CLPP Gene Variants Causing Perrault Syndrome Type 3 in Han Chinese Families: A Genotype-Phenotype Study.

IF 3.8 3区医学 Q2 GENETICS & HEREDITY

Human Genomics Pub Date : 2025-05-23 DOI:10.1186/s40246-025-00762-5

Xicui Long, Bingqian Yang, Wei Wang, Wan Peng, Xiaolu Wang, Wenyu Xiong, Man Liu, Huijun Yuan, Yu Lu

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引用次数: 0

Abstract

Background: Perrault syndrome is a rare autosomal recessive disorder characterized by sensorineural hearing loss (SNHL) and primary ovarian insufficiency (POI) secondary to ovarian dysgenesis. However, the mutation spectrum of disease-causing genes for Perrault syndrome in the Chinese population remains poorly understood. In this study, we report on two Chinese families with Perrault syndrome type 3 caused by novel CLPP gene variants. We also conducted a comprehensive literature review of CLPP gene variants in Perrault syndrome type 3 to elucidate genotype-phenotype associations.

Methods: Using Whole Genome Sequencing (WGS) data, two pedigrees with Perrault syndrome type 3 were ascertained in the Chinese Deafness Genetics Cohort through genotype-driven analysis. Variants were validated using Sanger sequencing and copy number quantification methods. In vitro analysis of splice site variants in the CLPP gene using the minigene assay.

Results: Two Han Chinese families were ascertained: one with compound heterozygous variants (c.270 + 1G > C and c.355A > C [p. Ile119Leu]) and the other with missense variant (c.400G > C [p. Asp134His]) together with a large deletion in CLPP. In vitro minigene assays confirmed that the c.270 + 1G > C variant causes intron 2 retention and an alternative 5' splice site in exon 2, leading to protein alteration. Among 33 Perrault syndrome type 3 patients in literature, 97% (31/32) had hearing loss, 55% (16/29) neurological disease, and 71% (15/21) females had POI. Including our 4 novel variants, 21 pathogenic CLPP gene variants have been reported, with 57% (12/21) missense and 43% (9/21) truncating variants, mainly in the ATP-dependent Clp protease proteolytic subunit. Biallelic truncating or missense plus truncating genotypes showed higher rates of neurological disease (p = 0.001), but no significant difference in hearing loss incidence compared to biallelic missense genotypes was observed.

Conclusion: This study highlights the challenges in diagnosing Perrault syndrome due to its genetically and clinically heterogeneity. By exploring novel variants and establishing genotype-phenotype correlations, we aim to improve the genetic diagnosis and consultation for this complex disorder.

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中国汉族家庭CLPP基因变异导致佩诺特综合征3型：一项基因型-表型研究

背景：Perrault综合征是一种罕见的常染色体隐性遗传病，其特征为感音神经性听力损失（SNHL）和继发于卵巢发育不良的原发性卵巢功能不全（POI）。然而，中国人群中佩诺特综合征致病基因的突变谱仍然知之甚少。在这项研究中，我们报道了两个由新型CLPP基因变异引起的Perrault综合征3型的中国家庭。我们还对Perrault综合征3型CLPP基因变异进行了全面的文献综述，以阐明基因型-表型之间的关联。方法：利用全基因组测序（WGS）数据，通过基因型驱动分析，确定中国耳聋遗传队列中2个Perrault综合征3型家系。使用Sanger测序和拷贝数定量方法验证变异。CLPP基因剪接位点变异的体外分析。结果：确定了2个汉族家族：1个具有复合杂合变异体（C .270 + 1G b> C和C . 355a > C）。Ile119Leu])和另一个带有错义变体(C . 400g > C [p.]Asp134His])以及CLPP的大量缺失。体外迷你基因分析证实，C .270 + 1G > C变异导致内含子2保留和外显子2的5'剪接位点替代，导致蛋白质改变。文献中33例Perrault综合征3型患者中，97%（31/32）有听力损失，55%（16/29）有神经系统疾病，71%（15/21）女性有POI。包括我们的4个新变体在内，已有21个致病性CLPP基因变体被报道，其中57%（12/21）错义，43%（9/21）截断，主要发生在atp依赖性Clp蛋白酶水解亚基中。双等位基因截断或错义加截断基因型显示出更高的神经系统疾病发生率（p = 0.001），但与双等位基因错义基因型相比，听力损失发生率无显著差异。结论：由于Perrault综合征的遗传和临床异质性，本研究突出了诊断Perrault综合征的挑战。通过探索新的变异和建立基因型-表型相关性，我们旨在改善这种复杂疾病的遗传诊断和咨询。

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

Human Genomics GENETICS & HEREDITY-

CiteScore

6.00

自引率

2.20%

发文量

审稿时长

11 weeks

期刊介绍： Human Genomics is a peer-reviewed, open access, online journal that focuses on the application of genomic analysis in all aspects of human health and disease, as well as genomic analysis of drug efficacy and safety, and comparative genomics. Topics covered by the journal include, but are not limited to: pharmacogenomics, genome-wide association studies, genome-wide sequencing, exome sequencing, next-generation deep-sequencing, functional genomics, epigenomics, translational genomics, expression profiling, proteomics, bioinformatics, animal models, statistical genetics, genetic epidemiology, human population genetics and comparative genomics.