CADASIL队列中血管性NOTCH3聚集与疾病严重程度的关联——对NOTCH3特异性疾病预测的启示

Association Between Vascular NOTCH3 Aggregation and Disease Severity in a CADASIL Cohort - Implications for NOTCH3 Variant-Specific Disease Prediction.

作者信息

Cerfontaine Minne N, Gravesteijn Gido, Hack Remco J, Dijkstra Kyra L, Rodríguez-Girondo Mar, Gesierich Benno, Witjes-Ané Marie-Noëlle W, van Doorn Remco, Duering Marco, Rutten Julie W, Lesnik Oberstein Saskia A J

机构信息

Department of Clinical Genetics, Leiden University Medical Center, Leiden, The Netherlands.

Department of Pathology, Leiden University Medical Center, Leiden, The Netherlands.

出版信息

Ann Neurol. 2025 Aug;98(2):273-285. doi: 10.1002/ana.27240. Epub 2025 Apr 23.

DOI:10.1002/ana.27240

PMID:40265482

Abstract

OBJECTIVE

Vascular NOTCH3 protein ectodomain aggregation is a pathological hallmark of cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL), a monogenic small vessel disease typically caused by cysteine-altering variants in NOTCH3. Given their high population frequency, these NOTCH3 variants are an important genetic contributor to stroke and vascular dementia worldwide. Disease severity in CADASIL is highly variable and is mainly determined by the position of the pathogenic NOTCH3 variant in the NOTCH3 ectodomain. Here, we aimed to investigate the association between NOTCH3 aggregation load in skin vessels, cysteine-altering NOTCH3 variants, and disease severity in a prospective cohort study of 212 patients with CADASIL with 39 distinct cysteine-altering NOTCH3 variants.

METHODS

NOTCH3 aggregation load in skin vessels was determined by calculating the NOTCH3 score; the fraction of skin vessel wall area positive for NOTCH3 staining. Variant-specific NOTCH3 scores were calculated for variants present in 10 or more participants, by averaging the NOTCH3 scores of individuals with that distinct variant. The associations between the NOTCH3 score, NOTCH3 variants, and neuroimaging and clinical outcomes were investigated using multivariable linear mixed models, Cox regression, and mediation analyses.

RESULTS

The NOTCH3 score was significantly associated with lifetime stroke probability and small vessel disease neuroimaging outcomes, but not with age. Variant-specific NOTCH3 scores reflected differences in disease severity associated with distinct NOTCH3 variants.

INTERPRETATION

These findings suggest that differences in NOTCH3 aggregation propensity underlie the differences in disease severity associated with NOTCH3 cysteine-altering variants, and show that NOTCH3-variant specific NOTCH3 scores can contribute to improved individualized disease prediction in CADASIL. ANN NEUROL 2025;98:273-285.

摘要

目的

血管性NOTCH3蛋白胞外结构域聚集是伴有皮质下梗死和白质脑病的大脑常染色体显性动脉病（CADASIL）的病理标志，CADASIL是一种单基因小血管疾病，通常由NOTCH3中改变半胱氨酸的变异引起。鉴于这些NOTCH3变异在人群中的高频率，它们是全球范围内中风和血管性痴呆的重要遗传因素。CADASIL的疾病严重程度高度可变，主要由致病性NOTCH3变异在NOTCH3胞外结构域中的位置决定。在此，我们旨在通过对212例患有39种不同的改变半胱氨酸的NOTCH3变异的CADASIL患者进行前瞻性队列研究，调查皮肤血管中NOTCH3聚集负荷、改变半胱氨酸的NOTCH3变异与疾病严重程度之间的关联。

方法

通过计算NOTCH3评分来确定皮肤血管中的NOTCH3聚集负荷；NOTCH3染色阳性的皮肤血管壁面积分数。对于10名或更多参与者中存在的变异，通过平均具有该独特变异的个体的NOTCH3评分来计算变异特异性NOTCH3评分。使用多变量线性混合模型、Cox回归和中介分析来研究NOTCH3评分、NOTCH3变异与神经影像学和临床结果之间的关联。