| Literature DB >> 17764690 |
Jonathan J Phillips1, Zhong-ping Yao, Wei Zhang, Stephen McLaughlin, Ernest D Laue, Carol V Robinson, Sophie E Jackson.
Abstract
The molecular chaperone Hsp90 is essential for the correct folding, maturation and activation of a diverse array of client proteins, including several key constituents of oncogenic processes. Hsp90 has become a focus of cancer research, since it represents a target for direct prophylaxis against multistep malignancy. Hydrogen-exchange mass spectrometry was used to study the structural and conformational changes undergone by full-length human Hsp90beta in solution upon binding of the kinase-specific co-chaperone Cdc37 and two Hsp90 ATPase inhibitors: Radicicol and the first-generation anticancer drug DMAG. Changes in hydrogen exchange pattern in the complexes in regions of Hsp90 remote to the ligand-binding site were observed indicating long-range effects. In particular, the interface between the N-terminal domain and middle domains exhibited significant differences between the apo and complexed forms. For the inhibitors, differences in the interface between the middle domain and the C-terminal domain were also observed. These data provide important insight into the structure of the biologically active form of the protein.Entities:
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Year: 2007 PMID: 17764690 DOI: 10.1016/j.jmb.2007.04.059
Source DB: PubMed Journal: J Mol Biol ISSN: 0022-2836 Impact factor: 5.469