扩大HSPB8相关肌病的范围:一种新型突变导致非典型儿科发病性轴向和肢腰受累,并伴有自噬异常和分子动力学研究。

IF 2.6 3区 生物学 Q2 GENETICS & HEREDITY Journal of Human Genetics Pub Date : 2024-11-15 DOI:10.1038/s10038-024-01305-x
Guiguan Yang, Xiaoqing Lv, Mengqi Yang, Yifei Feng, Guangyu Wang, Chuanzhu Yan, Pengfei Lin
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引用次数: 0

摘要

HSPB8 变异主要与周围神经病有关,但在肌病中出现这种变异却极为罕见。HSPB8相关肌病的遗传和临床谱系尚不完整。在本文中,我们不仅描述了中国首例HSPB8相关肌病病例,该病例的特征是HSPB8 C端区域的一个新型杂合子帧移位变异(c.576_579delinsCAG, p.Glu192Aspfs*55),而且还首次证实了这种特定的HSPB8变异与小儿发病的轴性和肢腰肌病之间的关联。肌肉病理学显示了肌纤维肌病的特征,以及炎症反应和空泡与肌浆特征病理学的新病理发现。功能研究显示,HSPB8与自噬标记物显著共定位,自噬相关蛋白上调,这表明自噬失调可能是导致该病病理过程的原因之一。此外,综合生物信息学分析和分子动力学模拟显示,突变体HSPB8的聚集倾向增加,结构和生化特性也发生了改变。我们的研究强调了在早发轴性肌病和肢腰肌病中考虑HSPB8突变的重要性,扩大了该病的遗传和表型谱。值得注意的是,我们的研究结果强调了自噬失调和异常蛋白聚集在发病机制中的关键作用,为潜在的治疗靶点提供了新的见解。
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Expanding the spectrum of HSPB8-related myopathy: a novel mutation causing atypical pediatric-onset axial and limb-girdle involvement with autophagy abnormalities and molecular dynamics studies.

Variants in HSPB8 are predominantly associated with peripheral neuropathies, but their occurrence in myopathies remains exceedingly rare. The genetic and clinical spectrum of HSPB8-related myopathy is not yet complete. Herein, we not only described the first Chinese case of HSPB8-related myopathy characterized by a novel heterozygous frameshift variant (c.576_579delinsCAG, p.Glu192Aspfs*55) in the C-terminal region of HSPB8, but also established the first association between this specific HSPB8 variant and pediatric-onset axial and limb-girdle myopathy. Muscle pathology revealed myofibrillar myopathy features and the novel pathological findings of inflammatory responses and vacuoles with sarcolemmal features pathology. Functional studies demonstrated significant colocalization of HSPB8 with autophagy markers and upregulation of autophagy-related proteins, which suggested that autophagic dysregulation may contribute to the pathological process of this disease. Furthermore, comprehensive bioinformatics analysis and molecular dynamics simulations revealed an increased propensity for aggregation, as well as altered structural and biochemical properties in the mutant HSPB8. Our study highlights the importance of considering HSPB8 mutations in early-onset axial and limb-girdle myopathy, expanding the genetic and phenotypic spectrum of the disease. Notably, our results underscore the critical role of autophagy dysregulation and aberrant protein aggregation in the pathogenesis, providing novel insights into potential therapeutic targets.

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来源期刊
Journal of Human Genetics
Journal of Human Genetics 生物-遗传学
CiteScore
7.20
自引率
0.00%
发文量
101
审稿时长
4-8 weeks
期刊介绍: The Journal of Human Genetics is an international journal publishing articles on human genetics, including medical genetics and human genome analysis. It covers all aspects of human genetics, including molecular genetics, clinical genetics, behavioral genetics, immunogenetics, pharmacogenomics, population genetics, functional genomics, epigenetics, genetic counseling and gene therapy. Articles on the following areas are especially welcome: genetic factors of monogenic and complex disorders, genome-wide association studies, genetic epidemiology, cancer genetics, personal genomics, genotype-phenotype relationships and genome diversity.
期刊最新文献
Identification of biallelic intronic EPM2A mutations in a Lafora disease kindred. Expanding the spectrum of HSPB8-related myopathy: a novel mutation causing atypical pediatric-onset axial and limb-girdle involvement with autophagy abnormalities and molecular dynamics studies. Novel variants in DNAH9 are present in two infertile patients with severe asthenospermia. Homozygous synonymous FAM111A variant underlies an autosomal recessive form of Kenny-Caffey syndrome. The distribution of regions of homozygosity (ROH) among consanguineous populations-implications for a routine genetic counseling service.
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