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Proximal 21q deletion as a result of a de novo unbalanced t(12;21) translocation in a patient with dysmorphic features, hepatomegaly, thick myocardium and delayed psychomotor development

机译:近21Q缺失,由于患者在患者中易患具有疑似特征的患者,肝脏肿大,厚心肌和延迟精神接受发育的临近21Q缺失

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IInterstitial 21q deletions can cause a wide spectrum of symptoms depending on the size and the location of the deletion. It has previously been suggested that the long arm of chromosome 21 can be divided into three regions based on the clinical severity of the patients and deletion of the region from 32.3 Mb to 37.1 Mb was more crucial than the deletion of other regions. In this study we describe a female patient with dysmorphic features, hepatomegaly, thick myocardium and psychomotor delay. Conventional karyotyping was initially interpreted as full monosomy 21, but subsequent chromosome microarray analysis suggested an approximately 18 Mb partial monosomy. Re-evaluation of the karyotype and fluorescence in situ hybridization revealed deletion of the proximal 21q11.2-q22.11 segment and insertion of 21q22.11-qter to 12qter. The deletion of the present case overlaps with two of the proposed regions including part of the proposed crucial region. This report emphasizes the relevance of investigating suspected full monosomies with high resolution methods and FISH in order to investigate the extent of the deletion and the presence of more complex rearrangements.
机译:IinterStitial 21Q删除可以根据删除的尺寸和位置造成广泛的症状。先前已经提出,染色体21的长臂可以基于患者的临床严重程度分为三个区域,并且从32.3MB到37.1 MB的区域缺失比其他地区的缺失更为关键。在这项研究中,我们描述了一种患有瘤畸形特征,肝肿大,厚心肌和精神热延迟的女性患者。常规的核型化最初被解释为全单体21,但随后的染色体微阵列分析表明了大约18 Mb的部分单糖果。原位杂交的核型和荧光重新评估揭示了近摄21Q11.2-Q22.11分段和插入21Q22.11- quter至12时的缺失。删除本病例与两个拟议区域中的两个重叠,包括所提出的至关重要区域的一部分。本报告强调了具有高分辨率方法和鱼类的可疑全单体的相关性,以研究缺失的程度和更复杂重排的存在。

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