Crystal structure of DnaK protein complexed with nucleotide exchange factor GrpE in DnaK chaperone system: insight into intermolecular communication

The conserved, ATP-dependent bacterial DnaK chaperones process client substrates with the aid of the co-chaperones DnaJ and GrpE. However, in the absence of structural information, how these proteins communicate with each other cannot be fully delineated. For the study reported here, we solved the c...

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Published inThe Journal of biological chemistry Vol. 287; no. 25; pp. 21461 - 21470
Main Authors Wu, Ching-Chung, Naveen, Vankadari, Chien, Chin-Hsiang, Chang, Yi-Wei, Hsiao, Chwan-Deng
Format Journal Article
LanguageEnglish
Published United States American Society for Biochemistry and Molecular Biology 15.06.2012
Subjects
Bacterial Proteins - chemistry
Bacterial Proteins - genetics
Bacterial Proteins - metabolism
Binding Sites
Crystallography, X-Ray
Geobacillus - chemistry
Geobacillus - genetics
Geobacillus - metabolism
Heat-Shock Proteins - chemistry
Heat-Shock Proteins - genetics
Heat-Shock Proteins - metabolism
Protein Multimerization
Protein Structure and Folding
Protein Structure, Quaternary
Protein Structure, Secondary
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Summary:The conserved, ATP-dependent bacterial DnaK chaperones process client substrates with the aid of the co-chaperones DnaJ and GrpE. However, in the absence of structural information, how these proteins communicate with each other cannot be fully delineated. For the study reported here, we solved the crystal structure of a full-length Geobacillus kaustophilus HTA426 GrpE homodimer in complex with a nearly full-length G. kaustophilus HTA426 DnaK that contains the interdomain linker (acting as a pseudo-substrate), and the N-terminal nucleotide-binding and C-terminal substrate-binding domains at 4.1-Å resolution. Each complex contains two DnaKs and two GrpEs, which is a stoichiometry that has not been found before. The long N-terminal GrpE α-helices stabilize the linker of DnaK in the complex. Furthermore, interactions between the DnaK substrate-binding domain and the N-terminal disordered region of GrpE may accelerate substrate release from DnaK. These findings provide molecular mechanisms for substrate binding, processing, and release during the Hsp70 chaperone cycle.
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ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.M112.344358