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7号染色体缺失/12号染色体重复可能是一例无脑叶全前脑畸形病例的病因。

7q Deletion/12q Duplication Is the Possible Cause of an Alobar Holoprosencephaly Case.

作者信息

Paspaliaris Vassilis, Vrachnis Nikolaos, Iliodromiti Zoe, Antonakopoulos Nikolaos, Papaioannou Giorgos, Vlachadis Nikolaos, Anastasiadou Foteini, Sotiriou Sotirios, Garas Antonios, Thomaidis Lorreta, Manolakos Emmanouil

机构信息

Access to genome (ATG P.C.), Clinical Laboratory Genetics, University of Athens, Athens, Greece.

Evgenideio Hospital, University of Athens, Athens, Greece.

出版信息

Mol Syndromol. 2017 Dec;9(1):52-57. doi: 10.1159/000481972. Epub 2017 Nov 24.

Abstract

Holoprosencephaly (HPE) spectrum disorder is the most common congenital malformation of the human brain with absence of or incomplete midline cleavage. Its cause is heterogenic, making genetic counseling a challenge. In this case report, a pregnancy affected by alobar HPE is described. Using aCGH, an 8.9-Mb deletion at 7q36.1q36.3 together with a 4.9-Mb duplication at 12q24.32q24.33 is assumed to be the possible reason for this alobar HPE case. It is discussed that disruption of key elements of the developing brain, taking environmental factors into account, contributes to the HPE spectrum. The use of aCGH for invasive prenatal testing is starting to become the standard technique, providing accurate information about the cause of congenital diseases for couples receiving genetic counseling.

摘要

全前脑畸形(HPE)谱系障碍是人类大脑最常见的先天性畸形,表现为中线分裂缺失或不完全。其病因具有异质性,这使得遗传咨询成为一项挑战。在本病例报告中,描述了一例受无脑叶型HPE影响的妊娠。使用比较基因组杂交(aCGH)技术,推测7号染色体长臂36.1区至36.3区的8.9兆碱基缺失以及12号染色体长臂24.32区至24.33区的4.9兆碱基重复可能是该无脑叶型HPE病例的病因。讨论指出,考虑到环境因素,发育中大脑关键要素的破坏会导致HPE谱系障碍。aCGH用于侵入性产前检测正开始成为标准技术,可为接受遗传咨询的夫妇提供有关先天性疾病病因的准确信息。

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