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TRAPPC9基因中的纯合剪接位点突变导致智力障碍和小头畸形。

A homozygous splice site mutation in TRAPPC9 causes intellectual disability and microcephaly.

作者信息

Kakar Naseebullah, Goebel Ingrid, Daud Shakeela, Nürnberg Gudrun, Agha Noor, Ahmad Adeel, Nürnberg Peter, Kubisch Christian, Ahmad Jamil, Borck Guntram

机构信息

Department of Biotechnology and Informatics, BUITEMS, Quetta, Pakistan.

出版信息

Eur J Med Genet. 2012 Dec;55(12):727-31. doi: 10.1016/j.ejmg.2012.08.010. Epub 2012 Aug 30.

DOI:10.1016/j.ejmg.2012.08.010
PMID:22989526
Abstract

Autosomal recessive intellectual disability is believed to be particularly prevalent in highly consanguineous populations and genetic isolates and may account for a quarter of all non-syndromic cases. Mutations in more than 50 genes have been reported to be involved in autosomal recessive intellectual disability, including TRAPPC9 (MIM 611966), mutations of which have been identified in six families from different geographical origins. We performed a clinical and molecular genetic study of a consanguineous Pakistani family segregating intellectual disability and microcephaly. SNP-array-based homozygosity mapping revealed suggestive linkage to four genomic regions including one on chromosome 8 that contained TRAPPC9. We detected a homozygous TRAPPC9 splice donor site mutation (c.1024+1G>T) that cosegregated with intellectual disability in the family and led to skipping of exon 3 and exons 3 and 4 in blood-derived patient RNA. We have thus identified a novel splice site mutation leading to exon skipping and premature termination of TRAPPC9 translation. These data further suggest that TRAPPC9 mutations -unlike mutations in the vast majority of the known intellectual disability-associated genes- constitute a more frequent cause of autosomal-recessive cognitive deficits, especially when microcephaly is also present.

摘要

常染色体隐性智力障碍在高度近亲通婚人群和遗传隔离群体中尤为普遍,可能占所有非综合征病例的四分之一。据报道,50多个基因的突变与常染色体隐性智力障碍有关,包括TRAPPC9(MIM 611966),在来自不同地理区域的6个家族中已鉴定出该基因的突变。我们对一个患有智力障碍和小头畸形的巴基斯坦近亲家族进行了临床和分子遗传学研究。基于单核苷酸多态性阵列(SNP-array)的纯合性定位显示与四个基因组区域存在提示性连锁,其中一个位于8号染色体上,包含TRAPPC9。我们检测到一个纯合的TRAPPC9剪接供体位点突变(c.1024+1G>T),该突变与家族中的智力障碍共分离,并导致患者血液来源的RNA中第3外显子以及第3和第4外显子缺失。我们因此鉴定出一种导致外显子跳跃和TRAPPC9翻译提前终止的新型剪接位点突变。这些数据进一步表明,与绝大多数已知的与智力障碍相关的基因突变不同,TRAPPC9突变是常染色体隐性认知缺陷更常见的原因,尤其是在同时存在小头畸形的情况下。

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