Abstract

Hereditary mutations within the MAPT (microtubule-associated protein tau) gene result in the pathologic and intra-neuronal aggregation of the tau protein that leads to frontotemporal dementia (FTD). The development of therapeutics for misfolded and abnormally processed (i.e. hyper-phosphorylated) tau species is necessary for sufferers of these autosomal tauopathic disorders and other neurological disorders which present with abnormal tau accumulation such as Alzheimer's disease (AD) and Parkinson's disease (PD). Molecular chaperones that are induced following a heat shock stimulus direct either the refolding of misfolded proteins and/or their targeting to the proteasome for degradation. Heat shock protein 90 (HSP90) inhibitors such as geldanamycin (GA) and its derivatives (17-allylamino-17-demethoxygeldanamycin; 17-AAG) can pharmacologically modulate chaperone levels and have recently been implicated for the treatment of cancer; sponsor NCI, Phase II) and mouse models of neurodegenerative disorders. In fact, Waza and colleagues recently showed that systemic administration of 17-AAG can markedly ameliorate motor impairments and life span in the spinal and bulbar muscular atrophy transgenic mouse model without detectable toxicity, by reducing amounts of monomeric and aggregated mutant androgen receptor. This study illustrates that Hsp90 inhibitors can be administrated chronically (20 weeks) and is well-tolerated. After screening a small panel of novel HSP90 inhibitors in a novel In-Cell Western assay that allows for direct intracellular quantitation of native and aberrant tau protein species, we identified a potent, blood brain barrier permeable HSP90 inhibitor (EC102) that significantly reduces abnormal tau species in vitro. In addition, we found that affected regions from human AD brain tissue have a significantly lower nanomolar binding affinity of Hsp90 for this novel inhibitor similar to tumor cells, while micromolar affinity was demonstrated in unaffected regions, comparable to normal cells. This suggests for the first time that in neurons, which progressively accumulate abnormal proteins in neurodegenerative disorders, and in this case AD, Hsp90 becomes engaged in active chaperoning and stabilization of these proteins and the Hsp90 adopts a novel high-affinity state. Thus these studies provide compelling evidence for the use of Hsp90 inhibitors to enhance Hsp90-mediated phospho-tau degradation in AD. We therefore propose that treatment with this compound may delay the progression of pathology and restore memory loss in mice that express a mutant form of human tau (P301L) driven by the tetracycline operator (rTg4510). ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Exploratory/Developmental Grants (R21)
Project #
1R21NS059363-01A1
Application #
7464465
Study Section
National Institute of Neurological Disorders and Stroke Initial Review Group (NSD)
Program Officer
Refolo, Lorenzo
Project Start
2008-02-01
Project End
2010-01-31
Budget Start
2008-02-01
Budget End
2009-01-31
Support Year
1
Fiscal Year
2008
Total Cost
$167,344
Indirect Cost

  Institution

Name
Mayo Clinic Jacksonville
Department
Type
DUNS #
153223151
City
Jacksonville
State
FL
Country
United States
Zip Code
32224

  Publications

Golde, Todd E; Petrucelli, Leonard; Lewis, Jada (2010) Targeting Abeta and tau in Alzheimer's disease, an early interim report. Exp Neurol 223:252-66
Deture, M; Hicks, C; Petrucelli, L (2010) Targeting heat shock proteins in tauopathies. Curr Alzheimer Res 7:677-84
Adams, Stephanie J; DeTure, Michael A; McBride, Melinda et al. (2010) Three repeat isoforms of tau inhibit assembly of four repeat tau filaments. PLoS One 5:e10810
Cook, Casey; Gass, Jennifer; Dunmore, Judith et al. (2009) Aging is not associated with proteasome impairment in UPS reporter mice. PLoS ONE 4:e5888
Cook, Casey; Petrucelli, Leonard (2009) A critical evaluation of the ubiquitin-proteasome system in Parkinson's disease. Biochim Biophys Acta 1792:664-75