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在淀粉样前体蛋白跨膜结构域的蛋白水解加工过程中,γ-切割依赖于ζ-切割。

gamma-Cleavage is dependent on zeta-cleavage during the proteolytic processing of amyloid precursor protein within its transmembrane domain.

作者信息

Zhao Guojun, Cui Mei-Zhen, Mao Guozhang, Dong Yunzhou, Tan Jianxin, Sun Longsheng, Xu Xuemin

机构信息

Department of Pathobiology, College of Veterinary Medicine, the University of Tennessee, Knoxville, 37996, USA.

出版信息

J Biol Chem. 2005 Nov 11;280(45):37689-97. doi: 10.1074/jbc.M507993200. Epub 2005 Sep 12.

Abstract

beta-Amyloid precursor protein apparently undergoes at least three major cleavages, gamma-, epsilon-, and the newly identified zeta-cleavage, within its transmembrane domain to produce secreted beta-amyloid protein (Abeta). However, the roles of epsilon- and zeta-cleavages in the formation of secreted Abeta and the relationship among these three cleavages, namely epsilon-, zeta-, and gamma-cleavages, remain elusive. We investigated these issues by attempting to determine the formation and turnover of the intermediate products generated by these cleavages, in the presence or absence of known gamma-secretase inhibitors. By using a differential inhibition strategy, our data demonstrate that Abeta(46) is an intermediate precursor of secreted Abeta. Our co-immunoprecipitation data also reveal that, as an intermediate, Abeta(46) is tightly associated with presenilin in intact cells. Furthermore, we identified a long Abeta species that is most likely the long sought after intermediate product, Abeta(49), generated by epsilon-cleavage, and this Abeta(49) is further processed by zeta- and gamma-cleavages to generate Abeta(46) and ultimately the secreted Abeta(40/42). More interestingly, our data demonstrate that gamma-cleavage not only occurs last but also depends on zeta-cleavage occurring prior to it, indicating that zeta-cleavage is crucial for the formation of secreted Abeta. Thus, we conclude that the C terminus of secreted Abeta is most likely generated by a series of sequential cleavages, namely first epsilon-cleavage which is then followed by zeta- and gamma-cleavages, and that Abeta(46) produced by zeta-cleavage is the precursor of secreted Abeta(40/42).

摘要

β-淀粉样前体蛋白显然在其跨膜结构域内至少经历三种主要切割,即γ-、ε-和新发现的ζ-切割,以产生分泌型β-淀粉样蛋白(Aβ)。然而,ε-和ζ-切割在分泌型Aβ形成中的作用以及这三种切割(即ε-、ζ-和γ-切割)之间的关系仍然不清楚。我们通过试图确定在存在或不存在已知γ-分泌酶抑制剂的情况下,这些切割产生的中间产物的形成和周转来研究这些问题。通过使用差异抑制策略,我们的数据表明Aβ(46)是分泌型Aβ的中间前体。我们的共免疫沉淀数据还显示,作为一种中间体,Aβ(46)在完整细胞中与早老素紧密相关。此外,我们鉴定出一种长链Aβ物种,它很可能是长期以来寻找的由ε-切割产生的中间产物Aβ(49),并且这种Aβ(49)进一步被ζ-和γ-切割加工以产生Aβ(46)并最终产生分泌型Aβ(40/42)。更有趣的是,我们的数据表明γ-切割不仅最后发生,而且取决于其之前发生的ζ-切割,这表明ζ-切割对于分泌型Aβ的形成至关重要。因此,我们得出结论:分泌型Aβ的C末端很可能是由一系列顺序切割产生的,即首先是ε-切割,然后是ζ-和γ-切割,并且由ζ-切割产生的Aβ(46)是分泌型Aβ(40/42)的前体。

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