Bloch Mercedes, Leonard Anissa, Diplas Andreas A, Pepermans Xavier, Emanuel Beverly S, Santa Rocca Maria, Revencu Nicole, Sznajer Yves
Center for Human Genetics, Cliniques Universitaires St. Luc, Université Catholique de Louvain, Brussels, Belgium.
Am J Med Genet A. 2014 Jul;164A(7):1789-94. doi: 10.1002/ajmg.a.36516. Epub 2014 Apr 3.
Interstitial deletions of the distal part of chromosome 2p seem to be rarely identified or reported: to date, only nine distinct patients have been published. The last three patients were diagnosed with the use of more recent molecular karyotyping technology (SNP array). We report on the natural history of an 8-year-old boy with dysmorphic features, postnatal overgrowth, microcephaly, generalized hypotonia, and global developmental delay. The diagnosis was accomplished by SNP array investigation that led to the identification of a de novo 7.4 Mb deletion of 2p23.2-p24.1. The present patient also developed a nonsyndromic auditory neuropathy. Since the deletion encompassed the OTOF gene, this haploinsufficiency suggests second allele sequencing as a possible cause (DFNB9). We describe the phenotype of the patient and review reports in patients with del 2p23 subsequent to the advent of the genomic era. At the time of identification of "new" micro- deletion and -duplication syndromes, the present report adds to the description of phenotype in patients with del(2)p(23.2;24.1) and the 2p23.2 region in particular.
2号染色体短臂远端的间质性缺失似乎很少被发现或报道:迄今为止,仅发表了9例不同的患者。最近的3例患者是通过使用更新的分子核型分析技术(SNP阵列)诊断出来的。我们报告了一名8岁男孩的自然病史,该男孩具有畸形特征、出生后过度生长、小头畸形、全身肌张力减退和全面发育迟缓。通过SNP阵列检测完成诊断,该检测发现了一个新的2p23.2-p24.1区域7.4 Mb的缺失。该患者还出现了非综合征性听觉神经病。由于该缺失包含OTOF基因,这种单倍剂量不足提示二等位基因测序可能是病因(DFNB9)。我们描述了该患者的表型,并回顾了基因组时代以来2p23缺失患者的报告。在发现“新的”微缺失和微重复综合征时,本报告补充了del(2)p(23.2;24.1)患者特别是2p23.2区域患者的表型描述。
