Institute of Genetic Medicine, Newcastle upon Tyne, England.
Medical Genetics Department, Rare Diseases and Personalized Medicine, Montpellier University Hospital, Montpellier, France.
Eur J Hum Genet. 2019 Nov;27(11):1677-1682. doi: 10.1038/s41431-019-0413-6. Epub 2019 Jun 14.
As a result of exome-based sequencing work performed by the DDD study, de novo variants in CNOT3 have emerged as a newly recognised cause of a developmental disorder. This paper describes molecular and clinical details of 16 probands with developmental disorders and de novo CNOT3 variants. It is the first such description of the developmental phenotype associated with CNOT3 variants. Eight of these cases were discovered as part of the DDD study, while the other eight were found as a result of large-scale sequencing work performed by other groups. A highly specific phenotype was not recognised in these 16 cases. The most consistent phenotypic features seen in subjects with de novo variants in CNOT3 were hypotonia, relatively small stature, developmental delay, behavioural problems and intellectual disability. There is no easily recognisable facial phenotype, but some common dysmorphic features such as anteverted nares, thin upper lip and low set eyebrows were shared among some of the probands. Haploinsufficiency appears to be the most likely mechanism of action, with eight cases found to have protein-truncating variants. Of the other eight cases (all missense variants), three share an amino acid substitution at the same position which may therefore represent an important functional domain.
由于 DDD 研究进行的外显子组测序工作,CNOT3 中的新生变异已成为一种新的发育障碍病因。本文描述了 16 名患有发育障碍和新生 CNOT3 变异的患者的分子和临床详细信息。这是首次对与 CNOT3 变异相关的发育表型进行描述。其中 8 例是作为 DDD 研究的一部分发现的,而另外 8 例是其他小组进行大规模测序工作的结果。在这 16 例中,没有识别出高度特异性的表型。在 CNOT3 新生变异的受试者中,最一致的表型特征是低张力、相对矮小的身材、发育迟缓、行为问题和智力障碍。没有易于识别的面部表型,但一些常见的畸形特征,如前鼻孔外翻、薄上唇和低眉,在一些先证者中是共有的。杂合功能缺失似乎是最可能的作用机制,其中 8 例发现有蛋白截断变异。在其他 8 例(均为错义变异)中,有 3 例共享相同位置的氨基酸取代,因此可能代表一个重要的功能域。
