Title
The crystal structure of the reduced, Zn<sup>2+</sup>-bound form of the B. subtilis Hsp33 chaperone and its implications for the activation mechanism
Date Issued
01 October 2004
Access level
open access
Resource Type
journal article
Author(s)
Janda I.
Devedjiev Y.
Derewenda U.
Dauter Z.
Bielnicki J.
Cooper D.
Joachimiak A.
Jakob U.
Derewenda Z.
University of Michigan
Abstract
The bacterial heat shock protein Hsp33 is a redox-regulated chaperone activated by oxidative stress. In response to oxidation, four cysteines within a Zn2+ binding C-terminal domain form two disulfide bonds with concomitant release of the metal. This leads to the formation of the biologically active Hsp33 dimer. The crystal structure of the N-terminal domain of the E. coli protein has been reported, but neither the structure of the Zn2+ binding motif nor the nature of its regulatory interaction with the rest of the protein are known. Here we report the crystal structure of the full-length B. subtilis Hsp33 in the reduced form. The structure of the N-terminal, dimerization domain is similar to that of the E. coli protein, although there is no domain swapping. The Zn2+ binding domain is clearly resolved showing the details of the tetrahedral coordination of Zn 2+ by four thiolates. We propose a structure-based activation pathway for Hsp33.
Start page
1901
End page
1907
Volume
12
Issue
10
Language
English
OCDE Knowledge area
Métodos de investigación bioquímica
Bioquímica, Biología molecular
Scopus EID
2-s2.0-4644266682
PubMed ID
Source
Structure
ISSN of the container
09692126
Sponsor(s)
We thank Dr. Frank Collart (Argonne National Laboratory) for providing the expression plasmid for the B. subtilis Hsp33, Aleksandra Gabrys for assistance in the early phase of this project, and Dr. Hauke Lilie for discussions. This work was supported by NIH Grant GM62615 to Z.S.D. and, in part, by NIH Grant GM065318 and a Burroughs Wellcome Fund Career Award to U.J.
Sources of information:
Directorio de Producción Científica
Scopus