基于 AICD 的 APP 代谢调控因子功能筛选。

An AICD-based functional screen to identify APP metabolism regulators.

机构信息

Department of Bioscience & Biotechnology, Drexel University, Philadelphia, PA, USA.

出版信息

Mol Neurodegener. 2007 Aug 24;2:15. doi: 10.1186/1750-1326-2-15.

DOI:10.1186/1750-1326-2-15

PMID:17718916

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2071909/

Abstract

BACKGROUND

A central event in Alzheimer's disease (AD) is the regulated intramembraneous proteolysis of the beta-amyloid precursor protein (APP), to generate the beta-amyloid (Abeta) peptide and the APP intracellular domain (AICD). Abeta is the major component of amyloid plaques and AICD displays transcriptional activation properties. We have taken advantage of AICD transactivation properties to develop a genetic screen to identify regulators of APP metabolism. This screen relies on an APP-Gal4 fusion protein, which upon normal proteolysis, produces AICD-Gal4. Production of AICD-Gal4 induces Gal4-UAS driven luciferase expression. Therefore, when regulators of APP metabolism are modulated, luciferase expression is altered.

RESULTS

To validate this experimental approach we modulated alpha-, beta-, and gamma-secretase levels and activities. Changes in AICD-Gal4 levels as measured by Western blot analysis were strongly and significantly correlated to the observed changes in AICD-Gal4 mediated luciferase activity. To determine if a known regulator of APP trafficking/maturation and Presenilin1 endoproteolysis could be detected using the AICD-Gal4 mediated luciferase assay, we knocked-down Ubiquilin 1 and observed decreased luciferase activity. We confirmed that Ubiquilin 1 modulated AICD-Gal4 levels by Western blot analysis and also observed that Ubiquilin 1 modulated total APP levels, the ratio of mature to immature APP, as well as PS1 endoproteolysis.

CONCLUSION

Taken together, we have shown that this screen can identify known APP metabolism regulators that control proteolysis, intracellular trafficking, maturation and levels of APP and its proteolytic products. We demonstrate for the first time that Ubiquilin 1 regulates APP metabolism in the human neuroblastoma cell line, SH-SY5Y.

摘要

背景

阿尔茨海默病（AD）的一个核心事件是β淀粉样前体蛋白（APP）的调节性跨膜蛋白水解，生成β淀粉样肽（Abeta）和 APP 细胞内结构域（AICD）。Abeta 是淀粉样斑块的主要成分，AICD 显示转录激活特性。我们利用 AICD 的转录激活特性开发了一种遗传筛选方法，以鉴定 APP 代谢的调节剂。该筛选依赖于 APP-Gal4 融合蛋白，该融合蛋白在正常蛋白水解时产生 AICD-Gal4。AICD-Gal4 的产生诱导 Gal4-UAS 驱动的荧光素酶表达。因此，当调节 APP 代谢的调节剂发生变化时，荧光素酶表达会发生变化。

结果

为了验证这种实验方法，我们调节了α-、β-和 γ-分泌酶的水平和活性。Western blot 分析测量的 AICD-Gal4 水平的变化与观察到的 AICD-Gal4 介导的荧光素酶活性的变化强烈且显著相关。为了确定是否可以使用 AICD-Gal4 介导的荧光素酶测定法检测已知的 APP 运输/成熟和 Presenilin1 内切酶的调节剂，我们敲低了泛素连接酶 1（Ubiquilin 1），并观察到荧光素酶活性降低。我们通过 Western blot 分析证实 Ubiquilin 1 调节 AICD-Gal4 水平，并且还观察到 Ubiquilin 1 调节总 APP 水平、成熟与不成熟 APP 的比例以及 PS1 内切酶切。

结论

总之，我们已经表明，该筛选可以鉴定已知的 APP 代谢调节剂，这些调节剂控制蛋白水解、细胞内运输、成熟以及 APP 及其蛋白水解产物的水平。我们首次证明泛素连接酶 1（Ubiquilin 1）在人神经母细胞瘤细胞系 SH-SY5Y 中调节 APP 代谢。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c05c/2071909/847bb272407c/1750-1326-2-15-1.jpg

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基于 AICD 的 APP 代谢调控因子功能筛选。

An AICD-based functional screen to identify APP metabolism regulators.

机构信息

Department of Bioscience & Biotechnology, Drexel University, Philadelphia, PA, USA.