基因变异所致Farber病1例胎儿的遗传学分析 - 中华医学遗传学杂志

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中华医学遗传学杂志

• 临床遗传学论著 •

ENGLISH ABSTRACT

ASAH1基因变异所致Farber病1例胎儿的遗传学分析

作者及单位信息

出版日期： 2025 -02 -10 ·

DOI： 10.3760/cma.j.cn511374-20240910-00482

Genetic analysis of a fetus with Farber lipogranulomatosis caused by ASAH1 gene variant

Authors Info & Affiliations

Liu Yingwen

Department of Integrated Birth Defect Control, Women and Children′s Hospital of Ningbo University, Ningbo, Zhejiang 315000, China

Yan Lulu

Department of Integrated Birth Defect Control, Women and Children′s Hospital of Ningbo University, Ningbo, Zhejiang 315000, China

Zhang Yuxin

Department of Integrated Birth Defect Control, Women and Children′s Hospital of Ningbo University, Ningbo, Zhejiang 315000, China

Han Chunxiao

Department of Integrated Birth Defect Control, Women and Children′s Hospital of Ningbo University, Ningbo, Zhejiang 315000, China

Li Haibo

Department of Integrated Birth Defect Control, Women and Children′s Hospital of Ningbo University, Ningbo, Zhejiang 315000, China

Published： 2025 -02 -10 ·

DOI： 10.3760/cma.j.cn511374-20240910-00482

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摘要

目的探讨1例 ASAH1基因变异所致Farber病胎儿的临床特点和基因变异。

方法选取2024年8月在宁波大学附属妇女儿童医院就诊的1例 ASAH1基因变异所致Farber病胎儿为研究对象。收集胎儿临床资料，对胎儿引产组织样本及其父母外周血样本进行全外显子组测序(WES)，对候选变异进行Sanger测序验证与生物信息学分析。本研究已通过本院医学伦理委员会审查(批准号：EC2020-048)。

结果产前胎儿超声发现本例胎儿全身水肿、心包积液、右侧胸腔积液、肠管回声增强。WES检测发现本例胎儿 ASAH1基因第2外显子发生c.101C>A(p.Ser34Ter)纯合无义变异，Sanger测序证实其父母均携带 ASAH1基因c.101C>A(p.Ser34Ter)杂合无义变异，该变异尚未被HGMD、ClinVar、1000 Genomes、ExAC、dbSNP及gnomAD等数据库收录。根据美国医学遗传学与基因组学学会(ACMG)《遗传变异分类标准与指南》，该变异被评为致病性(PM2_Supporting＋PVS1＋PM3_Supporting)。AlphaFold3模型蛋白结构预测显示， ASAH1基因c.101C>A变异使得其编码蛋白终止密码子提前出现，进而导致ASAH1蛋白仅N端存在小部分α螺旋结构，核心结构域α螺旋结构完全丧失，可能导致该蛋白功能丧失。

结论 ASAH1基因c.101C>A(p.Ser34Ter)变异导致的Farber病可能是本研究胎儿全身水肿的遗传学病因。c.101C>A(p.Ser34Ter)变异的检出丰富了Farber病的变异谱。

关键词： Farber脂肪肉芽肿病; ASAH1基因 ;水肿胎儿;全外显子组测序;酸性神经酰胺酶

ABSTRACT

ObjectiveTo explore the clinical characteristics and gene variant of a fetus with Farber lipogranulomatosis caused by ASAH1 gene variant.

MethodsA fetus with Farber lipogranulomatosis caused by ASAH1 gene variant diagnosed at Women and Children′s Hospital of Ningbo University in August 2024 was selected as the subject. Clinical data and abortion tissue samples of the fetus and peripheral blood samples of its parents were collected for whole exome sequencing (WES). Sanger sequencing validation and bioinformatics analysis were performed on candidate variants. This study was approved by Women and Children′s Hospital of Ningbo University (Ethics No. EC2020-048).

ResultsGeneralized skin oedema, pericardial effusion, right pleural effusion and increased bowel echogenicity of the fetus were founded by prenatal ultrasound. WES revealed that the fetus has harbored a homozygous c. 101C>A(p.Ser34Ter) variation in exon 2 of the ASAH1 gene. Sanger sequencing confirmed that both parents carry the heterozygous nonsense variation c. 101C>A (p.Ser34Ter) in ASAH1 gene, which has not been included in databases such as HGMD, ClinVar, 1000 Genomes, ExAC, dbSNP, and gnomAD. Based on the Standards and Guidelines for the Interpretation of Sequence Variants of the American College of Medical Genetics and Genomics (ACMG), the variant was predicted to be pathogenic (PM2_Supporting+ PVS1+ PM3_Supporting). The AlphaFold3 model protein structure prediction reveals that the c. 101C>A variant caused the premature appearance of a termination codon, resulting in only a small partial α-helix structure in the N-terminal of the encoded ASAH1 protein, with the complete loss of the α-helix structure in the core domain, which might lead to the loss of function of this protein.

ConclusionThe c. 101C>A(p.Ser34Ter) variant of the ASAH1 gene probably underlay the Farber lipogranulomatosis with hydrops fetalis in this fetus. The newly discovered c. 101C>A(p.Ser34Ter) variant has enriched the mutational spectrum of Farber lipogranulomatosis.

KEYWORDS： Farber lipogranulomatosis; ASAH1 gene ;Hydrops fetalis;Whole exome sequencing;Acid ceramidase

Corresponding author: Li Haibo, Email: mocdef.3ab61-obiahil

FUNDING:

Ningbo Medical and Health High-level Team Program（2022020405）

Key Technology Research and Development Program of Ningbo City（2023Z178）

Public Welfare Program of Ningbo City（2022S035）

Ningbo Sci-Tech Innovation YONGJIANG 2035（2024Z221）

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Copyright by Chinese Medical Association

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All articles published represent the opinions of the authors, and do not reflect the official policy of the Chinese Medical Association or the Editorial Board, unless this is clearly specified.

引用本文

刘颖文,闫露露,张玉鑫,等. ASAH1基因变异所致Farber病1例胎儿的遗传学分析 [J]. 中华医学遗传学杂志,2025,42(02)：232-237.

DOI:10.3760/cma.j.cn511374-20240910-00482

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未经授权，不得转载、摘编本刊文章，不得使用本刊的版式设计。

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Farber病(Farber lipogranulomatosis)[美国在线人类孟德尔遗传数据库(online mendelian inheritance in man，OMIM)中编号为228000]是一种酸性神经酰胺酶缺乏症，主要临床表现为早发性皮下结节、脂肪肉芽肿病、肝大、脾大、进行性关节变形、关节疼痛及喉部受累导致的声音嘶哑等，多于婴儿期或儿童早期发病，部分患者可能在早期死亡，轻、中度患者最长可存活至60岁，其患病率和发病率目前尚不明确 ^{[
1
]}。Farber病的致病基因为 ASAH1，该基因变异可导致2种不同的常染色体隐性遗传病，即Farber病和脊髓性肌萎缩伴进行性肌阵挛性癫痫(spinal muscular atrophy with progressive myoclonic epilepsy，SMA-PME)(OMIM中编号为159950)。由于临床症状复杂，Farber病的早期诊断非常困难。多数病例均在产后得以诊断，产前表型记录极少。迄今为止，国内仅报道了1例 ASAH1基因变异所致产前胎儿水肿的Farber病胎儿 ^{[
2
]}，其他多为印度和美国病例 ^{[
3
]}。笔者拟对1例 ASAH1基因变异所致Farber病胎儿的临床特点和基因变异进行分析，旨在提升临床医师对该病的诊疗认知水平。现将研究结果报道如下。

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摘要
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备注信息

A

通信作者：李海波，Email： mocdef.3ab61577-obiahil

B

作者贡献声明

刘颖文：论文撰写、统计分析；闫露露、张玉鑫、韩春晓：实验设计、数据分析；李海波：论文修改、指导研究、经费支持

C

利益冲突

所有作者均声明不存在利益冲突

D

基金项目：

宁波市医疗卫生高端团队项目 (2022020405)

宁波市重点技术研发项目 (2023Z178)

宁波市社会公益项目 (2022S035)

宁波市科创甬江2035项目 (2024Z221)

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