对临床诊断为阿尔茨海默病和额颞叶痴呆的中国患者中NOTCH3变异体的分析。
Analyses of NOTCH3 variants in Chinese patients with clinically diagnosed Alzheimer's disease and frontotemporal dementia.
作者信息
Nan Haitian, Chu Min, Yue Ailing, He Qianqian, Li Jieying, Liu Yanchen, Chi Lijun, Liu Xiaoyan, Peng Guoping, Wu Liyong
机构信息
Department of Neurology, Xuanwu Hospital, Capital Medical University, 45 Changchun Street, Beijing, 100053, China.
Sichuan Provincial Center for Mental Health, Sichuan Provincial People's Hospital, School of Medicine, University of Electronic Science and Technology of China, Chengdu, 610072, China.
出版信息
Alzheimers Res Ther. 2025 Aug 9;17(1):186. doi: 10.1186/s13195-025-01836-1.
BACKGROUND
A pathogenic variant in the NOTCH3 gene has been identified as the cause of cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL). Studies focusing on variants in NOTCH3 in Alzheimer's disease (AD) and frontotemporal dementia (FTD) cohorts have been limited. We aim to screen clinically diagnosed AD and FTD patients with unknown etiology for pathogenic variants in NOTCH3 in the Chinese population.
METHODS
This study included early-onset AD and FTD patients consecutively recruited from Xuanwu Hospital. We performed the whole exome sequencing of genomic DNA from the patients screened for rare, nonsynonymous, predicted deleterious NOTCH3 variants. The clinical characteristics of dementia patients with likely pathogenic NOTCH3 variants were described in detail.
RESULTS
Three hundred four AD and 261 FTD patients were screened for variants in the NOTCH3 gene. Four cysteine-altering NOTCH3 variants-c.1630C > T,p.(R544C); c.1672C > T,p.(R558C); c.1759C > T,p.(R587C); and c.1918C > T,p.(R640C)-were identified as likely pathogenic variants according to ACMG guidelines. All four patients with cysteine-altering variants were clinically diagnosed with AD or FTD and presented with characteristic clinical manifestations and neuroimaging profiles. Notably, they also showed mild periventricular and deep white matter signal changes on neuroimaging. Our study showed a 0.7% (4/565) occurrence of NOTCH3 pathogenic variants in Chinese early-onset dementia patients.
CONCLUSIONS
Our findings expand the mutational and phenotypic spectrum associated with NOTCH3. NOTCH3 pathogenic variants are present in clinically diagnosed AD and FTD patients. However, the absence of biomarkers to confirm AD or FTD diagnoses limits the interpretation of whether these cases represent comorbid conditions or phenotypic overlaps with CADASIL. Clinical identification of dementia patients with these variants at an early stage is challenging.
背景
NOTCH3基因的致病性变异已被确定为伴有皮质下梗死和白质脑病的常染色体显性遗传性脑动脉病(CADASIL)的病因。针对阿尔茨海默病(AD)和额颞叶痴呆(FTD)队列中NOTCH3变异的研究有限。我们旨在筛查中国人群中病因不明的临床诊断AD和FTD患者的NOTCH3致病性变异。
方法
本研究纳入了连续从宣武医院招募的早发性AD和FTD患者。我们对筛选出的罕见、非同义、预测有害的NOTCH3变异的患者基因组DNA进行了全外显子组测序。详细描述了可能具有致病性NOTCH3变异的痴呆患者的临床特征。
结果
对304例AD患者和261例FTD患者进行了NOTCH3基因变异筛查。根据美国医学遗传学与基因组学学会(ACMG)指南,四个改变半胱氨酸的NOTCH3变异——c.1630C>T,p.(R544C);c.1672C>T,p.(R558C);c.1759C>T,p.(R587C);和c.1918C>T,p.(R640C)——被确定为可能的致病性变异。所有四名具有改变半胱氨酸变异的患者均被临床诊断为AD或FTD,并表现出特征性的临床表现和神经影像学特征。值得注意的是,他们在神经影像学上还表现出轻度的脑室周围和深部白质信号改变。我们的研究显示,中国早发性痴呆患者中NOTCH�致病性变异的发生率为0.7%(4/565)。
结论
我们的研究结果扩展了与NOTCH3相关的突变和表型谱。NOTCH3致病性变异存在于临床诊断的AD和FTD患者中。然而,缺乏确认AD或FTD诊断的生物标志物限制了对这些病例是代表合并症还是与CADASIL表型重叠的解释。在早期临床识别这些变异的痴呆患者具有挑战性。
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