Nature and mRNA effect of 282 different NF1 point mutations: focus on splicing alterations

移码突变 生物 遗传学 点突变 RNA剪接 基因 突变 编码区 单链构象多态性 无声突变 核糖核酸 分子生物学 错义突变
作者
Eva Pros,Carolina de la Torre,Thamar Martín,Pere Fábregas,Eduard Serra,Conxi Lázaro
出处
期刊:Human Mutation [Wiley]
卷期号:29 (9): E173-E193 被引量:119
标识
DOI:10.1002/humu.20826
摘要

Neurofibromatosis type 1 (NF1) is a common autosomal dominant genetic disorder caused by mutations in the NF1 gene. In this paper we report our experience using the cDNA-SSCP/HD analysis as a mutational screening approach and the double characterization of all mutations at the DNA and RNA levels. Two hundred and eighty-two different mutations (in 374 independent patients) were identified, 140 of which were novel in our population. Most of these mutations are unique and distributed along the gene. However, we also detected 37 recurrent mutations. Our approach is limited with respect to the detection of single base substitutions, but it is highly effective in the detection of frameshift mutations and mutations that affect the correct splicing. Due to this bias we focus here in the characterization of these two types of mutations. Forty-seven percent of mutations found were frameshift mutations, with small deletions being 2.3 times more common than small insertions. At the mRNA level, 44% of mutations affected the correct splicing, 80% of them located in the consensus sequences, with the donor site being much more frequently involved. The remaining 20% consisted of mutations located in deep intronic sites and mutations located in the coding region. In general the latter group produces different types of mutated transcripts with specific proportions for each mutation. The double characterization of mutations at the DNA and RNA levels enables to detect a broader spectrum of mutations than any single level approach, and provides a greater understanding of their molecular pathogenesis.
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