不平衡易位8;Y (45,X,dic(Y;8)(q11.23;p23.1)):终端8p缺失的病例报告和回顾

K. Bosse , T. Eggermann , K. Van der Ven , R. Raff , H. Engels , G. Schwanitz
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引用次数: 7

摘要

本文报道一例罕见的新生不平衡Y/常染色体易位的男孩。该男孩的主要临床特征包括精神运动迟缓、扁平趾、头侧突出、耳后倾、眶上皮下组织丰满和鼻尖球根状。羊膜细胞的染色体分析显示单个X染色体和一个衍生8p染色体(核型:45,X,der(8)GTG)。随后的DAPI染色显示位于8p的Y染色体的失活着丝粒和异色物质Yq的缺失。利用Yp上的SRY和Yq上的DYS 240标记对胎儿血液DNA进行微卫星分析,证实存在精子发生相关因素。出生后FISH证实了8p的末端缺失。分子遗传学重鉴定显示8p单体为母系起源;因此,可以证明易位发生在受精卵中。8p基因的断点位于与心脏发育有关的基因GATA4的远端;我们的病人没有心脏问题的发现与GATA4二体的存在一致。只有FISH结合微卫星分析的应用才能在临床表型和末端8p的细微缺失之间建立精确的相关性;此外,可以排除父母复发的风险。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Unbalanced translocation 8;Y (45,X,dic(Y;8)(q11.23;p23.1)): case report and review of terminal 8p deletions

A boy with a rare unbalanced de novo Y/autosome translocation is presented. Main clinical features in the boy comprised a psychomotor delay, talipes planus, a dolichocephalus, low set and retroverted ears, supraorbital fullness of subcutaneous tissue and a bulbous nasal tip. Chromosomal analysis on amniocytes showed a single X chromosome and a derivative 8p (Karyotype: 45,X,der(8)GTG). The following DAPI staining revealed the inactivated centromere of the chromosome Y located on 8p and the absence of heterochromatic material Yq. Microsatellite analysis on fetal blood DNA using markers between SRY on Yp and DYS 240 on Yq proved presence of the spermatogenetic relevant factors. A terminal deletion of 8p was confirmed by FISH postnatally. Molecular genetic reassessment revealed the monosomy 8p to be of maternal origin; the translocation can thus be proven to have occurred in the zygote. The breakpoint in 8p was localised distal to GATA4, a gene which is involved in heart development; the finding that our patient did not suffer from cardiac problems agrees with the disomic presence of GATA4. Only the application of FISH combined with microsatellite analysis allowed a precise correlation between clinical phenotype and a subtle deletion of terminal 8p; futhermore, a recurrence risk for the parents could be excluded.

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