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TCTEX1D1 is a genetic modifier of disease progression in Duchenne muscular dystrophy

机译:TCTEX1D1是Duchenne肌营养不良症中疾病进展的遗传改性剂

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Duchenne muscular dystrophy (DMD) is caused by pathogenic variants in the DMD gene leading to the lack of dystrophin. Variability in the disease course suggests that other factors influence disease progression. With this study we aimed to identify genetic factors that may account for some of the variability in the clinical presentation. We compared whole-exome sequencing (WES) data in 27 DMD patients with extreme phenotypes to identify candidate variants that could affect disease progression. Validation of the candidate SNPs was performed in two independent cohorts including 301 (BIO-NMD cohort) and 109 (CINRG cohort of European ancestry) DMD patients, respectively. Variants in the Tctex1 domain containing 1 (TCTEX1D1) gene on chromosome 1 were associated with age of ambulation loss. The minor alleles of two independent variants, known to affect TCTEX1D1 coding sequence and induce skipping of its exon 4, were associated with earlier loss of ambulation. Our data show that disease progression of DMD is affected by a new locus on chromosome 1 and demonstrate the possibility to identify genetic modifiers in rare diseases by studying WES data in patients with extreme phenotypes followed by multiple layers of validation.
机译:Duchenne肌营养不良(DMD)是由DMD基因的致病变异引起的,导致缺乏患病素。疾病课程中的变异性表明其他因素会影响疾病进展。通过这项研究,我们的旨在识别可能考虑临床介绍中一些可变性的遗传因素。我们将全exome测序(WES)数据中的27名DMD患者进行了极端表型,以确定可能影响疾病进展的候选变体。候选SNP的验证分别在两个独立的队列中进行,其中包括301(Bio-NMD Cohort)和109(Cinrg群组欧洲血清群)DMD患者。含有1(TCTEX1D1)基因的TCTEX1结构域在染色体1上的变体与手提损失的年龄相关。两个独立变体的次要等位基因,已知影响TCTEX1D1编码序列并诱导其外显子4的跳跃,与早期的散布有关。我们的数据显示DMD的疾病进展受到染色体1的新轨迹的影响,并证明了通过在具有极端表型患者中研究WES数据,然后通过多层验证研究WES数据来鉴定稀有疾病中的遗传改性剂。

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