Two novel truncating variants of the ASPM gene identified in a nonconsanguineous Chinese family associated with primary microcephaly

先证者 医学 移码突变 胡说 血缘关系 遗传学 小头畸形 全球发育迟缓 无义突变 复合杂合度 基因 突变 外显子组测序 智力残疾 桑格测序 儿科 神经发育障碍 基因检测 错义突变 神经管 生物信息学 遗传咨询 病理 入射(几何) 家族史
作者
Shuqin Xu,Wenqian Zhang,Rui Zhou,Hui Huang,Wei Chen,Wenhao Xiang,Limei Liu,Jieping Song
出处
期刊:Clinical Dysmorphology [Lippincott Williams & Wilkins]
卷期号:31 (1): 1-5 被引量:4
标识
DOI:10.1097/mcd.0000000000000395
摘要

Primary autosomal recessive microcephaly 5 (MCPH5) is a rare neurodevelopmental disorder with a relatively high incidence in regions where consanguineous marriage is widely practiced; So far, only a few MCPH5 cases have been reported from China. Here, we report clinical and molecular characteristics of two Chinese MCPH5 patients, a 24-year-old woman proband and her brother, a 19-year-old man, from a nonconsanguineous family. Main manifestations in the proband were small head circumference, premature closure of fontanelles, impaired concentration and moderate intellectual disability. The proband's brother had similar symptoms, but he was hyperactive and had a more severe sloping forehead. Brain imaging revealed global reduction in brain size, especially in the frontal lobes bilaterally and anterior horns of lateral ventricles. Sequencing results revealed that both patients carried a novel nonsense variant p.Tyr2004* (c.6012_6013delTA) and a novel frameshift variant p.Arg2005Serfs*48 (c.6015_6016delGG) in the ASPM gene. These variants were interpreted to be pathogenic in the in-silico analysis. Our findings help to expand the mutation spectrum of ASPM and provide new opportunities for assisting the traditional clinical diagnosis on the cases with atypical characteristics.
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