Genotypic spectrum of ABCA4-associated retinal degenerations in 211 unrelated Mexican patients: identification of 22 novel disease-causing variants.

IF 2.3 3区生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY

Molecular Genetics and Genomics Pub Date : 2024-08-20 DOI:10.1007/s00438-024-02174-x

Oscar F Chacon-Camacho, Nancy Xilotl-de Jesús, Ernesto Calderón-Martínez, Vianey Ordoñez-Labastida, M Isabel Neria-Gonzalez, Rocío Villafuerte-de la Cruz, Augusto Martinez-Rojas, Juan Carlos Zenteno

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引用次数: 0

Abstract

The purpose of this study was to analyze and molecularly describe the largest group of patients with ABCA4-associated retinal degeneration in Latin America. Pathogenic variants in ABCA4, a member of the ATP Binding Cassette (ABC) transporters superfamily, is one of the most common causes of inherited visual deficiency in humans. Retinal phenotypes associated with genetic defects in ABCA4 are collectively known as ABCA4-associated retinal degenerations (ABCA4R), a group of recessively inherited disorders associated with a high allelic heterogeneity. While large groups of Caucasian and Asiatic individuals suffering from ABCA4R have been well characterized, molecular information from certain ethnic groups is limited or unavailable, precluding a more realistic knowledge of ABCA4-related mutational profile worldwide. In this study, we describe the molecular findings of a large group of 211 ABCA4R index cases from Mexico. Genotyping was performed using either next generation sequencing (NGS) of a retinal dystrophy genes panel or exome. ABCA4 targeted mutation testing was applied to a subgroup of subjects in whom founder mutations were suspected. A total of 128 different ABCA4 pathogenic variants were identified, including 22 previously unpublished variants. The most common type of genetic variation was single nucleotide substitutions which occurred in 92.7% (408/440 alleles). According to the predicted protein effect, the most frequent variant type was missense, occurring in 83.5% of disease-causing alleles (368/440). Mutations such as p.Ala1773Val are fully demonstrated as a founder effect in native inhabitants of certain regions of Mexico. This study also gives us certain indications of other founder effects that need to be further studied in the near future. This is the largest molecularly characterized ABCA4R Latin American cohort, and our results supports the value of conducting genetic screening in underrepresented populations for a better knowledge of the mutational profile leading to monogenic diseases.

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211 名无血缘关系的墨西哥患者 ABCA4 相关视网膜变性的基因型谱：鉴定出 22 个新型致病变体。

这项研究的目的是对拉丁美洲最大的一组 ABCA4 相关视网膜变性患者进行分析和分子描述。ABCA4是ATP结合盒（ABC）转运体超家族的成员，其致病变异是导致人类遗传性视力缺陷的最常见原因之一。与 ABCA4 遗传缺陷相关的视网膜表型统称为 ABCA4 相关视网膜变性（ABCA4R），这是一组隐性遗传疾病，具有高度等位基因异质性。虽然一大批白种人和亚洲人患 ABCA4R 的特征已被很好地描述，但来自某些种族群体的分子信息却很有限或无法获得，这使得人们无法更真实地了解全球 ABCA4 相关突变的概况。在本研究中，我们描述了一大批来自墨西哥的 211 例 ABCA4R 指数病例的分子研究结果。基因分型是通过视网膜营养不良基因面板或外显子组的新一代测序（NGS）进行的。ABCA4靶向突变检测适用于怀疑存在始祖突变的受试者亚群。共鉴定出128个不同的ABCA4致病变异，其中包括22个以前未发表过的变异。最常见的基因变异类型是单核苷酸置换，占 92.7%（408/440 个等位基因）。根据预测的蛋白质效应，最常见的变异类型是错义，出现在83.5%的致病等位基因中（368/440）。p.Ala1773Val这样的变异在墨西哥某些地区的原住民中被充分证明是一种创始效应。这项研究还为我们提供了其他创始效应的某些迹象，需要在不久的将来进一步研究。这是拉丁美洲最大的 ABCA4R 分子特征队列，我们的研究结果支持了在代表性不足的人群中进行基因筛查的价值，以便更好地了解导致单基因疾病的突变特征。

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

Molecular Genetics and Genomics 生物-生化与分子生物学

CiteScore

5.10

自引率

3.20%

发文量

134

审稿时长

1 months

期刊介绍： Molecular Genetics and Genomics (MGG) publishes peer-reviewed articles covering all areas of genetics and genomics. Any approach to the study of genes and genomes is considered, be it experimental, theoretical or synthetic. MGG publishes research on all organisms that is of broad interest to those working in the fields of genetics, genomics, biology, medicine and biotechnology. The journal investigates a broad range of topics, including these from recent issues: mechanisms for extending longevity in a variety of organisms; screening of yeast metal homeostasis genes involved in mitochondrial functions; molecular mapping of cultivar-specific avirulence genes in the rice blast fungus and more.