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Differing Microdeletion Sizes and Breakpoints in Chromosome 7q11.23 in Williams-Beuren Syndrome Detected by Chromosomal Microarray Analysis

机译:染色体微阵列分析检测威廉姆斯-布伦综合征的染色体7q11.23中不同的微缺失大小和断裂点。

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摘要

Williams-Beuren syndrome (WBS) manifests as supravalvular aortic stenosis, intellectual disability, developmental delay and characteristic facial features. The common WBS deletion region ranges from 1.55 to 1.84 Mb and primarily contains the ELN gene. We analyzed 10 patients diagnosed with 7q11.23 microdeletion syndrome by chromosomal microarray analysis. The clinical features of these patients varied from classic WBS to normal phenotype. All 10 patients exhibited different sizes and breakpoints of chromosome microdeletions ranging from 44 kb to 9.88 Mb. The hemizygosity of the ELN gene was detected in 7 patients, while a normal ELN gene was present in 3 other patients with small deletions. We observed that the phenotypic features of WBS varied in fetuses, children and adults, influenced by the genes, deletion size and breakpoint. Our findings provide more information on the genotype-phenotype correlations of WBS. However, further research is needed to explore the size and breakpoint effect and functions of the genes on chromosome 7q11.23.
机译:Williams-Beuren综合征(WBS)表现为瓣上主动脉瓣狭窄,智力障碍,发育迟缓和特征性面部特征。常见的WBS缺失区范围为1.55至1.84 Mb,主要包含ELN基因。我们通过染色体微阵列分析分析了10例诊断为7q11.23微缺失综合症的患者。这些患者的临床特征从经典WBS到正常表型不等。所有10位患者的染色体微缺失的大小和断裂点均不同,范围从44 kb至9.88 Mb。在7例患者中检测到ELN基因的半合子性,而在其他3例患者中,有少量缺失的患者中存在正常的ELN基因。我们观察到WBS的表型特征在胎儿,儿童和成人中有所不同,受基因,缺失大小和断点的影响。我们的发现提供了有关WBS基因型与表型相关性的更多信息。然而,需要进一步研究以探索染色体7q11.23上的基因的大小,断点作用和功能。

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