首页> 外文期刊>European journal of human genetics: EJHG >Exon deletions of the EP300 and CREBBP genes in two children with Rubinstein-Taybi syndrome detected by aCGH.
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Exon deletions of the EP300 and CREBBP genes in two children with Rubinstein-Taybi syndrome detected by aCGH.

机译:通过aCGH检测到的两名Rubinstein-Taybi综合征儿童的EP300和CREBBP基因外显子缺失。

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摘要

We demonstrate the utility of an exon coverage microarray platform in detecting intragenic deletions: one in exons 24-27 of the EP300 gene and another in exons 27 and 28 of the CREBBP gene in two patients with Rubinstein-Taybi syndrome (RSTS). RSTS is a heterogeneous disorder in which approximately 45-55% of cases result from deletion or mutations in the CREBBP gene and an unknown portion of cases result from gene changes in EP300. The first case is a 3-year-old female with an exonic deletion of the EP300 gene who has classic facial features of RSTS without the thumb and great toe anomalies, consistent with the milder skeletal phenotype that has been described in other RSTS cases with EP300 mutations. In addition, the mother of this patient also had preeclampsia during pregnancy, which has been infrequently reported. The second case is a newborn male who has the classical features of RSTS. Our results illustrate that exon-targeted array comparative genomic hybridization (aCGH) is a powerful tool for detecting clinically significant intragenic rearrangements that would be otherwise missed by aCGH platforms lacking sufficient exonic coverage or sequencing of the gene of interest.
机译:我们证明了外显子覆盖微阵列平台在检测基因内缺失中的作用:在两名患有鲁宾斯坦-泰比综合征(RSTS)的患者中,EP300基因的外显子24-27中一个,CREBBP基因的外显子27和28中另一个。 RSTS是一种异质性疾病,其中约45-55%的病例是由CREBBP基因的缺失或突变引起,而病例的未知部分是由EP300中的基因变化引起的。第一例是3岁女性,外显子缺失EP300基因,具有RSTS的典型面部特征,没有拇指和脚趾异常,与其他带有EP300的RSTS病例中描述的较轻的骨骼表型一致突变。另外,该患者的母亲在怀孕期间也有先兆子痫,这很少报道。第二例是具有RSTS经典特征的新生男性。我们的研究结果表明,以外显子为靶点的阵列比较基因组杂交(aCGH)是检测临床上重要的基因内重排的有力工具,否则,如果缺少足够的外显子覆盖或感兴趣基因的测序,aCGH平台可能会错过这些重排。

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