Vesalius Research Center, Flanders Institute for Biotechnology (VIB), Leuven, Belgium.
Arterioscler Thromb Vasc Biol. 2011 Dec;31(12):2881-8. doi: 10.1161/ATVBAHA.111.237859. Epub 2011 Sep 22.
Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL) is an adult-onset neurovascular disorder caused by stereotyped mutations in the NOTCH3 receptor. Elucidation of its pathobiology is still incomplete and remains a challenge, in part because the available preclinical mouse models to date do not reproduce the full spectrum of CADASIL pathology and clinical disease.
Here, we report a novel knock-in mouse with Arg170Cys substitution in murine Notch3, corresponding to the prevalent Arg169Cys substitution in CADASIL. The Notch3(Arg170Cys) mice displayed late-onset, dominant CADASIL arteriopathy with typical granular osmiophilic material deposition and developed brain histopathology including thrombosis, microbleeds, gliosis, and microinfarction. Furthermore, Notch3(Arg170Cys) mice experienced neurological symptoms with motor defects such as staggering gait and limb paresis.
This model, for the first time, phenocopies the arteriopathy and the histopathologic as well as clinical features of CADASIL and may offer novel opportunities to investigate disease pathogenesis.
伴皮质下梗死和白质脑病的脑常染色体显性遗传性动脉病(CADASIL)是一种由 NOTCH3 受体的定型突变引起的成年发病的神经血管疾病。其发病机制的阐明仍不完全,这仍然是一个挑战,部分原因是迄今为止可用的临床前小鼠模型不能复制 CADASIL 病理学和临床疾病的全部范围。
在这里,我们报告了一种新型的 Notch3 基因在 Arg170Cys 位置发生替换的小鼠,与 CADASIL 中常见的 Arg169Cys 替换相对应。 Notch3(Arg170Cys) 小鼠表现出晚发性、显性 CADASIL 血管病,伴有典型的颗粒性亲脂性物质沉积,并发展出包括血栓形成、微出血、神经胶质增生和微梗死在内的脑组织病理学改变。此外, Notch3(Arg170Cys) 小鼠出现了神经症状,如蹒跚步态和肢体瘫痪等运动缺陷。
该模型首次模拟了 CADASIL 的血管病以及组织病理学和临床特征,可能为研究疾病发病机制提供新的机会。
