Department of Genetics, Biology and Biochemistry, University of Torino, via Santena, 19-10126 Torino, Italy.
Neurogenetics. 2012 Aug;13(3):205-14. doi: 10.1007/s10048-012-0331-z. Epub 2012 May 3.
Megalencephalic leukoencephalopathy with subcortical cysts is an autosomal recessive disease characterized by early onset macrocephaly; developmental delay; motor disability in the form of progressive spasticity and ataxia; seizures; cognitive decline; and characteristic magnetic resonance imaging findings. Mutations in two genes, MLC1 (22q13.33; 75 % of patients) or HEPACAM (11q24; 20 % of patients), are associated with the disease. We describe an adult MLC patient with moderate clinical symptoms. MLC1 cDNA analysis from lymphoblasts showed a strong transcript reduction and identified a 246-bp pseudoexon containing a premature stop codon between exons 10 and 11, due to a homozygous c.895-226 T>G deep-intronic mutation. This category of mutations is often overlooked, being outside of canonically sequenced genomic regions. The mutation c.895-226 T>G has a leaky effect on splicing leaving part of the full-length transcript. Its role on splicing was confirmed using a minigene assay and an antisense morpholinated oligonucleotide targeted to the aberrant splice site in vitro, which partially abrogated the mutation effect.
巨脑白质脑病伴脑下囊肿是一种常染色体隐性疾病,其特征为早发性大头畸形;发育迟缓;以进行性痉挛和共济失调为形式的运动障碍;癫痫发作;认知能力下降;以及具有特征性的磁共振成像发现。两种基因(MLC1[22q13.33;75%的患者]或 HEPACAM[11q24;20%的患者])的突变与该疾病有关。我们描述了一位具有中度临床症状的成年 MLC 患者。从淋巴细胞中分析 MLC1 cDNA 显示强烈的转录减少,并确定了一个 246-bp 的假外显子,其中包含一个位于外显子 10 和 11 之间的提前终止密码子,这是由于纯合子 c.895-226 T>G 深内含子突变引起的。这种突变类别经常被忽视,因为它们不在常规测序的基因组区域内。突变 c.895-226 T>G 对剪接具有渗漏效应,导致全长转录本的一部分保留下来。使用小基因检测和针对体外异常剪接位点的反义修饰寡核苷酸在体外证实了其对剪接的作用,该反义修饰寡核苷酸部分消除了突变的影响。
