| Literature DB >> 24871807 |
Ery Kus Dwianingsih1, Rusdy Ghazali Malueka2, Atsushi Nishida2, Kyoko Itoh3, Tomoko Lee1, Mariko Yagi1, Kazumoto Iijima1, Yasuhiro Takeshima1, Masafumi Matsuo2.
Abstract
Duchenne muscular dystrophy (DMD), a progressive muscle-wasting disease, is mostly caused by exon deletion mutations in the DMD gene. The reading frame rule explains that out-of-frame deletions lead to muscle dystrophin deficiency in DMD. In outliers to this rule, deletion junction sequences have never previously been explored as splicing modulators. In a Japanese case, we identified a single exon 45 deletion in the patient's DMD gene, indicating out-of-frame mutation. However, immunohistochemical examination disclosed weak dystrophin signals in his muscle. Reverse transcription-PCR amplification of DMD exons 42 to 47 revealed a major normally spliced product with exon 45 deletion and an additional in-frame product with deletion of both exons 44 and 45, indicating upstream exon 44 skipping. We considered the latter to underlie the observed dystrophin expression. Remarkably, the junction sequence cloned by PCR walking abolished the splicing enhancer activity of the upstream intron in a chimeric doublesex gene pre-mRNA in vitro splicing. Furthermore, antisense oligonucleotides directed against the junction site counteracted this effect. These indicated that the junction sequence was a splicing silencer that induced upstream exon 44 skipping. It was strongly suggested that creation of splicing regulator is a modifier of dystrophinopathy.Entities:
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Year: 2014 PMID: 24871807 DOI: 10.1038/jhg.2014.36
Source DB: PubMed Journal: J Hum Genet ISSN: 1434-5161 Impact factor: 3.172