Alzheimer's disease (AD) is defined by two major pathological hallmarks, specifically senile plaques consisting of ?-amyloid (A?) and neurofibrillary tangles composed of abnormally phosphorylated and cleaved tau. A? is neurotoxic and can trigger a cascade of neurodegenerative events in AD. Tau abnormalities also contribute to AD progression. In addition, abnormal tau phosphorylation, cleavage, and mutations in the tau gene, MAPT can induce tau aggregation and consequent toxicity in neurons, leading to several other neurodegenerative tauopathic disorders which include progressive supranuclear palsy (PSP), Pick's disease, corticobasal degeneration, frontotemporal dementia and Parkinsonism linked to chromosome 17 (FTDP-17). Hence, identification of new factors mediating neurotoxicity caused by A? and/or tau is important for disease intervention. We recently identified a novel pro-apoptotic protein, appoptosin, and demonstrated that overexpression of appoptosion results in caspase-dependent apoptosis. Importantly, we found that appoptosin levels are elevated in neurons exposed to A? and [excitotoxic] glutamate stimulation, with increased levels in brain samples from AD and PSP patients. Increased appoptosin expression leads to caspase-mediated tau cleavage and concomitant tau aggregation and synaptic dysfunction in neurons. Appoptosin transduction impairs motor function and exacerbates neuropathology in tau Tg mice; whereas reduced expression of appoptosin inhibits tau cleavage and aggregation, and abrogates mitochondrial fragmentation, caspase activation and neuronal death caused by A? insults. Appoptosin+/- mice have normal learning/memory and LTP, but show reduced LTD and slowed memory decay, thereby implicating its involvement in synaptic plasticity. Moreover, a single nucleotide polymorphism (SNP) rs1768208(C/T) near the appoptosin gene was reported as a risk factor for PSP, AD, CBD and frontotemporal dementia and we demonstrate that the T-allele variant occurs much more frequently in PSP and correlates tightly with increased appoptosin expression. Therefore, we hypothesize that an upregulation of appoptosin expression induced by A? in AD, or controlled by the SNP rs1768208 in various tauopathies, plays a central role in inducing neurodegeneration, and that downregulation of appoptosin provides a novel strategy for disease intervention. In this proposal, we will further ascertain that appoptosin SNP and expression are associated with tauopathic diseases, and determine that the SNP rs1768208(C/T) variant regulates appoptosin expression. We will then determine whether caspases, tau and glutamate receptor dynamics are involved in appoptosin-mediated synaptic plasticity. Finally, we will corroborate the role of appoptosin in AD and other tauopathies in vivo by studying whether upregulation of appoptosin leads to tauopathy-related neuropathologies and behavior, and whether a decrease of appoptosin can ameliorate disease-related phenotypes in APP/tau bigenic mice. Results from these studies will establish appoptosin as a novel and important player and therapeutic target in AD and other tauopathies.

Public Health Relevance

Tauopathic neurodegenerative disorders such as Alzheimer's disease (AD), progressive supranuclear palsy (PSP), Pick's disease, corticobasal degeneration, and frontotemporal dementia and Parkinsonism linked to chromosome 17 (FTDP-17) are characterized by the deposition of abnormal tau protein in the brain. Although mechanisms driving tauopathies are currently unclear, we have recently identified a novel pro-apoptotic protein, appoptosin that may be crucial for the regulation of tau cleavage/aggregation in tauopathy. This study will further elucidate the role of appoptosin in tauopathic pathologies, thereby providing a pathological mechanism for these poorly characterized disorders, which may eventually to the formulation of effective treatment strategies.

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG038710-09
Application #
9718069
Study Section
Cell Death in Neurodegeneration Study Section (CDIN)
Program Officer
Yang, Austin Jyan-Yu
Project Start
2011-08-15
Project End
2019-12-31
Budget Start
2019-06-01
Budget End
2019-12-31
Support Year
9
Fiscal Year
2019
Total Cost
Indirect Cost
Name
Sanford Burnham Prebys Medical Discovery Institute
Department
Type
DUNS #
020520466
City
La Jolla
State
CA
Country
United States
Zip Code
92037
Lee, C Y Daniel; Daggett, Anthony; Gu, Xiaofeng et al. (2018) Elevated TREM2 Gene Dosage Reprograms Microglia Responsivity and Ameliorates Pathological Phenotypes in Alzheimer's Disease Models. Neuron 97:1032-1048.e5
Du, Ying; Zhao, Yingjun; Li, Chuan et al. (2018) Inhibition of PKC? reduces amyloid-? levels and reverses Alzheimer disease phenotypes. J Exp Med 215:1665-1677
Zhao, Dongdong; Meng, Jian; Zhao, Yingjun et al. (2018) RPS23RG1 Is Required for Synaptic Integrity and Rescues Alzheimer's Disease-Associated Cognitive Deficits. Biol Psychiatry :
Zhang, Hongfeng; Huang, Timothy; Hong, Yujuan et al. (2018) The Retromer Complex and Sorting Nexins in Neurodegenerative Diseases. Front Aging Neurosci 10:79
Simandi, Zoltan; Pajer, Krisztian; Karolyi, Katalin et al. (2018) Arginine Methyltransferase PRMT8 Provides Cellular Stress Tolerance in Aging Motoneurons. J Neurosci 38:7683-7700
Zhao, Yingjun; Wu, Xilin; Li, Xiaoguang et al. (2018) TREM2 Is a Receptor for ?-Amyloid that Mediates Microglial Function. Neuron 97:1023-1031.e7
Zhao, Yingjun; Li, Xiaoguang; Huang, Timothy et al. (2017) Intracellular trafficking of TREM2 is regulated by presenilin 1. Exp Mol Med 49:e405
Zhu, Bing; Jiang, LuLin; Huang, Timothy et al. (2017) ER-associated degradation regulates Alzheimer's amyloid pathology and memory function by modulating ?-secretase activity. Nat Commun 8:1472
Huang, Timothy Y; Zhao, Yingjun; Jiang, Lu-Lin et al. (2017) SORLA attenuates EphA4 signaling and amyloid ?-induced neurodegeneration. J Exp Med 214:3669-3685
Zheng, Qiuyang; Zheng, Xiaoyuan; Zhang, Lishan et al. (2017) The Neuron-Specific Protein TMEM59L Mediates Oxidative Stress-Induced Cell Death. Mol Neurobiol 54:4189-4200

Showing the most recent 10 out of 42 publications