Abstract

The amyloid precursor protein (APR) is sequentially cleaved by BACE1 and PS/y-secretase to yield A(3. APLP2 undergoes similar processing, resulting in the production of an Ap-like peptide. We have recently identified a third substrate for BACE1 and PS/y-secretase activities, the (32-subunit ((32) of the voltage-gated sodium channel (Nav1). Nav1s are almost exclusively responsible for the rising phase of action potentials. Our preliminary data indicate that BACE1-/y-secretase-mediated processing of (32 regulates sodium channel function and both mRNA and protein levels of a NaJ a-subunit, Nav1.1, in neuronal cells and BACE1 transgenic mice. In AD patient brains with elevated BACE1 levels, we also found elevated (32 C-terminal fragments and Nav1.1 levels. Interestingly, increased incidence of epileptic seizures has been associated with AD, more frequently with familial forms AD caused by mutations in PS1. Mutations in both a- and (3- subunits of the Najs have been linked to epileptic symptoms, induced by both decreased and increased sodium channel activity resulting in an imbalance in sodium channel function. Therefore, altered BACE1/ysecretase- mediated cleavages may result in two separate AD-associated pathogenic events, changes in A(3 generation (toxic amyloid formation) and sodium channel malfunction (epileptic seizures). To define the factors regulating these cleavages, here we propose to address the hypothesis that novel binding proteins regulate the processing and metabolism of (32 and these may be shared by APP and/or APLP2. In these studies, we will primarily characterize (32 processing and metabolism since this protein is not as well characterized as APP. We will take advantage of APLP2 as a third BACE1/y-secretase substrate.
In Specific Aim 1 we identify novel binding partners for (32 and assess their functional significance in proteolytic processing of (32. If these interacting proteins are shared by APP or APLP2, we will also study whether they affect processing APP or APLP2 including A(3 generation.
Specific Aim 2 will characterize metabolic pathways of (32 regulating sodium channel function, and whether these are shared by APP and APLP2. Since all three proteins share localization to lipid rafts, we will analyze these in addition to all major subcellular compartments for the presence of BACE1/y-secretase substrates. We will assess the effect of newly identified binding partners on metabolic pathways of (32 and on sodium channel function in cell-based assays and in vivo. The effects of seizure-associated FAD mutations in PS1 on sodium channel levels and function will also be determined in cells and in vivo. Results from these experiments will uncover novel processing or metabolic pathways that may lead to therapeutic strategies aimed at reducing A(3 generation as well as normalizing membrane excitability in AD patients with epileptic symptoms. Lay language: We propose to understand aspects of how amyloid is formed in the brains of Alzheimer's patients and why some patients develop seizures. This information can help find therapies for Alzheimer's disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG015379-13
Application #
8127707
Study Section
Special Emphasis Panel (ZAG1)
Project Start
Project End
Budget Start
2010-09-01
Budget End
2011-08-31
Support Year
13
Fiscal Year
2010
Total Cost
$463,077
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
030811269
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Jorfi, Mehdi; D'Avanzo, Carla; Kim, Doo Yeon et al. (2018) Three-Dimensional Models of the Human Brain Development and Diseases. Adv Healthc Mater 7:
Hartmann, Stephanie; Zheng, Fang; Kyncl, Michele C et al. (2018) ?-Secretase BACE1 Promotes Surface Expression and Function of Kv3.4 at Hippocampal Mossy Fiber Synapses. J Neurosci 38:3480-3494
Norambuena, Andrés; Wallrabe, Horst; Cao, Rui et al. (2018) A novel lysosome-to-mitochondria signaling pathway disrupted by amyloid-? oligomers. EMBO J 37:
Funane, Tsukasa; Hou, Steven S; Zoltowska, Katarzyna Marta et al. (2018) Selective plane illumination microscopy (SPIM) with time-domain fluorescence lifetime imaging microscopy (FLIM) for volumetric measurement of cleared mouse brain samples. Rev Sci Instrum 89:053705
Zoltowska, Katarzyna Marta; Maesako, Masato; Meier, Joshua et al. (2018) Novel interaction between Alzheimer's disease-related protein presenilin 1 and glutamate transporter 1. Sci Rep 8:8718
Park, Joseph; Wetzel, Isaac; Marriott, Ian et al. (2018) A 3D human triculture system modeling neurodegeneration and neuroinflammation in Alzheimer's disease. Nat Neurosci 21:941-951
Chatila, Zena K; Kim, Eunhee; Berlé, Clara et al. (2018) BACE1 Regulates Proliferation and Neuronal Differentiation of Newborn Cells in the Adult Hippocampus in Mice. eNeuro 5:
Zoltowska, Katarzyna Marta; Berezovska, Oksana (2018) Dynamic Nature of presenilin1/?-Secretase: Implication for Alzheimer's Disease Pathogenesis. Mol Neurobiol 55:2275-2284
Jorfi, Mehdi; D'Avanzo, Carla; Tanzi, Rudolph E et al. (2018) Human Neurospheroid Arrays for In Vitro Studies of Alzheimer's Disease. Sci Rep 8:2450
Kara, Eleanna; Marks, Jordan D; Fan, Zhanyun et al. (2017) Isoform- and cell type-specific structure of apolipoprotein E lipoparticles as revealed by a novel Forster resonance energy transfer assay. J Biol Chem 292:14720-14729

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