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Characterization of Variegate Porphyria Mutations Using a Minigene Approach

机译:使用小基因方法表征斑叶紫菜突变

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摘要

Porphyrias are a group of metabolic diseases that affect the skin and/or nervous system. In 2008, three unrelated patients were diagnosed with variegate porphyria at the CIPYP (Centro de Investigaciones sobre Porfirinas y Porfirias). Sequencing of the protoporphyrinogen oxidase gene, the gene altered in this type of porphyria, revealed three previously undescribed mutations: c.338+3insT, c.807G>A, and c.808-1G>C. As these mutations do not affect the protein sequence, we hypothesized that they might be splicing mutations. RT-PCRs performed on the patient’s mRNAs showed normal mRNA or no amplification at all. This result indicated that the aberrant spliced transcript is possibly being degraded. In order to establish whether they were responsible or not for the patient’s disease by causing aberrant splicing, we utilized a minigene approach. We found that the three mutations lead to exon skipping; therefore, the abnormal mRNAs are most likely degraded by a mechanism such as nonsense-mediated decay. In conclusion, these mutations are responsible for the disease because they alter the normal splicing pathway, thus providing a functional explanation for the appearance of disease and highlighting the use of minigene assays to complement transcript analysis.
机译:卟啉症是一组影响皮肤和/或神经系统的代谢性疾病。 2008年,在CIPYP(Centro de Investigaciones sobre Porfirinas y Porfirias),三名不相关的患者被诊断为杂色卟啉症。原卟啉原氧化酶基因的序列(在这种类型的卟啉症中发生了改变)揭示了三个以前未描述的突变:c.338 + 3insT,c.807G> A和c.808-1G> C。由于这些突变不影响蛋白质序列,因此我们假设它们可能是剪接突变。对患者的mRNA进行的RT-PCR显示mRNA正常或完全没有扩增。该结果表明异常的剪接转录本可能被降解。为了确定它们是否通过引起异常剪接而对患者的疾病负责,我们采用了一种小基因方法。我们发现这三个突变导致外显子跳跃。因此,异常mRNA最有可能通过无意义介导的衰变等机制降解。总之,这些突变是造成疾病的原因,因为它们改变了正常的剪接途径,从而为疾病的出现提供了功能上的解释,并着重指出了使用小基因检测技术来补充转录本分析。

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