Dentici Maria Lisa, Niceta Marcello, Pantaleoni Francesca, Barresi Sabina, Bencivenga Paola, Dallapiccola Bruno, Digilio Maria Cristina, Tartaglia Marco
Genetics and Rare Diseases Research Division, Ospedale Pediatrico Bambino Gesù, IRCCS, Rome, Italy.
Am J Med Genet A. 2017 Jul;173(7):1965-1969. doi: 10.1002/ajmg.a.38255. Epub 2017 May 7.
Exome sequencing has led to the comprehension of the molecular bases of several forms of neurodevelopmental disorders, a clinically heterogeneous group of diseases characterized by intellectual disability (ID) and autism spectrum disorder (ASD). De novo mutations in POGZ has been causally linked to isolated ASD and syndromic ID, only recently. Here we report on a 15 year-old girl in whom exome sequencing allowed to identify a de novo POGZ truncating mutation as the molecular cause underlying a complex phenotype apparently not fitting any recognized syndrome. We describe the evolution of her clinical features with age, and review published clinical data of patients with POGZ mutations to systematically analyze the clinical spectrum associated with mutations. Our finding expands the clinical and molecular spectrum of POGZ mutations. Revision of the literature indicate that moderate to severe ID, microcephaly, variable CNS malformations, reduced growth, brachytelephalangy, and facial dysmorphism represent recurrent features associated with POGZ mutations.
外显子组测序有助于理解多种形式的神经发育障碍的分子基础,这是一组临床异质性疾病,其特征为智力残疾(ID)和自闭症谱系障碍(ASD)。直到最近,POGZ基因的新生突变才被因果性地与孤立性ASD和综合征性ID联系起来。在此,我们报告一名15岁女孩,通过外显子组测序发现了一个新生的POGZ截断突变,该突变是一种明显不符合任何已确认综合征的复杂表型的分子病因。我们描述了她临床特征随年龄的演变,并回顾已发表的POGZ突变患者的临床数据,以系统分析与突变相关的临床谱。我们的发现扩展了POGZ突变的临床和分子谱。文献综述表明,中度至重度ID、小头畸形、可变的中枢神经系统畸形、生长发育迟缓、短指畸形和面部畸形是与POGZ突变相关的反复出现的特征。
