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2q37.3缺失综合征:两例具有高度独特面部表型、与精神分裂症性精神病关联不一致且在2q37.3上存在共享缺失断点区域的病例。

2q37.3 Deletion Syndrome: Two Cases with Highly Distinctive Facial Phenotype, Discordant Association with Schizophrenic Psychosis, and Shared Deletion Breakpoint Region on 2q37.3.

作者信息

Mehraein Yasmin, Pfob Martina, Steinlein Ortrud, Aichinger Eric, Eggert Marlene, Bubendorff Valerie, Mannhart Adelina, Müller Stefan

机构信息

Institute of Human Genetics, University Hospital, Ludwig Maximilian University of Munich, Munich, Germany.

出版信息

Cytogenet Genome Res. 2015;146(1):33-8. doi: 10.1159/000431389. Epub 2015 Jun 19.

Abstract

2q37.3 deletion syndrome belongs to the chromosomal 2q37 deletion spectrum which clinically resembles Albright hereditary osteodystrophy (AHO) syndrome. It is is mainly characterized by short stature, obesity, round face, brachydactyly type E, intellectual disability, behavioral problems, and variable intellectual deficits. Different from classical AHO syndrome, patients with 2q37 deletion syndrome lack renal parathyroid hormone resistance (pseudohypoparathyroidism) and soft tissue ossification. So far, deletion mapping or molecular breakpoint analyses of 2q37 have been performed in only few patients. Here, we report on 2 patients with 2q37.3 deletion syndrome. In both patients the breakpoint of the 5.5-Mb terminal microdeletion could be narrowed down to the same ∼ 200-kb interval on 2q37.3 by BAC-FISH and/or array-CGH. Flanking low-copy repeats may indicate a classical microdeletion syndrome genesis for the 2q37.3 microdeletion subgroup. Clinical evaluation revealed intellectual deficits and type E brachydactyly typical for classical AHO syndrome together with distinctive facial dysmorphisms not present in the former. Furthermore, one patient presented with schizophrenic psychosis, an observation that would be in accordance with previous reports about an association between schizophrenia susceptibility and an unknown gene within the chromosomal region 2q37.

摘要

2q37.3缺失综合征属于染色体2q37缺失谱系,临床上类似于奥尔布赖特遗传性骨营养不良(AHO)综合征。其主要特征为身材矮小、肥胖、圆脸、E型短指、智力残疾、行为问题以及不同程度的智力缺陷。与经典的AHO综合征不同,2q37缺失综合征患者不存在肾甲状旁腺激素抵抗(假性甲状旁腺功能减退)和软组织骨化现象。迄今为止,仅对少数患者进行了2q37的缺失定位或分子断点分析。在此,我们报告2例2q37.3缺失综合征患者。通过BAC-FISH和/或阵列比较基因组杂交技术,在这2例患者中,5.5兆碱基末端微缺失的断点均被缩小至2q37.3上相同的约200千碱基区间。侧翼低拷贝重复序列可能提示2q37.3微缺失亚组存在典型的微缺失综合征成因。临床评估显示,患者存在经典AHO综合征典型的智力缺陷和E型短指,同时伴有前者所没有的独特面部畸形。此外,1例患者出现精神分裂症性精神病,这一观察结果与先前关于精神分裂症易感性与染色体区域2q37内未知基因之间关联的报道相符。

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