Biallelic variants in ERLIN1: a series of 13 individuals with spastic paraparesis.

IF 3.8 2区 生物学 Q2 GENETICS & HEREDITY
Human Genetics Pub Date : 2024-11-01 Epub Date: 2024-10-04 DOI:10.1007/s00439-024-02702-0
Guillaume Cogan, Maha S Zaki, Mahmoud Issa, Boris Keren, Marine Guillaud-Bataille, Florence Renaldo, Arnaud Isapof, Pauline Lallemant, Giovanni Stevanin, Lena Guillot-Noel, Thomas Courtin, Julien Buratti, Cécile Freihuber, Joseph G Gleeson, Robyn Howarth, Alexandra Durr, Jean-Madeleine de Sainte Agathe, Cyril Mignot
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引用次数: 0

Abstract

Biallelic variants in the ERLIN1 gene were recently reported as the cause of two motor neuron degeneration diseases, SPG62 and a recessive form of amyotrophic lateral sclerosis. However, only 12 individuals from five pedigrees have been identified so far. Thus, the description of the disease remains limited. Following the discovery of a homozygous pathogenic variant in a girl with SPG62, presenting with intellectual disability, and epilepsy, we gathered the largest series of SPG62 cases reported so far (13 individuals) to better understand the phenotype associated with ERLIN1. We collected molecular and clinical data for 13 individuals from six families with ERLIN1 biallelic variants. We performed RNA-seq analyses to characterize intronic variants and used Alphafold and a transcripts database to characterize the molecular consequences of the variants. We identified three new variants suspected to alter the bell-shaped ring formed by the ERLIN1/ERLIN2 complex. Affected individuals had childhood-onset paraparesis with slow progression. Six individuals presented with gait ataxia and three had superficial sensory loss. Aside from our proband, none had intellectual disability or epilepsy. Biallelic pathogenic ERLIN1 variants induce a rare, predominantly pure, spastic paraparesis, with possible cerebellar and peripheral nerve involvement.

ERLIN1的双倍变体:13例痉挛性截瘫患者的系列研究。
最近有报道称,ERLIN1 基因的双叶变体是两种运动神经元变性疾病(SPG62 和一种隐性肌萎缩侧索硬化症)的病因。然而,迄今为止,仅从五个血统中鉴定出 12 个个体。因此,对该疾病的描述仍然有限。在一名患有 SPG62 并伴有智力障碍和癫痫的女孩身上发现了一个同卵致病变体后,我们收集了迄今为止报道的最大系列的 SPG62 病例(13 例),以更好地了解与 ERLIN1 相关的表型。我们收集了来自六个ERLIN1双倍变体家庭的13名患者的分子和临床数据。我们进行了 RNA-seq 分析,以确定内含子变异的特征,并使用 Alphafold 和转录本数据库来确定变异的分子后果。我们发现了三个疑似改变 ERLIN1/ERLIN2 复合物形成的钟形环的新变异。受影响的个体在儿童时期就出现了偏瘫,且进展缓慢。六人出现步态共济失调,三人出现浅表感觉缺失。除我们的原型外,其他人都没有智力障碍或癫痫。双倍拷贝致病性ERLIN1变体会诱发一种罕见的、以单纯性为主的痉挛性截瘫,并可能累及小脑和周围神经。
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来源期刊
Human Genetics
Human Genetics 生物-遗传学
CiteScore
10.80
自引率
3.80%
发文量
94
审稿时长
1 months
期刊介绍: Human Genetics is a monthly journal publishing original and timely articles on all aspects of human genetics. The Journal particularly welcomes articles in the areas of Behavioral genetics, Bioinformatics, Cancer genetics and genomics, Cytogenetics, Developmental genetics, Disease association studies, Dysmorphology, ELSI (ethical, legal and social issues), Evolutionary genetics, Gene expression, Gene structure and organization, Genetics of complex diseases and epistatic interactions, Genetic epidemiology, Genome biology, Genome structure and organization, Genotype-phenotype relationships, Human Genomics, Immunogenetics and genomics, Linkage analysis and genetic mapping, Methods in Statistical Genetics, Molecular diagnostics, Mutation detection and analysis, Neurogenetics, Physical mapping and Population Genetics. Articles reporting animal models relevant to human biology or disease are also welcome. Preference will be given to those articles which address clinically relevant questions or which provide new insights into human biology. Unless reporting entirely novel and unusual aspects of a topic, clinical case reports, cytogenetic case reports, papers on descriptive population genetics, articles dealing with the frequency of polymorphisms or additional mutations within genes in which numerous lesions have already been described, and papers that report meta-analyses of previously published datasets will normally not be accepted. The Journal typically will not consider for publication manuscripts that report merely the isolation, map position, structure, and tissue expression profile of a gene of unknown function unless the gene is of particular interest or is a candidate gene involved in a human trait or disorder.
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