人类耳聋基因序列和拷贝数变异的联合检查提高了对遗传性耳聋病例的诊断。

Q2 Medicine

BMC Ear, Nose and Throat Disorders Pub Date : 2014-09-10 eCollection Date: 2014-01-01 DOI:10.1186/1472-6815-14-9

Haiting Ji, Jingqiao Lu, Jianjun Wang, Huawei Li, Xi Lin

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引用次数: 30

摘要

背景:拷贝数变异(拷贝数变异)是人类基因组结构变异的主要类型，在人群中比DNA序列变异更常见。CNVs是人类遗传和表型多样性的重要因素。许多CNVs要么与疾病抗性有关，要么被确定为疾病的原因。目前对CNVs在引起耳聋中的作用知之甚少。目前，传统的遗传分析方法无法分析CNVs来研究耳聋。在这里，我们检测了影响正常听力所需的80个基因的DNA序列变异和CNVs。方法:采用基于杂交的方法捕获耳聋基因的编码区，并使用Illumina平台通过标准下一代测序(NGS)协议进行处理。在同一反应中杂交在一起的样品进行分析以获得CNVs。使用基于读取深度的方法在单个外显子的分辨率上测量CNVs。采用定量PCR (qPCR)方法对结果进行验证。结果:在79例临床诊断为感音神经性听力损失的散发病例中，我们在16例中发现了先前报道的致病序列突变。此外，我们在27个耳聋基因中共鉴定出97个CNV(72个CNV增加，25个CNV减少)。这些CNV包括可能直接对已知听力所必需的蛋白质功能产生有害影响的纯合缺失，以及杂合缺失和CNV增益与可能潜在损害基因功能的耳聋基因序列突变相结合。结论:我们研究了已知耳聋基因的CNVs如何导致耳聋。这里提供的数据可以作为解释CNVs如何破坏耳聋基因正常功能的基础。这些结果可能会大大扩展我们对各种类型的基因突变如何导致人类耳聋的理解。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Combined examination of sequence and copy number variations in human deafness genes improves diagnosis for cases of genetic deafness.

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Combined examination of sequence and copy number variations in human deafness genes improves diagnosis for cases of genetic deafness.

Background: Copy number variations (CNVs) are the major type of structural variation in the human genome, and are more common than DNA sequence variations in populations. CNVs are important factors for human genetic and phenotypic diversity. Many CNVs have been associated with either resistance to diseases or identified as the cause of diseases. Currently little is known about the role of CNVs in causing deafness. CNVs are currently not analyzed by conventional genetic analysis methods to study deafness. Here we detected both DNA sequence variations and CNVs affecting 80 genes known to be required for normal hearing.

Methods: Coding regions of the deafness genes were captured by a hybridization-based method and processed through the standard next-generation sequencing (NGS) protocol using the Illumina platform. Samples hybridized together in the same reaction were analyzed to obtain CNVs. A read depth based method was used to measure CNVs at the resolution of a single exon. Results were validated by the quantitative PCR (qPCR) based method.

Results: Among 79 sporadic cases clinically diagnosed with sensorineural hearing loss, we identified previously-reported disease-causing sequence mutations in 16 cases. In addition, we identified a total of 97 CNVs (72 CNV gains and 25 CNV losses) in 27 deafness genes. The CNVs included homozygous deletions which may directly give rise to deleterious effects on protein functions known to be essential for hearing, as well as heterozygous deletions and CNV gains compounded with sequence mutations in deafness genes that could potentially harm gene functions.

Conclusions: We studied how CNVs in known deafness genes may result in deafness. Data provided here served as a basis to explain how CNVs disrupt normal functions of deafness genes. These results may significantly expand our understanding about how various types of genetic mutations cause deafness in humans.

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来源期刊

BMC Ear, Nose and Throat Disorders Medicine-Otorhinolaryngology

CiteScore

3.30

自引率

0.00%

发文量

期刊介绍： BMC Ear, Nose and Throat Disorders is an open access journal publishing original peer-reviewed research articles in all aspects of the prevention, diagnosis and management of ear, nose and throat disorders, as well as related molecular genetics, pathophysiology, and epidemiology. BMC Ear, Nose and Throat Disorders (ISSN 1472-6815) is indexed/tracked/covered by PubMed, CAS, EMBASE, Scopus and Google Scholar.