Phosphorylation Dynamics Regulate Hsp27-Mediated Rescue of Neuronal Plasticity Deficits in Tau Transgenic Mice

Abisambra, Jose F.; Blair, Laura J.; Hill, Shannon E.; Jones, Jeffrey R.; Kraft, Clara; Rogers, Justin T.; Koren, John; Jinwal, Umesh K.; Lawson, Lisa Y.; Johnson, Amelia G.; Wilcock, Donna M.; O’Leary, John C.; Jansen-West, Karen; Muschol, Martin; Golde, Todd E.; Weeber, Edwin J.; Banko, Jessica L.; Dickey, Chad A.

doi:10.1523/jneurosci.3155-10.2010

Cited by 104 publications

(135 citation statements)

References 41 publications

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“…We used dynamic light scattering (DLS) to assess how the Hsp90/FKBP51 complex was regulating the kinetics of global tau aggregation (44). For these studies, tau aggregation was induced with heparin sulfate in the presence of Hsp90 or FKBP51 alone and in the presence of Hsp90 and FKBP51 together.…”

Section: Fkbp51 Depletion Reduces Tau Levels In Brainmentioning

confidence: 99%

“…FKBP51 expression was observed in the HPC; however, the AAV did not transduce all neurons ( Figure 4A). Due to this typical limitation of AAV use, a fluorescent masking technique previously developed by our lab was used to evaluate the levels of tau in neurons express- ing the AAV product, in this case FKBP51 or GFP (44). Triple-immunofluorescent staining of sections for FKBP51, total tau, and the neuronal marker, NeuN, revealed that the amount of tau found within FKBP51-positive neurons was significantly increased compared with tau levels in neurons overexpressing GFP (Figure 4, B and C).…”

Section: Fkbp51 Depletion Reduces Tau Levels In Brainmentioning

confidence: 99%

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Accelerated neurodegeneration through chaperone-mediated oligomerization of tau

et al. 2013

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Aggregation of tau protein in the brain is associated with a class of neurodegenerative diseases known as tauopathies. FK506 binding protein 51 kDa (FKBP51, encoded by FKBP5) forms a mature chaperone complex with Hsp90 that prevents tau degradation. In this study, we have shown that tau levels are reduced throughout the brains of Fkbp5 -/-mice. Recombinant FKBP51 and Hsp90 synergized to block tau clearance through the proteasome, resulting in tau oligomerization. Overexpression of FKBP51 in a tau transgenic mouse model revealed that FKBP51 preserved the species of tau that have been linked to Alzheimer's disease (AD) pathogenesis, blocked amyloid formation, and decreased tangle load in the brain. Alterations in tau turnover and aggregate structure corresponded with enhanced neurotoxicity in mice. In human brains, FKBP51 levels increased relative to age and AD, corresponding with demethylation of the regulatory regions in the FKBP5 gene. We also found that higher FKBP51 levels were associated with AD progression. Our data support a model in which age-associated increases in FKBP51 levels and its interaction with Hsp90 promote neurotoxic tau accumulation. Strategies aimed at attenuating FKBP51 levels or its interaction with Hsp90 have the potential to be therapeutically relevant for AD and other tauopathies.

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Section: Fkbp51 Depletion Reduces Tau Levels In Brainmentioning

confidence: 99%

Section: Fkbp51 Depletion Reduces Tau Levels In Brainmentioning

confidence: 99%

Accelerated neurodegeneration through chaperone-mediated oligomerization of tau

et al. 2013

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“…Until now, HSPB1, HSPB5, and HSPB8 have been the most widely studied members. They have been found to reduce protein aggregates caused by proteins containing an expanded polyQ tract (HSPB8 [20]), tau (HSPB1 [34][35][36]), amyloid-beta (HSPB1, HSPB5, and HSPB8 [37,38]), TDP43 (HSPB8 [15]) and SOD1 (HSPB1, HSPB5, and HSPB8 [18,39]). However, only little is known about were treated with bortezomib (100 nM) or with 3-MA (20 mM) and wortmannin (200 nM) overnight.…”

Section: Discussionmentioning

confidence: 99%

HSPA1A-Independent Suppression of PARK2 C289G Protein Aggregation by Human Small Heat Shock Proteins

Minoia

Grit

Kampinga

2014

Molecular and Cellular Biology

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The C289G mutation of the parkin E3-ubiquitin protein ligase (PARK2) is associated with autosomal recessive juvenile onset Parkinson's disease and was found to be associated with protein aggregation. Members of the human small heat shock proteins (HSPBs) have been implicated in protein degradation and prevention of protein aggregation. In this study, we show that of the 10 HSPB members, individual overexpression of HSPB1, HSPB2, HSPB4, and HSPB7 suppresses PARK2 C289G-associated protein aggregation. Intriguingly, the protective actions of these HSPBs are not impaired upon inactivation of the ATP-dependent HSP70 chaperone machines. Depending on the HSPB member the protective actions involve either autophagic or proteasomal degradation pathways.

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“…Quantification and Statistical Analyses-Quantification of all blots was performed using ImageJ software as described previously (30). Graphs are plotted based on relative intensity values.…”

Section: Methodsmentioning

confidence: 99%

Glucose-regulated Protein 94 Triage of Mutant Myocilin through Endoplasmic Reticulum-associated Degradation Subverts a More Efficient Autophagic Clearance Mechanism

Suntharalingam

Abisambra

O’Leary

et al. 2012

Journal of Biological Chemistry

116

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Background: Mutant myocilin accumulates in the endoplasmic reticulum for unknown reasons. Results: Glucose-regulated protein (Grp) 94 depletion reduces mutant myocilin by engaging autophagy. Conclusion: Grp94 triages mutant myocilin through ER-associated degradation, subverting autophagy. Significance: Treating glaucoma could be possible by inhibiting Grp94 and reducing its novel client, mutant myocilin.

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Phosphorylation Dynamics Regulate Hsp27-Mediated Rescue of Neuronal Plasticity Deficits in Tau Transgenic Mice

Cited by 104 publications

References 41 publications

Accelerated neurodegeneration through chaperone-mediated oligomerization of tau

Accelerated neurodegeneration through chaperone-mediated oligomerization of tau

HSPA1A-Independent Suppression of PARK2 C289G Protein Aggregation by Human Small Heat Shock Proteins

Glucose-regulated Protein 94 Triage of Mutant Myocilin through Endoplasmic Reticulum-associated Degradation Subverts a More Efficient Autophagic Clearance Mechanism

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