The high-affinity HSP90-CHIP complex recognizes and selectively degrades phosphorylated tau client proteins

Dickey, Chad A.; Kamal, Adeela; Lundgren, Karen; Klosak, Natalia; Bailey, Rachel M.; Dunmore, Judith; Ash, Peter E.A.; Shoraka, Sareh; Zlatković, Jelena; Eckman, Christopher B.; Patterson, Cam; Dickson, Dennis W.; Nahman, N. Stanley; Hutton, Michael; Burrows, Francis; Petrucelli, Leonard

doi:10.1172/jci29715

articleJournal of Clinical InvestigationFeb 15, 2007BRONZE OA

The high-affinity HSP90-CHIP complex recognizes and selectively degrades phosphorylated tau client proteins

CAChad A. Dickey AKAdeela Kamal KLKaren Lundgren NKNatalia Klosak RMRachel M. Bailey

Jacksonville College · Mayo Clinic in Florida · +5 more institutions

PubMed

Indexed incrossrefdoajpubmed

Abstract

A primary pathologic component of Alzheimer's disease (AD) is the formation of neurofibrillary tangles composed of hyperphosphorylated tau (p-tau). Expediting the removal of these p-tau species may be a relevant therapeutic strategy. Here we report that inhibition of Hsp90 led to decreases in p-tau levels independent of heat shock factor 1 (HSF1) activation. A critical mediator of this mechanism was carboxy terminus of Hsp70-interacting protein (CHIP), a tau ubiquitin ligase. Cochaperones were also involved in Hsp90-mediated removal of p-tau, while those of the mature Hsp90 refolding complex prevented this effect. This is the first demonstration to our knowledge that blockade of the refolding pathway promotes…

Citation impact

635

total citations

FWCI: 16.55
Percentile: 100%
References: 51

Citations per year

Authors

16

Topics & keywords

Topics

Keywords

Hsp90
Phosphorylation
Cell biology
Chemistry
Chip
Biochemistry
Computational biology
Computer science

No related works found for this paper.