Akbariazar Elinaz, Ebrahimpour Mohammad, Akbari Saeedeh, Arzhanghi Sanaz, Abedini Seydeh Sedigheh, Najmabadi Hossein, Kahrizi Kimia
Msc of human genetics, University of Social Welfare & Rehabilitation Sciences, Tehran, Iran.
Bsc in Nursing, Genetics Research Center, University of Social Welfare & Rehabilitation Sciences, Tehran, Iran.
Iran J Child Neurol. 2013 Spring;7(2):23-30.
Autosomal recessive primary microcephaly (MCPH) is a neurodevelopmental and genetically heterogeneous disorder with decreased head circumference due to the abnormality in fetal brain growth. To date, nine loci and nine genes responsible for the situation have been identified. Mutations in the ASPM gene (MCPH5) is the most common cause of MCPH. The ASPM gene with 28 exons is essential for normal mitotic spindle function in embryonic neuroblasts.
MATERIALS & METHODS: We have ascertained twenty-two consanguineous families with intellectual disability and different ethnic backgrounds from Iran. Ten out of twenty-two families showed primary microcephaly in clinical examination. We investigated MCPH5 locus using homozygosity mapping by microsatellite marker.
Sequence analysis of exon 8 revealed a deletion of nucleotide (T) in donor site of splicing site of ASPM in one family. The remaining nine families were not linked to any of the known loci .More investigation will be needed to detect the causative defect in these families.
[corrected] We detected a novel mutation in the donor splicing site of exon 8 of the ASPM gene. This deletion mutation can alter the ASPM transcript leading to functional impairment of the gene product.
常染色体隐性原发性小头畸形(MCPH)是一种神经发育性且基因异质性疾病,因胎儿脑生长异常导致头围减小。迄今为止,已确定了9个与该病相关的基因座和9个基因。ASPM基因(MCPH5)突变是MCPH最常见的病因。含有28个外显子的ASPM基因对胚胎成神经细胞中正常有丝分裂纺锤体功能至关重要。
我们确定了来自伊朗的22个有智力障碍且具有不同种族背景的近亲家庭。22个家庭中有10个在临床检查中表现出原发性小头畸形。我们通过微卫星标记采用纯合性定位法研究了MCPH5基因座。
外显子8的序列分析显示,在一个家庭中,ASPM剪接位点供体部位的核苷酸(T)缺失。其余9个家庭与任何已知基因座均无连锁关系。需要进行更多研究以检测这些家庭中的致病缺陷。
我们在ASPM基因外显子8的供体剪接位点检测到一个新突变。这种缺失突变可改变ASPM转录本,导致基因产物功能受损。
