Early presentation of spastic paraparesis in individuals carrying PSEN1 mutations: a clinical and genetic analysis.

IF 7.9 1区医学 Q1 CLINICAL NEUROLOGY

Alzheimer's Research & Therapy Pub Date : 2025-04-30 DOI:10.1186/s13195-025-01744-4

Kang-Yang Jih, Ting-Rong Hsu, Jong-Ling Fuh, Tse-Hao Lee, Yung-Shuan Lin, Shih-Yu Fang, Yi-Chu Liao, Yi-Chung Lee

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Abstract

Background: Mutations in the presenilin 1 gene (PSEN1) are well-known causes of early-onset familial Alzheimer's disease, but they can also present with atypical phenotypes such as pure spastic paraparesis. This study aims to investigate the clinical and genetic features of PSEN1 variants in patients mainly manifested with hereditary spastic paraparesis (HSP)-like phenotypes.

Methods: Mutational analysis was performed in 242 unrelated Taiwanese patients with clinically suspected HSP using a targeted resequencing panel covering the entire coding regions of PSEN1, along with 76 genes associated with HSP and 55 genes linked to HSP-like phenotypes.

Results: Two of the 242 patients (0.8%) were found to carry the pathogenic PSEN1 variants (p.P284S and p.F386S). In addition to the two probands, six affected family members were further identified to have the pathogenic PSEN1 variants. Six of these eight patients (75%) presented with spastic paraparesis as their initial symptom, one suffered from cognitive decline, and another manifested with personality change. The average age of symptom onset was 40.1 ± 4.8 years. Except for one patient, cognitive decline developed in all subjects before the last follow-up. For the patient carrying the PSEN1 p.P284S variant, amyloid deposition in bilateral lateral temporal, frontal, precuneus, and parietal regions was evident by amyloid PET, but no hippocampus atrophy was found on brain MRI. For the three patients carrying the PSEN1 p.F386S variant, brain atrophy with dilated ventricles were noted in the patient initially presented with personality changes, but normal MRI findings in the other two patients manifested with spastic paraparesis.

Conclusions: Spastic paraparesis can be the initial and isolated clinical presentation of PSEN1 mutations. We identified eight patients from two families carrying a pathogenic PSEN1 variant, all but one carriers have developed cognitive symptoms. PSEN1 related spastic paraparesis usually has a later age of onset compared to other common hereditary spastic paraparesis subtypes, and the family history of early onset dementia might be obscure. Our findings suggested that PSEN1 variants are a rare cause of spastic paraparesis but should be considered especially in those with a later age of onset.

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携带PSEN1突变的个体早期表现为痉挛性麻痹：临床和遗传分析。

背景：早老素1基因（PSEN1）突变是众所周知的早发性家族性阿尔茨海默病的原因，但它们也可以表现为非典型表型，如纯粹的痉挛性麻痹。本研究旨在探讨PSEN1变异在主要表现为遗传性痉挛性截瘫（HSP）样表型的患者中的临床和遗传特征。方法：对242例台湾临床疑似热休克患者进行突变分析，使用靶向重测序面板覆盖PSEN1的整个编码区，以及76个与热休克相关的基因和55个与热休克样表型相关的基因。结果：242例患者中2例（0.8%）携带PSEN1致病性变异（p.P284S和p.F386S）。除2名先证者外，6名受影响的家庭成员被进一步鉴定为具有致病性PSEN1变异。8例患者中有6例（75%）以痉挛性麻痹为首发症状，1例表现为认知能力下降，另1例表现为人格改变。平均发病年龄为40.1±4.8岁。除一名患者外，所有受试者在最后一次随访前均出现认知能力下降。对于携带PSEN1 p.P284S变异的患者，淀粉样蛋白PET显示双侧颞外侧、额叶、楔前叶和顶叶区有明显的淀粉样蛋白沉积，但脑MRI未发现海马萎缩。对于携带PSEN1 p.F386S变异的三名患者，在最初表现为人格改变的患者中发现脑萎缩和心室扩张，但其他两名患者的MRI检查结果正常，表现为痉挛性截瘫。结论：痉挛性麻痹可能是PSEN1突变的初始和孤立的临床表现。我们从两个家族中确定了8名携带致病性PSEN1变异的患者，除1名携带者外，其他携带者均出现认知症状。与其他常见的遗传性痉挛性截瘫亚型相比，PSEN1相关的痉挛性截瘫的发病年龄通常较晚，早发性痴呆的家族史可能不清楚。我们的研究结果表明，PSEN1变异是痉挛性截瘫的罕见原因，但在发病年龄较晚的患者中应特别考虑。

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

Alzheimer's Research & Therapy 医学-神经病学

CiteScore

13.10

自引率

3.30%

发文量

172

审稿时长

>12 weeks

期刊介绍： Alzheimer's Research & Therapy is an international peer-reviewed journal that focuses on translational research into Alzheimer's disease and other neurodegenerative diseases. It publishes open-access basic research, clinical trials, drug discovery and development studies, and epidemiologic studies. The journal also includes reviews, viewpoints, commentaries, debates, and reports. All articles published in Alzheimer's Research & Therapy are included in several reputable databases such as CAS, Current contents, DOAJ, Embase, Journal Citation Reports/Science Edition, MEDLINE, PubMed, PubMed Central, Science Citation Index Expanded (Web of Science) and Scopus.