A Novel Mutation (Lys31Arg) in the DMD Gene Impacts on Neuromuscular Dysfunctions Found by Whole Exome Sequencing and In Silico Analyses in an Iranian Family.

Q3 Medicine

Current aging science Pub Date : 2024-01-01 DOI:10.2174/0118746098280408240112112414

Vahid Omarmeli, Kai-Uwe Lewandrowski, Marjan Assefi, Hanieh Faizmahdavi, Alireza Sharafshah, Nasrin Mansouri

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引用次数: 0

Abstract

Background: Duchene Muscular Disorder (DMD) is a severe X-linked recessive neuromuscular disease. Previous reports predicted that one-third of cases with a fatal X-linked recessive disease will be caused by a novel mutation, and the mutation rate for DMD seems to be higher in males.

Objective: A novel mutation in the DMD gene DMD (NM_004006.3):c.92A>G (p.Lys31Arg) is suggested for males because of their heterozygous mothers carrying the mutant alleles.

Method: Whole Exome Sequencing (WES) was done for a 25-year-old female followed by the screening of the novel mutation in her parents and her brother by the Sanger sequencing technique. Some in silico analyses were run to find the putative alterations in wild-type and mutant structures by PolyPhen-2 and Mupro. Notably, SWISS-MODEL was performed to build a reliable model for the mutant allele based on the PDB ID: 1DXX structure. Also, superimposition was done by PyMol.

Results: WES analysis revealed three novel mutations including DLD (exon13:c.G1382A:p. G461E), ABCA3 (exon12:c.G1404C:p.W468C), and DMD (exon2:c.A92G:p.K31R) in the case. Focusing on DMD mutation, Sanger sequencing of the patient's parents and brother indicated no mutant allele in her mother and brother but a mutant allele in her father as a hemizygous pattern. In silico analyses showed no considerable change regarding pathogenic impact.

Conclusion: In conclusion, our findings revealed no pathogenic effect of the new mutation (K31R) of the DMD gene in an Iranian 25-year-old woman. Because of the DMD importance in preclinical diagnosis, these data may shed a light on the diagnosis of this mutation in future pregnancies.

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通过对一个伊朗家庭进行全外显子组测序和 In Silico 分析，发现 DMD 基因中的一个新突变（Lys31Arg）对神经肌肉功能障碍有影响。

背景介绍杜氏肌肉病（DMD）是一种严重的X连锁隐性神经肌肉病。以前的报告预测，在致命的 X 连锁隐性疾病中，有三分之一的病例是由新型突变引起的，而 DMD 的突变率似乎在男性中更高：目的：DMD基因DMD（NM_004006.3）中的一个新突变：c.92A>G（p.Lys31Arg）被认为是男性的突变，因为他们的母亲是携带突变等位基因的杂合子：方法：对一名 25 岁的女性进行了全外显子组测序（WES），然后用 Sanger 测序技术在其父母和兄弟中筛查了新型突变。通过 PolyPhen-2 和 Mupro，对野生型和突变型结构中的推测改变进行了一些默观分析。值得注意的是，通过 SWISS-MODEL，我们根据 PDB ID：1DXX 结构为突变等位基因建立了一个可靠的模型。此外，还利用 PyMol 进行了叠加：结果：WES分析发现了病例中的三个新突变，包括DLD（exon13:c.G1382A:p.G461E）、ABCA3（exon12:c.G1404C:p.W468C）和DMD（exon2:c.A92G:p.K31R）。针对 DMD 基因突变，对患者的父母和兄弟进行了 Sanger 测序，结果显示其母亲和兄弟中没有突变等位基因，但其父亲中存在突变等位基因，为半等位基因模式。硅学分析表明，该基因对致病性的影响没有显著变化：总之，我们的研究结果表明，在一名 25 岁的伊朗女性身上，DMD 基因的新突变 (K31R) 没有致病作用。鉴于 DMD 在临床前诊断中的重要性，这些数据可能会对今后妊娠中该基因突变的诊断有所启示。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Current aging science Medicine-Geriatrics and Gerontology

CiteScore

3.90

自引率

0.00%

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