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首页> 外文期刊>Neuromuscular disorders: NMD >Polymorphism in the TOMM40 gene modifies the risk of developing sporadic inclusion body myositis and the age of onset of symptoms
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Polymorphism in the TOMM40 gene modifies the risk of developing sporadic inclusion body myositis and the age of onset of symptoms

机译:TOMM40基因的多态性改变了发生偶发性包涵体肌炎的风险和症状发作的年龄

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摘要

A polyT repeat in an intronic polymorphism (rs10524523) in the TOMM40 gene, which encodes an outer mitochondrial membrane translocase involved in the transport of amyloid-β and other proteins into mitochondria, has been implicated in Alzheimer's disease and APOE-TOMM40 genotypes have been shown to modify disease risk and age at onset of symptoms. Because of the similarities between Alzheimer's disease and sporadic inclusion body myositis (s-IBM), and the importance of amyloid-β and mitochondrial changes in s-IBM, we investigated whether variation in poly-T repeat lengths in rs10524523 also influence susceptibility and age at onset in a cohort of 90 Caucasian s-IBM patients (55 males; age 69.1. ±. 9.6). In carriers of APOE ε3/. ε3 or ε3. /ε4, genotypes with a very long (VL) poly-T repeat were under-represented in s-IBM compared to controls and were associated with a later age at symptom onset, suggesting that these genotypes may be protective. Our study is the first to suggest that polymorphisms in genes controlling mitochondrial function can influence susceptibility to s-IBM and have disease modifying effects. However, further studies in other s-IBM populations are needed to confirm these findings, as well as expression studies of different TOMM40 alleles in muscle tissue.
机译:TOMM40基因内含子多态性(rs10524523)中的polyT重复序列编码阿尔茨海默氏病,并且编码APOE-TOMM40基因型与编码淀粉样β和其他蛋白质进入线粒体的线粒体外膜转座酶有关。改变症状发作时的疾病风险和年龄。由于阿尔茨海默氏病和偶发性包涵体肌炎(s-IBM)之间的相似性,以及s-IBM中淀粉样β和线粒体变化的重要性,我们调查了rs10524523中poly-T重复长度的变化是否也影响了易感性和年龄在90名高加索s-IBM患者队列中发病(男性55例;年龄69.1。±。9.6)。在APOEε3/中。 ε3或ε3。 /ε4,与对照组相比,s-IBM中具有非常长(VL)重复T重复序列的基因型的代表性不足,并且与症状发作时的年龄较高相关,表明这些基因型可能是保护性的。我们的研究首次表明控制线粒体功能的基因中的多态性可以影响对s-IBM的敏感性并具有改善疾病的作用。但是,需要在其他s-IBM人群中进行进一步研究以证实这些发现,以及在肌肉组织中不同TOMM40等位基因的表达研究。

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