Identification of 13 novel pathogenic SLC25A13 variants and comparison of the genetic spectrum among different geographic regions: Molecular characterization of a large cohort of citrin deficiency in China

IF 3.5 2区生物学 Q2 ENDOCRINOLOGY & METABOLISM

Molecular genetics and metabolism Pub Date : 2025-09-01 DOI:10.1016/j.ymgme.2025.109238

Rui-Lan Cheng , Jian-Wu Qiu , Qin Zhou , Joseph Hong Saberon , Jian Shi , Mei Deng , Li Guo , Feng-Ping Chen , Wei-Xia Lin , Yuan-Zong Song

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引用次数: 0

Abstract

Objective

Citrin deficiency (CD), caused by biallelic pathogenic variants in SLC25A13, remains underdiagnosed due to allelic heterogeneity, variants of uncertain significance (VUS), and technical limitations. This study aimed to improve the diagnosis of CD by identifying novel pathogenic SLC25A13 variants and characterizing the variant spectrum and geographic distribution in a large Chinese pediatric cohort.

Methods

Polymerase chain reaction (PCR)-based methods and Sanger sequencing were performed to identify pathogenic SLC25A13 variants in 220 pediatric patients with clinically suspected CD and their parents from 2016 to 2024. We functionally validated novel missense and splice-site variants using agc1-knockout yeast modeling and minigene assays, respectively. Data from these 191 newly diagnosed CD patients (2016–2024) were combined with data from 274 previously reported CD cases (2005–2016) and from 186 additional CD patients diagnosed via next-generation sequencing since 2016. The SLC25A13 variant spectrum and geographic distribution were then analyzed in this combined cohort. Statistical analyses were performed using Chi-square/Fisher's exact tests and one-way analysis of variance, as appropriate.

Results

A large cohort of 651 CD patients was assembled, and 13 novel pathogenic SLC25A13 variants were identified, including c.177_189del, c.188del, c.212 + 3 A > G, c.889G > T, c.1193 T > A, c.1210G > T, c.1352 T > A, c.1620del, c.1722del, c.1799_1800insAAA, c.1853_1855dup, c.1603_1609dup, and c.819-16 T > A. The most frequent variants were c.852_855del (57.56 %), c.1751-5_1751–4ins(2684) (10.06 %), c.1638_1660dup (8.42 %), and c.615 + 5G > A (7.93 %). The variant c.329-3_329-2ins(6072) ranked fifth at 2.13 %. In the Chinese mainland, the variant c.852_855del was most prevalent in southern and southwestern provinces, c.1638_1660dup was enriched in eastern coastal regions, and c.1751-5_1751–4ins(2684) reached its highest frequency in Sichuan Province (29.7 %).

Conclusions

The study established the largest CD cohort to date, expanded the SLC25A13 variant spectrum, and delineated the distinct geographic distribution of these variants. These findings refined diagnostic protocols and emphasized the necessity for population-tailored genetic screening to optimize early diagnosis of CD.

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13个SLC25A13新致病变异的鉴定及不同地理区域遗传谱的比较：中国柑橘素缺乏症大队列的分子特征

目的：由于等位基因异质性、不确定意义变异（VUS）和技术限制，SLC25A13双等位基因致病变异引起的卵黄素缺乏症（CD）仍未得到充分诊断。本研究旨在通过鉴定新的致病SLC25A13变异，并在中国大型儿科队列中描述变异谱和地理分布，以提高CD的诊断水平。方法采用聚合酶链反应（PCR）方法和Sanger测序对2016 - 2024年220例临床疑似CD患儿及其父母的SLC25A13致病变异进行鉴定。我们分别使用agc1敲除酵母模型和迷你基因分析对新的错义和剪接位点变异进行了功能验证。来自这191名新诊断的CD患者（2016 - 2024）的数据与先前报告的274例CD病例（2005-2016）的数据以及自2016年以来通过下一代测序诊断的额外186例CD患者的数据相结合。然后在这个联合队列中分析SLC25A13变异谱和地理分布。采用卡方/费雪精确检验和单因素方差分析进行统计分析。结果对651例CD患者进行了大队列分析，鉴定出13种新的SLC25A13致病变异，包括c.177_189del、c.188del、c.212 + 3 A > G、c.889G > T、c.1193T >； A, c.1210G >； T, c.1352T > A、c.1620del、c.1722del、c.1799_1800insAAA、c.1853_1855dup、c.1603_1609dup和c.819-16 T >； A最常见的变异是c.852_855del（57.56%）、c.1751-5_1751-4ins(2684)（10.06%）、c.1638_1660dup（8.42%）和c.615 + 5G >； A（7.93%）。改型c.329-3_329-2ins（6072）排在第5位，为2.13%。在中国大陆，c.852_855del变异在南部和西南省份最为普遍，c.1638_1660dup富集于东部沿海地区，c.1751-5_1751-4ins（2684）在四川省出现频率最高（29.7%）。该研究建立了迄今为止最大的CD队列，扩展了SLC25A13变异谱，并描绘了这些变异的独特地理分布。这些发现完善了诊断方案，并强调了针对人群进行遗传筛查以优化乳糜泻早期诊断的必要性。

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 metabolism 生物-生化与分子生物学

CiteScore

5.90

自引率

7.90%

发文量

621

审稿时长

34 days

期刊介绍： Molecular Genetics and Metabolism contributes to the understanding of the metabolic and molecular basis of disease. This peer reviewed journal publishes articles describing investigations that use the tools of biochemical genetics and molecular genetics for studies of normal and disease states in humans and animal models.