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  4. The Role of γ-Secretase Activating Protein (GSAP) and Imatinib in the Regulation of γ-Secretase Activity and Amyloid-β Generation
 
research article

The Role of γ-Secretase Activating Protein (GSAP) and Imatinib in the Regulation of γ-Secretase Activity and Amyloid-β Generation

Hussain, Ishrut
•
Fabrègue, Julien
•
Anderes, Laurence
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2013
Journal of Biological Chemistry

gamma-Secretase is a large enzyme complex comprising presenilin, nicastrin, presenilin enhancer 2, and anterior pharynx-defective 1 that mediates the intramembrane proteolysis of a large number of proteins including amyloid precursor protein and Notch. Recently, a novel gamma-secretase activating protein (GSAP) was identified that interacts with gamma-secretase and the C-terminal fragment of amyloid precursor protein to selectively increase amyloid-beta production. In this study we have further characterized the role of endogenous and exogenous GSAP in the regulation of gamma-secretase activity and amyloid-beta production in vitro. Knockdown of GSAP expression in N2a cells decreased amyloid-beta levels. In contrast, overexpression of GSAP in HEK cells expressing amyloid precursor protein or in N2a cells had no overt effect on amyloid-beta generation. Likewise, purified recombinant GSAP had no effect on amyloid-beta generation in two distinct in vitro gamma-secretase assays. In subsequent cellular studies with imatinib, a kinase inhibitor that reportedly prevents the interaction of GSAP with the C-terminal fragment of amyloid precursor protein, a concentration-dependent decrease in amyloid-beta levels was observed. However, no interaction between GSAP and the C-terminal fragment of amyloid precursor protein was evident in co-immunoprecipitation studies. In addition, subchronic administration of imatinib to rats had no effect on brain amyloid-beta levels. In summary, these findings suggest the roles of GSAP and imatinib in the regulation of gamma-secretase activity and amyloid-beta generation are uncertain.

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Type
research article
DOI
10.1074/jbc.M112.370924
PubMed ID

23209290

Author(s)
Hussain, Ishrut
Fabrègue, Julien
Anderes, Laurence
Ousson, Solenne
Borlat, Frédéric
Eligert, Valérie
Berger, Sébastien
Dimitrov, Mitko
Alattia, Jean-René
Fraering, Patrick C.
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Date Issued

2013

Published in
Journal of Biological Chemistry
Volume

288

Issue

4

Start page

2521

End page

2531

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
CMSN  
Available on Infoscience
February 20, 2013
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/88984
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