Back to Search Start Over

Binding of a small molecule at a protein-protein interface regulates the chaperone activity of Hsp70-Hsp40

Authors :
Wisén, S
Bertelsen, EB
Thompson, AD
Patury, S
Ung, P
Chang, L
Evans, CG
Walter, GM
Wipf, P
Carlson, HA
Brodsky, JL
Zuiderweg, ERP
Gestwicki, JE
Wisén, S
Bertelsen, EB
Thompson, AD
Patury, S
Ung, P
Chang, L
Evans, CG
Walter, GM
Wipf, P
Carlson, HA
Brodsky, JL
Zuiderweg, ERP
Gestwicki, JE
Publication Year :
2010

Abstract

Heat shock protein 70 (Hsp70) is a highly conserved molecular chaperone that plays multiple roles in protein homeostasis. In these various tasks, the activity of Hsp70 is shaped by interactions with co-chaperones, such as Hsp40. The Hsp40 family of co-chaperones binds to Hsp70 through a conserved J-domain, and these factors stimulate ATPase and protein-folding activity. Using chemical screens, we identified a compound, 115-7c, which acts as an artificial co-chaperone for Hsp70. Specifically, the activities of 115-7c mirrored those of a Hsp40; the compound stimulated the ATPase and protein-folding activities of a prokaryotic Hsp70 (DnaK) and partially compensated for a Hsp40 loss-of-function mutation in yeast. Consistent with these observations, NMR and mutagenesis studies indicate that the binding site for 115-7c is adjacent to a region on DnaK that is required for J-domain-mediated stimulation. Interestingly, we found that 115-7c and the Hsp40 do not compete for binding but act in concert. Using this information, we introduced additional steric bulk to 115-7c and converted it into an inhibitor. Thus, these chemical probes either promote or inhibit chaperone functions by regulating Hsp70-Hsp40 complex assembly at a native protein-protein interface. This unexpected mechanism may provide new avenues for exploring how chaperones and co-chaperones cooperate to shape protein homeostasis. © 2010 American Chemical Society.

Details

Database :
OAIster
Notes :
text/plain, English
Publication Type :
Electronic Resource
Accession number :
edsoai.ocn854984804
Document Type :
Electronic Resource