Advances in understanding Alzheimer's disease (AD) have partially clarified the composition of 2 major lesions in the AD brain, i.e. amyloid rich senile plaques (Sps) and neurofibrillary abnormalities including neurofibrillary tangles (NFTs), dystrophic plaque-associated neurites and neuropil threads (NTs). Specifically, the filamentous components in Sps assemble from incompletely degraded Beta-amyloid or A4 peptides (BetaA4) derived from 1 or more of 3 major amyloid precusor proteins (APPs) in brain (i.e. APP695, APP751 and APP770) while the paired helical filaments (PHFs) in NFTs, dystrophic plaque neurites and Nts are abnormally phosphorylated tau derivatives (known as PHFtau or A680. Although recently identified mutations in the APP gene may play a role in the etiology of AD in a small subset of patients with familial AD (FAD), increasing evidence suggests that AD results from the abnormal metabolism of APPs and tau. This has prompted efforts to establish models of AD pathology in mice bearing BetaA4 containing partial or complete APP transgenes, and in rats injected with BetaA4 or SP cores. However, the development of additional animal models that more closely mimick AD is critical for elucidating the etiology and pathogenesis of AD. To this end, the goal of Project #4 is to establish alternative models of AD pathology in rodents. To probe the biology of PHFs and their interactions with BetaA4 in vivo, we will extend recent work from our lab in which A68 proteins were injected into rat brains and induced long lived co-deposits of rodent BetaA4 at the injections site. Additionally, we will probe the in vivo generation of BetaA4 in rodents transplanted with cultured human neurons (NT2N cells derived from the NT2 cell line) that constitutively secrete BetaA4 and express APP695 almost to the exclusion of APP751/770. Studies also will be conducted on transplants of transfected NT2N cells that over express APP695 or APP751 with and without a FAD mutation. The injected A68 proteins and grafts of the NT2N human neurons will be introduced into regions of the rodent brain that are homologous with regions of the human AD brain that accumulate abundant (hippocampus) or negligible (cerebellum) amyloid and neurofibrillary lesions. The analysis of injected A68 and NT2N grafts will be carried out at post- operation survival times of days to 24 months using biochemical methods as well as by immunohistochemistry in conjunction with light, confocal an electron microscopy. These strategies to model major AD lesions in the rodent brain should lead to significant new insights into the pathogenesis of AD.

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG011542-04
Application #
5204907
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
4
Fiscal Year
1996
Total Cost
Indirect Cost
Brunden, Kurt R; Ballatore, Carlo; Lee, Virginia M-Y et al. (2012) Brain-penetrant microtubule-stabilizing compounds as potential therapeutic agents for tauopathies. Biochem Soc Trans 40:661-6
Hurtado, David E; Molina-Porcel, Laura; Carroll, Jenna C et al. (2012) Selectively silencing GSK-3 isoforms reduces plaques and tangles in mouse models of Alzheimer's disease. J Neurosci 32:7392-402
Hurtado, David E; Molina-Porcel, Laura; Iba, Michiyo et al. (2010) A{beta} accelerates the spatiotemporal progression of tau pathology and augments tau amyloidosis in an Alzheimer mouse model. Am J Pathol 177:1977-88
Xu, Shaohua; Brunden, Kurt R; Trojanowski, John Q et al. (2010) Characterization of tau fibrillization in vitro. Alzheimers Dement 6:110-7
Brunden, Kurt R; Ballatore, Carlo; Crowe, Alex et al. (2010) Tau-directed drug discovery for Alzheimer's disease and related tauopathies: a focus on tau assembly inhibitors. Exp Neurol 223:304-10
Crowe, Alex; Huang, Wenwei; Ballatore, Carlo et al. (2009) Identification of aminothienopyridazine inhibitors of tau assembly by quantitative high-throughput screening. Biochemistry 48:7732-45
Chen, Xiao-Han; Johnson, Victoria E; Uryu, Kunihiro et al. (2009) A lack of amyloid beta plaques despite persistent accumulation of amyloid beta in axons of long-term survivors of traumatic brain injury. Brain Pathol 19:214-23
Brunden, Kurt R; Trojanowski, John Q; Lee, Virginia M-Y (2009) Advances in tau-focused drug discovery for Alzheimer's disease and related tauopathies. Nat Rev Drug Discov 8:783-93
Shineman, Diana W; Dain, Aleksandra S; Kim, Minkyu L et al. (2009) Constitutively active Akt inhibits trafficking of amyloid precursor protein and amyloid precursor protein metabolites through feedback inhibition of phosphoinositide 3-kinase. Biochemistry 48:3787-94
Kim, Minkyu L; Zhang, Bin; Mills, Ian P et al. (2008) Effects of TNFalpha-converting enzyme inhibition on amyloid beta production and APP processing in vitro and in vivo. J Neurosci 28:12052-61

Showing the most recent 10 out of 94 publications