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  4. Functional interaction of Heat Shock protein 90 and beclin 1 modulates toll-like receptor-mediated autophagy
 
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Functional interaction of Heat Shock protein 90 and beclin 1 modulates toll-like receptor-mediated autophagy

Journal
FASEB Journal
Journal Volume
25
Journal Issue
8
Pages
2700-2710
Date Issued
2011
Author(s)
LI-CHUNG HSU  
Xu, C.
Liu, J.
Hsu, L.-C.
Luo, Y.
Xiang, R.
Chuang, T.-H.
DOI
10.1096/fj.10-167676
URI
http://www.scopus.com/inward/record.url?eid=2-s2.0-80051688648&partnerID=MN8TOARS
http://scholars.lib.ntu.edu.tw/handle/123456789/362023
Abstract
Autophagy is one of the downstream effector mechanisms for elimination of intracellular microbes following activation of the Toll-like receptors (TLRs). Although the detailed molecular mechanism for this cellular process is still unclear, Beclin 1, a key molecule for autophagy, has been suggested to play a role. Heat shock protein 90 (Hsp90) is a molecular chaperone that regulates the stability of signaling proteins. Herein, we show that Hsp90 forms a complex with Beclin 1 through an evolutionarily conserved domain to maintain the stability of Beclin 1. In monocytic cells, geldanamycin (GA), an Hsp90 inhibitor, effectively promoted proteasomal degradation of Beclin 1 in a concentration-dependent (EC(50) 100 nM) and time-dependent (t(50) 2 h) manner. In contrast, KNK437/Hsp inhibitor I had no effect. Hsp90 specifically interacted with Beclin 1 but not with other adapter proteins in the TLR signalsome. Treatment of cells with GA inhibited TLR3- and TLR4-mediated autophagy. In addition, S. typhimurium infection-induced autophagy was blocked by GA treatment. This further suggested a role of the Hsp90/Beclin 1 in controlling autophagy in response to microbial infections. Taken together, our data revealed that by maintaining the homeostasis of Beclin 1, Hsp90 plays a novel role in TLR-mediated autophagy.
Type
journal article

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