Increased localization of APP-C99 in mitochondria-associated ER
membranes causes mitochondrial dysfunction in Alzheimer disease

Acin-Perez, Rebeca; Agrawal, Rishi R; Area-Gomez, Estela; Chan, Robin B.; Di Paolo, Gilbert; Enriquez, José Antonio; Freyberg, Zachary Z.; Guardia-Laguarta, Cristina; Larrea, Delfina; Macaluso, Frank P.; Mehler, Mark F.; Montesinos, Jorge; Pera, Marta; Perumal, Geoffrey S.; Schon, Eric A.; Velasco, Kevin R.; Xu, Yimeng

Increased localization of APP-C99 in mitochondria-associated ER membranes causes mitochondrial dysfunction in Alzheimer disease

Authors: Rebeca Acin-Perez
Rishi R Agrawal
Estela Area-Gomez
Robin B. Chan
Gilbert Di Paolo
José Antonio Enriquez
Zachary Z. Freyberg
Cristina Guardia-Laguarta
Delfina Larrea
Frank P. Macaluso
Mark F. Mehler
Jorge Montesinos
Marta Pera
Geoffrey S. Perumal
Eric A. Schon
Kevin R. Velasco
Yimeng Xu
Publication date: 1 January 2017
Publisher: 'EMBO'
Doi

Abstract

In the amyloidogenic pathway associated with Alzheimer disease (AD), the amyloid precursor protein (APP) is cleaved by beta-secretase to generate a 99-aa C-terminal fragment (C99) that is then cleaved by c-secretase to generate the beta-amyloid (Ab) found in senile plaques. In previous reports, we and others have shown that c-secretase activity is enriched in mitochondria-associated endoplasmic reticulum (ER) membranes (MAM) and that ER-mitochondrial connectivity and MAM function are upregulated in AD. We now show that C99, in addition to its localization in endosomes, can also be found in MAM, where it is normally processed rapidly by c-secretase. In cell models of AD, however, the concentration of unprocessed C99 increases in MAM regions, resulting in elevated sphingolipid turnover and an altered lipid composition of both MAM and mitochondrial membranes. In turn, this change in mitochondrial membrane composition interferes with the proper assembly and activity of mitochondrial respiratory supercomplexes, thereby likely contributing to the bioenergetic defects characteristic of AD.We thank Drs. Orian Shirihai and Marc Liesa (UCLA) for assistance with the Seahorse measurements, Dr. Huaxi Xu (Sanford Burnham Institute) for the APP-DKO MEFs and Dr. Mark Mattson (NIH) for the PS1 knock-in mice, Drs. Arancio and Teich for the APP-KO mice tissues used in these studies, Dr. Hua Yang (Columbia University) for mouse husbandry, and Drs. Marc Tambini, Ira Tabas, and Serge Przedborski for helpful comments. This work was supported by the Fundacion Alfonso Martin Escudero (to M.P.); the Alzheimer's Drug Discovery Foundation, the Ellison Medical Foundation, the Muscular Dystrophy Association, the U.S. Department of Defense W911NF-12-1-9159 and W911F-15-1-0169), and the J. Willard and Alice S. Marriott Foundation (to E.A.S.); the U.S. National Institutes of Health (P01-HD080642 and P01-HD032062 to E.A.S.; NS071571 and HD071593 to M.F.M.; R01-NS056049 and P50-AG008702 to G.D.P.; 1S10OD016214-01A1 to G.S.P. and F.P.M, and K01-AG045335 to E.A.-G.), the Lucien Cote Early Investigator Award in Clinical Genetics from the Parkinson's Disease Foundation (PDF-CEI-1364 and PDF-CEI-1240) to C.G.-L., and National Defense Science and Engineering Graduate Fellowship (FA9550-11-C-0028) to R.R.A.S