Division of Developmental Medicine, Boston Children's Hospital, Harvard Medical School, Boston, Massachusetts, USA.
Division of Genetics and Genomics, Boston Children's Hospital, Harvard Medical School, Boston, Massachusetts, USA.
Am J Med Genet A. 2021 Aug;185(8):2384-2390. doi: 10.1002/ajmg.a.62254. Epub 2021 May 18.
TCF7L2 encodes transcription factor 7-like 2 (OMIM 602228), a key mediator of the evolutionary conserved canonical Wnt signaling pathway. Although several large-scale sequencing studies have implicated TCF7L2 in intellectual disability and autism, both the genetic mechanism and clinical phenotype have remained incompletely characterized. We present here a comprehensive genetic and phenotypic description of 11 individuals who have been identified to carry de novo variants in TCF7L2, both truncating and missense. Missense variation is clustered in or near a high mobility group box domain, involving this region in these variants' pathogenicity. All affected individuals present with developmental delays in childhood, but most ultimately achieved normal intelligence or had only mild intellectual disability. Myopia was present in approximately half of the individuals, and some individuals also possessed dysmorphic craniofacial features, orthopedic abnormalities, or neuropsychiatric comorbidities including autism and attention-deficit/hyperactivity disorder (ADHD). We thus present an initial clinical and genotypic spectrum associated with variation in TCF7L2, which will be important in informing both medical management and future research.
TCF7L2 编码转录因子 7 样 2(OMIM 602228),是进化保守的经典 Wnt 信号通路的关键介质。尽管几项大规模的测序研究表明 TCF7L2 与智力障碍和自闭症有关,但遗传机制和临床表型仍未完全阐明。我们在此介绍了 11 名个体的综合遗传和表型描述,这些个体被鉴定为携带 TCF7L2 的新生变异,包括截断和错义变异。错义变异聚集在或靠近高迁移率族盒结构域,使该区域成为这些变体致病性的一部分。所有受影响的个体在儿童时期都表现出发育迟缓,但大多数最终达到了正常智力,或只有轻度智力障碍。约一半的个体存在近视,一些个体还存在颅面畸形特征、骨畸形异常或神经精神共病,包括自闭症和注意缺陷/多动障碍(ADHD)。因此,我们提出了与 TCF7L2 变异相关的初始临床和基因型谱,这对于告知医疗管理和未来的研究都非常重要。
