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首页> 外文期刊>BMC Medical Genetics >Severe congenital microcephaly with 16p13.11 microdeletion combined with NDE1 mutation, a case report and literature review
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Severe congenital microcephaly with 16p13.11 microdeletion combined with NDE1 mutation, a case report and literature review

机译:严重的先天性微术,16P13.11微缺蛋糕联合NDE1突变,案例报告和文献综述

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摘要

Microcephaly is a disorder characterized by severe impairment in brain development, reduced brain and head size. Congenital severe microcephaly is very rare, and NDE1 deletion and genetic mutations are important contributors. Single nucleotide polymorphism (SNP) chromosomal microarray analysis (CMA) and muation screening of NDE1 gene were performed in an 8-month patient with severe congenital microcephaly, and/or his parents. Genetic studies found a 16p13.11 deletion containing NDE1 gene, and a novel NDE1 mutation c.555_556GC?>?CT on the non-deleted homolog, inherited from his phenotypically normal parents, respectively. The 2?bp nucleotide change results in a missense mutation p.K185?N and a nonsense mutation p.Q186X. We also conducted literaturte review to compare the clinical phenotypes of our patient to those of cases previously reported with NDE1 mutations, and found all patients had mental retardation, severe microcephaly, and corpus callosum agenesis. This is the first Chinese reported with microcephaly caused by NDE1 mutations. NDE1 is a critical pathogenetic gene in severe congenital microcephaly. Sequencing NDE1 and CMA in patients with severe congenital microcephaly may be warranted.
机译:微头是一种疾病,其特征在于大脑发育严重损伤,脑和头部大小降低。先天性严重的微症是非常罕见的,NDE1缺失和基因突变是重要的贡献者。单核苷酸多态性(SNP)染色体微阵列分析(CMA)和NDE1基因的牛筛选在8个月的患者中进行严重的先天性微微术,和/或他的父母进行。遗传学研究发现含有NDE1基因的16p13.11缺失,并且新的NDE1突变C.555_556GC?>ΔCT在非缺失的同源物上,分别从他的表型正常父母遗传。 2?BP核苷酸变化导致致畸突变P.k185?n和非阵容突变p.q186x。我们还进行了文学审查,以将患者的临床表型与先前用NDE1突变报告的案件进行比较,发现所有患者患有精神病迟缓,严重的微症和胼callosum患者。这是第一个用NDE1突变引起的微微畸形报道的中国人。 NDE1是严重先天性微术中的批判性致病基因。可以保证测序NDE1和严重先天性微头患者的NDE1和CMA。

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