2002
DOI: 10.1016/s0014-5793(02)03752-3
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Interdomain interaction through helices A and B of DnaK peptide binding domain

Abstract: In order to better de¢ne the structural elements involved in allosteric signalling, wild-type DnaK and three deletion mutants of the peptide binding domain have been characterized by biophysical (steady-state and time-resolved £uorescence) and biochemical methods. In the presence of ATP the chemical environment of the single tryptophan residue of DnaK, located in the ATPase domain, becomes less polar, as seen by a blue shift of the emission maximum and a shortening of the £uorescence lifetime, and its accessib… Show more

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Cited by 71 publications
(114 citation statements)
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References 22 publications
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“…The ATPase activity of the DnaK1-554 mutant (0.42 mol ATP (mol protein) Ϫ1 min Ϫ1 ) was higher than those of wt DnaK and the other deletion mutants, which were found to be similar to the published value of 0.12 mol ATP (mol protein) Ϫ1 min Ϫ1 (9). This result might be caused by a cis-interaction of hydrophobic residues at the C-terminal half of helix B with the peptide-binding site, as was shown recently for a similar construct (8).…”
Section: Resultssupporting
confidence: 82%
See 1 more Smart Citation
“…The ATPase activity of the DnaK1-554 mutant (0.42 mol ATP (mol protein) Ϫ1 min Ϫ1 ) was higher than those of wt DnaK and the other deletion mutants, which were found to be similar to the published value of 0.12 mol ATP (mol protein) Ϫ1 min Ϫ1 (9). This result might be caused by a cis-interaction of hydrophobic residues at the C-terminal half of helix B with the peptide-binding site, as was shown recently for a similar construct (8).…”
Section: Resultssupporting
confidence: 82%
“…In this context, a recent work indicates that helix D is engaged in maintaining stable DnaK-peptide complexes, and that helix E and the last 31 residues at the C terminus might contact the ATPase domain (8). Furthermore, the finding that helix A and the C-terminal half of helix B are involved in interdomain communication (9) points to the importance of the lid subdomain in maintaining the functionality of DnaK. Besides these functions, it has also been proposed that the lid of DnaK and other Hsp70 proteins might interact with DnaJ (10).…”
mentioning
confidence: 98%
“…C, upon rapid mixing with ATP, fp5 release follows the same kinetic profile in DnaK(1-631) (red), D628A (green), and wild type DnaK (blue). D, DnaK(1-631) (red), D628A (green), and wild type (blue) display the same characteristic blue shift and intensity quench of Trp fluorescence upon ATP binding, indicating that they undergo productive interdomain docking (7,41). The lower and more lightly shaded traces are from measurements after ATP addition.…”
Section: Dnak C-terminal Region Is Not Required For Binding Of a Peptmentioning
confidence: 95%
“…Nucleotide-binding domain residue Trp-102 undergoes fluorescence emission changes upon binding of ATP and in the presence of the SBD lid and is therefore a probe for functional ATP-induced interdomain docking (41). The physical proximity of the disordered C-terminal tail to the structured SBD lid suggests that C-terminal mutation might alter lid interaction with the nucleotide-binding domain.…”
Section: Dnak C-terminal Region Is Not Required For Binding Of a Peptmentioning
confidence: 99%
“…As can be deduced from the crystal structure of bovine Hsc70, mutations N175A/D176A and E240A/V241A affect close contact ionic and hydrophobic interactions that directly connect the NBD with helix A of the SBD (N175A/D176A and E240A/ V241A) and with an adjacent part of the SBD ␤-sheet subdomain (E240A/V241A). Both structural elements have been implicated in the allosteric mechanism because helix A forms the basis of the ␣-helical lid that covers the peptide-binding pocket formed by the ␤-sheet subdomain (54,55). Additionally, apart from directly disrupting molecular contacts between NBD and SBD, the mutations could affect interdomain communication by interfering with the insertion of the hydrophobic domain linker segment into a hydrophobic cleft between subdomains IA and IIA of the NBD.…”
Section: Discussionmentioning
confidence: 99%