Division of Neurology/Molecular Brain Science, Kobe University Graduate School of Medicine, Kobe 650-0017, Japan.
Nature. 2011 Oct 5;478(7367):127-31. doi: 10.1038/nature10456.
Fukuyama muscular dystrophy (FCMD; MIM253800), one of the most common autosomal recessive disorders in Japan, was the first human disease found to result from ancestral insertion of a SINE-VNTR-Alu (SVA) retrotransposon into a causative gene. In FCMD, the SVA insertion occurs in the 3' untranslated region (UTR) of the fukutin gene. The pathogenic mechanism for FCMD is unknown, and no effective clinical treatments exist. Here we show that aberrant messenger RNA (mRNA) splicing, induced by SVA exon-trapping, underlies the molecular pathogenesis of FCMD. Quantitative mRNA analysis pinpointed a region that was missing from transcripts in patients with FCMD. This region spans part of the 3' end of the fukutin coding region, a proximal part of the 3' UTR and the SVA insertion. Correspondingly, fukutin mRNA transcripts in patients with FCMD and SVA knock-in model mice were shorter than the expected length. Sequence analysis revealed an abnormal splicing event, provoked by a strong acceptor site in SVA and a rare alternative donor site in fukutin exon 10. The resulting product truncates the fukutin carboxy (C) terminus and adds 129 amino acids encoded by the SVA. Introduction of antisense oligonucleotides (AONs) targeting the splice acceptor, the predicted exonic splicing enhancer and the intronic splicing enhancer prevented pathogenic exon-trapping by SVA in cells of patients with FCMD and model mice, rescuing normal fukutin mRNA expression and protein production. AON treatment also restored fukutin functions, including O-glycosylation of α-dystroglycan (α-DG) and laminin binding by α-DG. Moreover, we observe exon-trapping in other SVA insertions associated with disease (hypercholesterolemia, neutral lipid storage disease) and human-specific SVA insertion in a novel gene. Thus, although splicing into SVA is known, we have discovered in human disease a role for SVA-mediated exon-trapping and demonstrated the promise of splicing modulation therapy as the first radical clinical treatment for FCMD and other SVA-mediated diseases.
福山肌营养不良症(FCMD;MIM253800)是日本最常见的常染色体隐性遗传病之一,是首例发现的由祖先插入 SINE-VNTR-Alu(SVA)反转录转座子到致病基因而导致的人类疾病。在 FCMD 中,SVA 插入发生在 fukutin 基因的 3'非翻译区(UTR)。FCMD 的发病机制尚不清楚,也没有有效的临床治疗方法。在这里,我们表明,由 SVA 外显子捕获引起的异常信使 RNA(mRNA)剪接是 FCMD 的分子发病机制。定量 mRNA 分析确定了缺失 FCMD 患者转录本的区域。该区域跨越 fukutin 编码区 3'端的一部分、3'UTR 的近端部分和 SVA 插入。相应地,FCMD 患者和 SVA 敲入模型小鼠的 fukutin mRNA 转录本短于预期长度。序列分析显示,由 SVA 中的强受体位点和 fukutin 外显子 10 中的罕见替代供体位点引发的异常剪接事件。产生的产物截断了 fukutin 羧基(C)末端并添加了 129 个由 SVA 编码的氨基酸。针对剪接受体位点、预测的外显子剪接增强子和内含子剪接增强子的反义寡核苷酸(AON)的引入,防止了 FCMD 患者和模型小鼠细胞中 SVA 的致病外显子捕获,挽救了正常的 fukutin mRNA 表达和蛋白产生。AON 治疗还恢复了 fukutin 的功能,包括 α- 二聚糖(α-DG)的 O-糖基化和 α-DG 对层粘连蛋白的结合。此外,我们观察到与疾病相关的其他 SVA 插入(高胆固醇血症、中性脂质贮积病)和人类特异性 SVA 插入到一个新基因中的外显子捕获。因此,尽管已知 SVA 插入,但我们在人类疾病中发现了 SVA 介导的外显子捕获的作用,并证明了剪接调节治疗作为 FCMD 和其他 SVA 介导的疾病的第一个激进临床治疗方法的前景。
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