Exploring novel MYH7 gene variants using in silico analyses in Korean patients with cardiomyopathy.

IF 2.1 4区 医学 Q3 GENETICS & HEREDITY BMC Medical Genomics Pub Date : 2024-09-05 DOI:10.1186/s12920-024-02000-8
Oc-Hee Kim, Jihyun Kim, Youngjun Kim, Soyoung Lee, Beom Hee Lee, Bong-Jo Kim, Hyun-Young Park, Mi-Hyun Park
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Abstract

Background: Pathogenic variants of MYH7, which encodes the beta-myosin heavy chain protein, are major causes of dilated and hypertrophic cardiomyopathy.

Methods: In this study, we used whole-genome sequencing data to identify MYH7 variants in 397 patients with various cardiomyopathy subtypes who were participating in the National Project of Bio Big Data pilot study in Korea. We also performed in silico analyses to predict the pathogenicity of the novel variants, comparing them to known pathogenic missense variants.

Results: We identified 27 MYH7 variants in 41 unrelated patients with cardiomyopathy, consisting of 20 previously known pathogenic/likely pathogenic variants, 2 variants of uncertain significance, and 5 novel variants. Notably, the pathogenic variants predominantly clustered within the myosin motor domain of MYH7. We confirmed that the novel identified variants could be pathogenic, as indicated by high prediction scores in the in silico analyses, including SIFT, Mutation Assessor, PROVEAN, PolyPhen-2, CADD, REVEL, MetaLR, MetaRNN, and MetaSVM. Furthermore, we assessed their damaging effects on protein dynamics and stability using DynaMut2 and Missense3D tools.

Conclusions: Overall, our study identified the distribution of MYH7 variants among patients with cardiomyopathy in Korea, offering new insights for improved diagnosis by enriching the data on the pathogenicity of novel variants using in silico tools and evaluating the function and structural stability of the MYH7 protein.

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利用硅学分析探索韩国心肌病患者的新型 MYH7 基因变异。
背景:编码β-肌球蛋白重链蛋白的MYH7的致病变体是导致扩张型和肥厚型心肌病的主要原因:在这项研究中,我们利用全基因组测序数据,在参加韩国国家生物大数据项目试点研究的397名不同心肌病亚型患者中鉴定了MYH7变体。我们还进行了硅学分析,预测新型变异的致病性,并将它们与已知的致病性错义变异进行比较:结果:我们在41名无亲属关系的心肌病患者中发现了27个MYH7变异体,其中包括20个以前已知的致病/可能致病变异体、2个意义不确定的变异体和5个新型变异体。值得注意的是,致病变异主要集中在 MYH7 的肌球蛋白运动结构域。我们证实,已发现的新型变异可能是致病性的,因为它们在硅学分析(包括SIFT、Mutation Assessor、PROVEAN、PolyPhen-2、CADD、REVEL、MetaLR、MetaRNN和MetaSVM)中的预测得分很高。此外,我们还使用 DynaMut2 和 Missense3D 工具评估了它们对蛋白质动态和稳定性的破坏性影响:总之,我们的研究确定了韩国心肌病患者中MYH7变体的分布情况,通过使用硅学工具丰富了新型变体的致病性数据,并评估了MYH7蛋白的功能和结构稳定性,为改进诊断提供了新的见解。
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来源期刊
BMC Medical Genomics
BMC Medical Genomics 医学-遗传学
CiteScore
3.90
自引率
0.00%
发文量
243
审稿时长
3.5 months
期刊介绍: BMC Medical Genomics is an open access journal publishing original peer-reviewed research articles in all aspects of functional genomics, genome structure, genome-scale population genetics, epigenomics, proteomics, systems analysis, and pharmacogenomics in relation to human health and disease.
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