Schiff Manuel, Delahaye Andrée, Andrieux Joris, Sanlaville Damien, Vincent-Delorme Catherine, Aboura Azzedine, Benzacken Brigitte, Bouquillon Sonia, Elmaleh-Berges Monique, Labalme Audrey, Passemard Sandrine, Perrin Laurence, Manouvrier-Hanu Sylvie, Edery Patrick, Verloes Alain, Drunat Séverine
Department of Pediatric Neurology & Metabolic Diseases, APHP-Robert DEBRE University Hospital, Paris, France.
Eur J Med Genet. 2010 Sep-Oct;53(5):303-8. doi: 10.1016/j.ejmg.2010.06.009. Epub 2010 Jul 3.
The 17p13.3 deletion syndrome (or Miller-Dieker syndrome, MDS, MIM 247200) is characterized by lissencephaly, mental retardation and facial dysmorphism. The phenotype is attributed to haploinsufficiency of two genes present in the minimal critical region of MDS: PAFAH1B1 (formerly referred to as LIS1) and YWHAE. Whereas isolated PAFAH1B1 deletion causes lissencephaly, YWHAE is a candidate for the dysmorphic phenotype associated with MDS.
We describe clinical, neuroradiological and molecular data in four patients with a 17p13.3 deletion distal to PAFAH1B1 involving YWHAE.
All patients presented with mild or moderate developmental delay and pre and/or post-natal growth retardation. Patients A, B and C had neuro-imaging anomalies: leucoencephalopathy with macrocephaly (patients A and C), Chiari type 1 malformation (patient A) and paraventricular cysts (patient C). Patient B had patent ductus arteriosus and pulmonary arterial hypertension. Patient C had unilateral club foot. Patient D had enlarged Virchow Robin spaces, microcornea, and chorioretinal and lens coloboma. Array-CGH revealed de novo terminal 17p13.3 deletions for patient A and B, and showed interstitial 17p13.3 deletions of 1.4 Mb for patient C and of 0.5 Mb for patient D. In all patients, PAFAH1B1 was not deleted.
Our patients confirm that 17p deletion distal to PAFAH1B1 have a distinctive phenotype : mild mental retardation, moderate to severe growth restriction, white matter abnormalities and developmental defects including Chiari type 1 malformation and coloboma. Our patients contribute to the delineation and clinical characterization of 17p13.3 deletion distal to PAFAH1B1 and highlight the role of the region containing YWHAE in brain and eye development and in somatic growth.
17p13.3缺失综合征(或米勒-迪克尔综合征,MDS,MIM 247200)的特征为无脑回畸形、智力发育迟缓及面部畸形。该表型归因于MDS最小关键区域存在的两个基因单倍剂量不足:PAFAH1B1(以前称为LIS1)和YWHAE。虽然单独的PAFAH1B1缺失会导致无脑回畸形,但YWHAE是与MDS相关的畸形表型的候选基因。
我们描述了4例PAFAH1B1远端17p13.3缺失且涉及YWHAE的患者的临床、神经放射学和分子数据。
所有患者均表现为轻度或中度发育迟缓以及产前和/或产后生长发育迟缓。患者A、B和C有神经影像学异常:伴有巨头畸形的白质脑病(患者A和C)、Chiari 1型畸形(患者A)和脑室旁囊肿(患者C)。患者B有动脉导管未闭和肺动脉高压。患者C有单侧马蹄内翻足。患者D有扩大的Virchow Robin间隙、小角膜以及脉络膜视网膜和晶状体缺损。阵列比较基因组杂交(Array-CGH)显示患者A和B为新发的17p13.3末端缺失,患者C为1.4 Mb的17p13.3间质缺失,患者D为0.5 Mb的17p13.3间质缺失。所有患者的PAFAH1B1均未缺失。
我们的患者证实PAFAH1B1远端17p缺失具有独特的表型:轻度智力发育迟缓、中度至重度生长受限、白质异常以及包括Chiari 1型畸形和缺损在内的发育缺陷。我们的患者有助于明确PAFAH1B1远端17p13.3缺失的特征及临床特点,并突出了包含YWHAE的区域在脑和眼发育以及躯体生长中的作用。
