An estimation of global genetic prevalence of PLA2G6-associated neurodegeneration.

IF 3.4 2区医学 Q2 GENETICS & HEREDITY

Orphanet Journal of Rare Diseases Pub Date : 2024-10-18 DOI:10.1186/s13023-024-03275-x

Amina Kurtovic-Kozaric, Moriel Singer-Berk, Jordan Wood, Emily Evangelista, Leena Panwala, Amanda Hope, Stefanie M Heinrich, Samantha Baxter, Mark J Kiel

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引用次数: 0

Abstract

Background: PLA2G6-associated neurodegeneration (PLAN) comprises three diseases with overlapping features: infantile neuroaxonal dystrophy (INAD), atypical neuroaxonal dystrophy (atypical NAD), and PLA2G6-related dystonia-parkinsonism. INAD is an early onset disease characterized by progressive loss of vision, muscular control, and mental skills. The prevalence of PLA2G6-associated diseases has not been previously calculated.

Methods: To provide the most accurate prevalence estimate, we utilized two independent approaches: database-based approach which included collecting variants from ClinVar, Human Gene Mutation Database (HGMD) and high confidence predicted loss-of-function (pLoF) from gnomAD (Rare Genomes Project Genetic Prevalence Estimator; GeniE), and literature-based approach which gathered variants through Mastermind Genomic Search Engine (Genomenon, Inc). Genetic prevalence of PLAN was calculated based on allele frequencies from gnomAD, assuming Hardy-Weinberg equilibrium.

Results: In the PLA2G6 gene, our analysis found 122 pathogenic, 82 VUS, and 15 variants with conflicting interpretations (pathogenic vs VUS) between two approaches. Allele frequency was available for 58 pathogenic, 42 VUS, and 15 conflicting variants in gnomAD database. If pathogenic and/or conflicting variants are included, the overall genetic prevalence was estimated to be between 1 in 987,267 to 1 in 1,570,079 pregnancies, with the highest genetic prevalence in African/African-American (1 in 421,960 to 1 in 365,197) and East-Asian (1 in 683,978 to 1 in 190,771) populations.

Conclusion: Our estimates highlight the significant underdiagnosis of PLA2G6-associated neurodegeneration and underscores the need for increased awareness and diagnostic efforts. Furthermore, our study revealed a higher carrier frequency of PLA2G6 variants in African and Asian populations, stressing the importance of expanded genetic sequencing in non-European populations to ensure accurate and comprehensive diagnosis. Future research should focus on confirming our findings and implementing expanded sequencing strategies to facilitate maximal and accurate diagnosis, particularly in non-European populations.

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PLA2G6相关神经变性的全球遗传流行率估算。

背景：PLA2G6相关神经变性（PLAN）包括三种具有重叠特征的疾病：婴儿神经轴性营养不良症（INAD）、非典型神经轴性营养不良症（NAD）和PLA2G6相关肌张力障碍-帕金森病。INAD是一种早发性疾病，其特征是逐渐丧失视力、肌肉控制能力和智力。PLA2G6 相关疾病的患病率以前从未计算过：为了提供最准确的患病率估计，我们采用了两种独立的方法：一种是基于数据库的方法，包括从ClinVar、人类基因突变数据库（HGMD）和gnomAD（罕见基因组计划遗传患病率估计器；GeniE）的高置信度预测功能缺失（pLoF）中收集变异；另一种是基于文献的方法，通过Mastermind基因组搜索引擎（Genomenon，Inc）收集变异。根据 gnomAD 中的等位基因频率计算 PLAN 的遗传流行率，并假定哈代-温伯格平衡（Hardy-Weinberg equilibrium）：在 PLA2G6 基因中，我们的分析发现了 122 个致病变异、82 个 VUS 变异和 15 个变异，两种方法对这些变异的解释存在冲突（致病变异与 VUS 变异）。在 gnomAD 数据库中有 58 个致病变异、42 个 VUS 变异和 15 个冲突变异的等位基因频率。如果将致病变异体和/或冲突变异体包括在内，总体遗传患病率估计为每 987,267 到 1,570,079 例妊娠中有 1 例，其中非洲/非裔美国人（每 421,960 到 365,197 例妊娠中有 1 例）和东亚人（每 683,978 到 190,771 例妊娠中有 1 例）的遗传患病率最高：我们的估算结果突显了 PLA2G6 相关神经变性的诊断率严重不足，并强调了提高意识和加强诊断工作的必要性。此外，我们的研究显示，非洲和亚洲人群中 PLA2G6 变体的携带者频率较高，这强调了在非欧洲人群中扩大基因测序以确保准确和全面诊断的重要性。未来的研究应侧重于证实我们的发现，并实施扩大测序策略，以促进最大限度的准确诊断，尤其是在非欧洲人群中。

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

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.