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Identification of copy number variants associated with BPES-like phenotypes

机译:鉴定与BPES样表型相关的拷贝数变异

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Blepharophimosis–Ptosis–Epicanthus inversus syndrome (BPES) is a well-characterized rare syndrome that includes an eyelid malformation associated with (type I) or without premature ovarian failure (type II). Patients with typical BPES have four major characteristics: blepharophimosis, ptosis, epicanthus inversus and telecanthus. Mutations in the FOXL2 gene, encoding a forkhead transcription factor, are responsible for the majority of both types of BPES. However, many patients with BPES-like features, i.e., having at least two major characteristics of BPES, have an unidentified cause. Here, we report on a group of 27 patients with BPES-like features, but without an identified genetic defect in the FOXL2 gene or flanking region. These patients were analyzed with whole-genome high-density arrays in order to identify copy number variants (CNVs) that might explain the BPES-like phenotype. In nine out of 27 patients (33%) CNVs not previously described as polymorphisms were detected. Four of these patients displayed psychomotor retardation as an additional clinical characteristic. In conclusion, we demonstrate that BPES-like phenotypes are frequently caused by CNVs, and we emphasize the importance of whole-genome copy number screening to identify the underlying genetic causes of these phenotypes.
机译:支气管上睑下垂—上睑下垂—Epicanthus逆综合征(BPES)是一种特征明确的罕见综合征,包括与(I型)或无卵巢早衰(II型)相关的眼睑畸形。患有典型BPES的患者具有四个主要特征:睑缘上睑下垂,眼睑下垂,上can倒and和长can。编码叉头转录因子的FOXL2基因突变是造成这两种类型BPES的主要原因。但是,许多具有BPES样特征的患者,即具有BPES的至少两个主要特征的患者,原因不明。在这里,我们报道了一组27例具有BPES样特征,但在FOXL2基因或侧翼区域未发现遗传缺陷的患者。用全基因组高密度阵列对这些患者进行分析,以鉴定可能解释BPES样表型的拷贝数变异(CNV)。在27例患者中,有9例(33%)检测到CNV,以前没有描述其多态性。这些患者中有四例表现出精神运动迟缓,这是另一种临床特征。总之,我们证明了BPES样表型经常是由CNV引起的,并且我们强调了全基因组拷贝数筛选对确定这些表型的潜在遗传原因的重要性。

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