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在哺乳动物中,Nicastrin是早老素/γ-分泌酶复合物组装以介导Notch信号传导以及β-淀粉样前体蛋白加工和运输所必需的。

Nicastrin is required for assembly of presenilin/gamma-secretase complexes to mediate Notch signaling and for processing and trafficking of beta-amyloid precursor protein in mammals.

作者信息

Li Tong, Ma Guojun, Cai Huaibin, Price Donald L, Wong Philip C

机构信息

Department of Pathology, The Johns Hopkins University School of Medicine, Baltimore, Maryland 21205-2196, USA.

出版信息

J Neurosci. 2003 Apr 15;23(8):3272-7. doi: 10.1523/JNEUROSCI.23-08-03272.2003.

Abstract

Recent studies indicate that nicastrin (NCT) and presenilins form functional components of a multimeric gamma-secretase complex required for the regulated intramembraneous proteolysis of Notch and beta-amyloid (Abeta) precursor protein (APP). To determine whether nicastrin is required for proteolytic processing of Notch and APP in mammals and the role of nicastrin in presenilin/gamma-secretase complex assembly, we generated nicastrin-deficient (NCT-/-) mice and derived fibroblasts from NCT-/- embryos. Nicastrin-null embryos died by embryonic day 10.5 and exhibited several patterning defects, including abnormal somite segmentation, phenotypes that are reminiscent of embryos lacking Notch1 or both presenilins. Importantly, secretion of Abeta peptides is abolished in NCT-/- fibroblasts, whereas it is reduced by approximately 50% in NCT+/- cells; the failure to generate Abeta peptides in NCT-/- cells is accompanied by destabilization of the presenilin/gamma-secretase complex and accumulation of APP-C-terminal fragments. Moreover, APP trafficking analysis in NCT-/- fibroblasts revealed a significant delay in the rate of APP reinternalization compared with that of control cells. Together, these results establish that nicastrin is an essential component of the multimeric gamma-secretase complex in mammals required for both gamma-secretase activity and APP trafficking and suggest that nicastrin may be a valuable therapeutic target for Alzheimer's disease.

摘要

近期研究表明,尼卡斯特林(NCT)和早老素形成了多聚体γ-分泌酶复合物的功能组件,该复合物是Notch和β-淀粉样蛋白(Aβ)前体蛋白(APP)进行膜内蛋白水解调控所必需的。为了确定尼卡斯特林在哺乳动物中对Notch和APP的蛋白水解加工是否必需,以及尼卡斯特林在早老素/γ-分泌酶复合物组装中的作用,我们构建了尼卡斯特林缺陷型(NCT-/-)小鼠,并从NCT-/-胚胎中获得了成纤维细胞。尼卡斯特林缺失的胚胎在胚胎第10.5天死亡,并表现出多种模式缺陷,包括体节分割异常,这些表型让人联想到缺乏Notch1或同时缺乏两种早老素的胚胎。重要的是,NCT-/-成纤维细胞中Aβ肽的分泌被消除,而在NCT+/-细胞中分泌减少了约50%;NCT-/-细胞中无法产生Aβ肽伴随着早老素/γ-分泌酶复合物的不稳定和APP C末端片段的积累。此外,对NCT-/-成纤维细胞的APP转运分析显示,与对照细胞相比,APP再内化速率显著延迟。总之,这些结果表明尼卡斯特林是哺乳动物中多聚体γ-分泌酶复合物的必需成分,对γ-分泌酶活性和APP转运均不可或缺,并提示尼卡斯特林可能是阿尔茨海默病的一个有价值的治疗靶点。

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