University of Wisconsin-Madison, Madison, WI 53705, USA.
Eur J Hum Genet. 2013 Apr;21(4):455-9. doi: 10.1038/ejhg.2012.165. Epub 2012 Aug 22.
We report clinical findings that extend the phenotype of the ~550 kb 16p11.2 microdeletion syndrome to include a rare, severe, and persistent pediatric speech sound disorder termed Childhood Apraxia of Speech (CAS). CAS is the speech disorder identified in a multigenerational pedigree ('KE') in which half of the members have a mutation in FOXP2 that co-segregates with CAS, oromotor apraxia, and low scores on a nonword repetition task. Each of the two patients in the current report completed a 2-h assessment protocol that provided information on their cognitive, language, speech, oral mechanism, motor, and developmental histories and performance. Their histories and standard scores on perceptual and acoustic speech tasks met clinical and research criteria for CAS. Array comparative genomic hybridization analyses identified deletions at chromosome 16p11.2 in each patient. These are the first reported cases with well-characterized CAS in the 16p11.2 syndrome literature and the first report of this microdeletion in CAS genetics research. We discuss implications of findings for issues in both literatures.
我们报告了一些临床发现,这些发现扩展了~550 kb 16p11.2 微缺失综合征的表型,包括一种罕见的、严重的、持续性的儿童言语障碍,称为儿童言语运动障碍(CAS)。CAS 是在一个多代系谱(“KE”)中发现的言语障碍,其中一半的成员有 FOXP2 突变,该突变与 CAS、口运动性构音障碍和非词重复任务的低分共分离。本报告中的两位患者均完成了 2 小时评估方案,该方案提供了他们的认知、语言、言语、口腔机制、运动和发育史以及表现的信息。他们的病史和感知和声学言语任务的标准分数符合 CAS 的临床和研究标准。阵列比较基因组杂交分析在每位患者中均发现 16p11.2 染色体缺失。这些是在 16p11.2 综合征文献中首次报道的具有明确特征的 CAS 病例,也是在 CAS 遗传学研究中首次报道该微缺失病例。我们讨论了这些发现对两个文献中的问题的影响。
