上印迹PLAGL1位点的低甲基化。我们通过MS-MLPA验证了这种低甲基化，并进一步表明甲基化损失很可能是由马赛克增殖引起的。考虑到在23个个体中检测到PLAGL1突变的可能性非常低，我们的观察结果进一步支持了BEEC与印迹疾病之间的联系。出生缺陷研究(A辑)106:724-728,2016。©2016 Wiley期刊公司

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Birth defects research. Part A, Clinical and molecular teratology 医药科学, 胎儿发育与产前诊断, 生殖系统/围生医学/新生儿

CiteScore

1.86

自引率

0.00%

发文量

审稿时长

3 months