Fang Shih-Yu, Hsiao Cheng-Tsung, Jih Kang-Yang, Tsai Yu-Sheun, Lai Kuan-Lin, Chou Cheng-Ta, Liao Yi-Chu, Lee Yi-Chung
Department of Neurology, Taipei Veterans General Hospital, Taipei, Taiwan, ROC.
Department of Neurology, National Yang Ming Chiao Tung University of Medicine, Taipei, Taiwan, ROC.
Ann Clin Transl Neurol. 2025 Jan;12(1):158-168. doi: 10.1002/acn3.52265. Epub 2024 Dec 3.
The genetic causes of a significant number of patients with cerebellar ataxia remain unsolved. Variations in the ITM2B gene, typically linked to dominantly inherited dementia, can sometimes present with cerebellar ataxia as an early symptom. This study aims to investigate the role of ITM2B variations in a Taiwanese cohort with unsolved cerebellar ataxia.
Genetic analysis of ITM2B was performed in 212 unrelated Taiwanese patients with unsolved cerebellar ataxia. Eight short tandem repeat markers flanking ITM2B were genotyped to analyze the associated haplotype. Affected carriers underwent comprehensive clinical evaluations.
A heterozygous ITM2B variant, c.800G>T (p.(Ter267LeuextTer11)), was identified in three patients. Haplotype analysis demonstrated a shared haplotype linked to this variant in the three families, suggesting a founder effect. The three probands and additional three affected relatives presented with cerebellar ataxia and unsteady gait with an average onset age of 43.2 years. Most participants had no cognitive impairment at symptom onset but experienced memory decline, oculomotor disturbances, lower limb spasticity, and extensor plantar responses within 2-5 years. Magnetic resonance imaging and spectroscopy revealed progressive extension of white matter hyperintensity over periventricular and subcortical regions, subtle hippocampal atrophy, preserved cerebellar volumes, and decreased N-acetylaspartate/creatine ratio over the vermis.
ITM2B mutations accounted for 1.4% of cerebellar ataxia cases in the Taiwanese cohort, with patients carrying ITM2B c.800G>T descending from a common ancestor. This study underscores the importance of considering ITM2B variations as a potential cause of cerebellar ataxia, even in the absence of dementia at the initial presentation.
相当一部分小脑性共济失调患者的遗传病因仍未明确。ITM2B基因变异通常与显性遗传性痴呆相关,有时也会以小脑性共济失调作为早期症状出现。本研究旨在调查ITM2B基因变异在一组病因未明的台湾小脑性共济失调患者中的作用。
对212名无亲缘关系的台湾小脑性共济失调病因未明患者进行ITM2B基因分析。对ITM2B侧翼的8个短串联重复序列标记进行基因分型,以分析相关单倍型。对受影响的携带者进行全面的临床评估。
在3名患者中鉴定出一种杂合的ITM2B变异,即c.800G>T(p.(Ter267LeuextTer11))。单倍型分析显示这三个家族中存在与该变异相关的共享单倍型,提示存在奠基者效应。三名先证者和另外三名受影响的亲属表现为小脑性共济失调和步态不稳,平均发病年龄为43.2岁。大多数参与者在症状出现时没有认知障碍,但在2至5年内出现了记忆力下降、眼球运动障碍、下肢痉挛和跖伸反应。磁共振成像和波谱分析显示,脑室周围和皮质下区域的白质高信号逐渐扩展,海马轻度萎缩,小脑体积保留,蚓部N-乙酰天门冬氨酸/肌酸比值降低。
在台湾队列中,ITM2B突变占小脑性共济失调病例的1.4%,携带ITM2B c.800G>T变异的患者来自共同祖先。本研究强调了即使在初始表现时没有痴呆,也应将ITM2B变异视为小脑性共济失调潜在病因的重要性。
