Abstract

Alzheimer's Disease (AD) is thought to involve early synapse loss. Familial AD is most often caused by mutations in presenilins, which are the catalytic subunits of g-secretase. Inactivation of g-secretase in adult mice by conditional deletion of its presenilin or nicastrin subunits causes synaptic impairments followed by neurodegeneration, but the relation of the loss of g-secretase acitivity, the observed synaptic impairments, and the neurodegeneration is unclear, as is the connection between these processes and human AD. The present project will focus on clarifying the synaptic function of g-secretase in mature neurons and its relation to neurodegeneration, using mice as a model system. The project proposes four specific aims to address this overall goal. The first two specific aims will mechanistically characterize the synaptic impairments that are caused by g-secretase inactivation in young adult mice in vivo, and analyze their relation to the neurodegeneration that develops at a later stage after g-secretase inactivation. The third and fourth specific aim will then test the hypothesis that at least some of the synaptic functions of g-secretase that are impaired upon its inactivation may be mediated by g-secretase-dependent cleavage of presynaptic neurexins and postsynaptic neuroligins, which are trans-synaptic cell-adhesion molecules that bind to each other and act as master regulators of synaptic properties. Strikingly in this context, neurexins and neuroligins were shown previously to be substrates for g-secretase, were genetically linked to AD, and are arguably the most plausible mediators of g-secretase function at the synapse. To test the involvement of neurexins and neuroligins in the synaptic functions of g-secretase, the project will characterize the site and regulation of the g-secretase- dependent cleavage of neurexins and neuroligins, and probe the function of this cleavage using conditional knockout mice of these molecules. Moreover, the project will examine whether inactivation of neurexin- and/or neuroligin-cleavage promotes neurodegeneration. Viewed together, the experiments of this project will thus not only characterize the synaptic function of g-secretase and its relation to neurodegeneration, but also determine whether the synaptic function of g-secretase involves the cleavage of neurexins and/or neuroligins and whether such cleavage may play a contributory role in the pathogenesis of AD.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Specialized Center (P50)
Project #
5P50AG047366-04
Application #
9483594
Study Section
Special Emphasis Panel (ZAG1)
Project Start
Project End
Budget Start
2018-05-01
Budget End
2019-04-30
Support Year
4
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Stanford University
Department
Type
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94304

  Publications

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Cocoros, Noelle M; Ording, Anne G; Horváth-Puhó, Erzsébet et al. (2018) In utero exposure to the 1918 pandemic influenza in Denmark and risk of dementia. Influenza Other Respir Viruses 12:314-318
Weintraub, Sandra; Besser, Lilah; Dodge, Hiroko H et al. (2018) Version 3 of the Alzheimer Disease Centers' Neuropsychological Test Battery in the Uniform Data Set (UDS). Alzheimer Dis Assoc Disord 32:10-17
Svensson, Elisabeth; Henderson, Victor W; Szépligeti, Szimonetta et al. (2018) Tonsillectomy and risk of Parkinson's disease: A danish nationwide population-based cohort study. Mov Disord 33:321-324
Wilmoth, Kristin; LoBue, Christian; Clem, Matthew A et al. (2018) Consistency of traumatic brain injury reporting in older adults with and without cognitive impairment. Clin Neuropsychol 32:524-529
Henderson, V W (2018) Progesterone and human cognition. Climacteric 21:333-340
Ting, Simon Kang Seng; Foo, Heidi; Chia, Pei Shi et al. (2018) Dyslexic Characteristics of Chinese-Speaking Semantic Variant of Primary Progressive Aphasia. J Neuropsychiatry Clin Neurosci 30:31-37

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