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成熟糖基化的尼卡斯特林水平受到调控,并与淀粉样前体蛋白的γ-分泌酶加工过程相关。

The levels of mature glycosylated nicastrin are regulated and correlate with gamma-secretase processing of amyloid beta-precursor protein.

作者信息

Arawaka Shigeki, Hasegawa Hiroshi, Tandon Anurag, Janus Christopher, Chen Fusheng, Yu Gang, Kikuchi Kenji, Koyama Shingo, Kato Takeo, Fraser Paul E, St George-Hyslop Peter

机构信息

Centre for Research in Neurodegenerative Diseases, Tanz Neuroscience Building, University of Toronto, Toronto, Ontario, Canada.

出版信息

J Neurochem. 2002 Dec;83(5):1065-71. doi: 10.1046/j.1471-4159.2002.01207.x.

Abstract

Nicastrin, a type-I transmembrane glycoprotein, is a necessary component of the high molecular weight presenilin (PS) complexes that mediate intramembranous cleavage of beta-amyloid precursor protein (betaAPP) and Notch. Nicastrin undergoes trafficking-dependent glycosylation maturation, and PS1 interacts preferentially with these maturely glycosylated forms of nicastrin. We investigated the effects of differing levels of the immature and mature endoglycosidase-H-resistant forms of nicastrin on Abeta40- and Abeta42-peptide secretion in several cell lines stably expressing a mutant nicastrin (D336A/Y337A) that increases Abeta secretion. There was no correlation between Abeta secretion and the level of over-expression of the immature forms of nicastrin. The total level of mature nicastrin remained constant, but mutant nicastrin replaced endogenous mature nicastrin in varying degrees. Differences in the levels of mature mutant nicastrin positively correlated with Abeta secretion, but did not influence either betaAPP trafficking or processing by alpha- and beta-secretases. Proper trafficking and terminal maturation of nicastrin is therefore a necessary event for the regulated intramembranous proteolysis of betaAPP.

摘要

尼卡斯特林是一种I型跨膜糖蛋白,是高分子量早老素(PS)复合物的必要组成部分,该复合物介导β-淀粉样前体蛋白(βAPP)和Notch的膜内裂解。尼卡斯特林经历依赖于运输的糖基化成熟过程,并且早老素1(PS1)优先与这些糖基化成熟形式的尼卡斯特林相互作用。我们研究了不同水平的未成熟和成熟的对内切糖苷酶-H有抗性的尼卡斯特林对几种稳定表达增加β淀粉样蛋白(Aβ)分泌的突变型尼卡斯特林(D336A/Y337A)的细胞系中Aβ40和Aβ42肽分泌的影响。Aβ分泌与未成熟形式的尼卡斯特林的过表达水平之间没有相关性。成熟尼卡斯特林的总水平保持恒定,但突变型尼卡斯特林在不同程度上取代了内源性成熟尼卡斯特林。成熟突变型尼卡斯特林水平的差异与Aβ分泌呈正相关,但不影响βAPP的运输或α-和β-分泌酶的加工。因此,尼卡斯特林的正确运输和终末成熟是βAPP膜内蛋白水解调控的必要事件。

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