中国人群中 X 连锁遗传性听力损失的基因组和表型图谱

IF 3.4 2区 医学 Q2 GENETICS & HEREDITY
Haifeng Feng, Shasha Huang, Ying Ma, Jinyuan Yang, Yijin Chen, Guojian Wang, Mingyu Han, Dongyang Kang, Xin Zhang, Pu Dai, Yongyi Yuan
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引用次数: 0

摘要

听力损失(HL)是全球最常见的先天性感官缺陷,其致病基因变异超过 150 个。然而,在中国的 HL 群体中,X 连锁遗传在 HL 中的病因贡献和临床表现仍不清楚。在本研究中,我们聚焦于 X 连锁遗传性 HL,旨在评估其对遗传性 HL 的贡献,并确定基因型与表型之间的关系。我们基于新一代测序和第三代测序对 3646 例非亲缘关系的 HL 患者进行了 X 连锁遗传性 HL 的分子流行病学调查。我们还根据文献综述讨论了与 X 连锁非综合征 HL 相关基因有关的临床特征。在我们的患者中,诊断率为 52.72%(1922/3646);由 X 染色体上的基因引起的 HL 在该队列中的总贡献率约为 1.14%(22/1922),其中由 POU3F4 变异引起的病例约占 59%(13/22)。我们发现,在所有病例中,X 连锁 HL 都是先天性的,或在儿童期就开始发病,某些基因具有代表性的听力学特征或典型的耳蜗畸形。基因型和表型分析表明,PRPS1 和 AIFM1 的致病变异主要属于错义类型,这表明表型变异与被替换的残基对结构和功能产生的不同影响有关。导致蛋白质产物截断的 SMPX 变异与 DFNX4 有关,DFNX4 会导致 10 岁前后的典型听力特征,而非截断蛋白质通常会导致远端肌病。携带 POU3F4 或 COL4A6 变体的患者没有发现表型差异。我们的工作初步评估了 X 连锁基因在遗传性 HL(约 1.14%)中的分子贡献。本文报告的 15 个新型变异扩大了这些基因的突变范围。分析基因型与表型的关系对 X 连锁 HL 的精确诊断和遗传咨询很有价值。阐明 HL 的致病机制和听力学特征还能指导治疗方法的选择。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Genomic and phenotypic landscapes of X-linked hereditary hearing loss in the Chinese population
Hearing loss (HL) is the most common sensory birth deficit worldwide, with causative variants in more than 150 genes. However, the etiological contribution and clinical manifestations of X-linked inheritance in HL remain unclear within the Chinese HL population. In this study, we focused on X-linked hereditary HL and aimed to assess its contribution to hereditary HL and identify the genotype–phenotype relationship. We performed a molecular epidemiological investigation of X-linked hereditary HL based on next-generation sequencing and third-generation sequencing in 3646 unrelated patients with HL. We also discussed the clinical features associated with X-linked non-syndromic HL-related genes based on a review of the literature. We obtained a diagnostic rate of 52.72% (1922/3646) among our patients; the aggregate contribution of HL caused by genes on the X chromosome in this cohort was ~ 1.14% (22/1922), and POU3F4 variants caused ~ 59% (13/22) of these cases. We found that X-linked HL was congenital or began during childhood in all cases, with representative audiological profiles or typical cochlear malformations in certain genes. Genotypic and phenotypic analyses showed that causative variants in PRPS1 and AIFM1 were mainly of the missense type, suggesting that phenotypic variability was correlated with the different effects that the replaced residues exert on structure and function. Variations in SMPX causing truncation of the protein product were associated with DFNX4, which resulted in typical audiological profiles before and after the age of 10 years, whereas nontruncated proteins typically led to distal myopathy. No phenotypic differences were identified in patients carrying POU3F4 or COL4A6 variants. Our work constitutes a preliminary evaluation of the molecular contribution of X-linked genes in heritable HL (~ 1.14%). The 15 novel variants reported here expand the mutational spectrum of these genes. Analysis of the genotype–phenotype relationship is valuable for X-linked HL precise diagnostics and genetic counseling. Elucidation of the pathogenic mechanisms and audiological profiles of HL can also guide choices regarding treatment modalities.
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来源期刊
Orphanet Journal of Rare Diseases
Orphanet Journal of Rare Diseases 医学-医学:研究与实验
CiteScore
6.30
自引率
8.10%
发文量
418
审稿时长
4-8 weeks
期刊介绍: Orphanet Journal of Rare Diseases is an open access, peer-reviewed journal that encompasses all aspects of rare diseases and orphan drugs. The journal publishes high-quality reviews on specific rare diseases. In addition, the journal may consider articles on clinical trial outcome reports, either positive or negative, and articles on public health issues in the field of rare diseases and orphan drugs. The journal does not accept case reports.
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