Direct inter-subdomain interactions switch between the closed and open forms of the Hsp70 nucleotide-binding domain in the nucleotide-free state

Shida, Meiri; Arakawa, Akihiko; Ishii, Ryohei; Kishishita, S.; Takagi, Tetsuo; Kukimoto-Niino, Mutsuko; Sugano, Sumio; Tanaka, Akiko; Shirouzu, Mikako; Yokoyama, Shigeyuki

doi:10.1107/s0907444909053979

Cited by 23 publications

(29 citation statements)

References 52 publications

(52 reference statements)

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“…32 It has been suggested previously that the closed conformation is apparently stabilized by the formation of a solvent exposed salt-bridge between glutamic acid-268 and lysine-56. 35 Intrigued by the formation of this intramolecular interaction, we then sought to generate a co-crystal structure with the bacterial natural product sangivamycin 10 ( K D = 3.3 μM) (Figure 4). …”

Section: Results and Discussionmentioning

confidence: 99%

Exploiting Protein Conformational Change to Optimize Adenosine-Derived Inhibitors of HSP70

et al. 2016

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HSP70 is a molecular chaperone and a key component of the heat-shock response. Because of its proposed importance in oncology, this protein has become a popular target for drug discovery, efforts which have as yet brought little success. This study demonstrates that adenosine-derived HSP70 inhibitors potentially bind to the protein with a novel mechanism of action, the stabilization by desolvation of an intramolecular salt-bridge which induces a conformational change in the protein, leading to high affinity ligands. We also demonstrate that through the application of this mechanism, adenosine-derived HSP70 inhibitors can be optimized in a rational manner.

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Section: Results and Discussionmentioning

confidence: 99%

Exploiting Protein Conformational Change to Optimize Adenosine-Derived Inhibitors of HSP70

et al. 2016

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“…ATP complex was built by substituting ADP with ATP-Mg 2+ coordinates obtained from 2EA8 structure [44]. Hsp110 X-ray structure of S. cerevisiae (PDB ID: 3C7N_A [12]) in complex with ATP-Mg 2+ was utilized as starting point.…”

Section: Methodsmentioning

confidence: 99%

Molecular Mechanism of Allosteric Communication in Hsp70 Revealed by Molecular Dynamics Simulations

et al. 2012

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Investigating ligand-regulated allosteric coupling between protein domains is fundamental to understand cell-life regulation. The Hsp70 family of chaperones represents an example of proteins in which ATP binding and hydrolysis at the Nucleotide Binding Domain (NBD) modulate substrate recognition at the Substrate Binding Domain (SBD). Herein, a comparative analysis of an allosteric (Hsp70-DnaK) and a non-allosteric structural homolog (Hsp110-Sse1) of the Hsp70 family is carried out through molecular dynamics simulations, starting from different conformations and ligand-states. Analysis of ligand-dependent modulation of internal fluctuations and local deformation patterns highlights the structural and dynamical changes occurring at residue level upon ATP-ADP exchange, which are connected to the conformational transition between closed and open structures. By identifying the dynamically responsive protein regions and specific cross-domain hydrogen-bonding patterns that differentiate Hsp70 from Hsp110 as a function of the nucleotide, we propose a molecular mechanism for the allosteric signal propagation of the ATP-encoded conformational signal.

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“…The NMR data yielded a range of conformations of this substance ( Figures S2C and S2D), which were then subjected to computational analysis to elucidate the low energy conformation of free Az ( Figure S2E). The conformational information and STD NMR data were utilized for molecular docking studies with HSP70 (PDB code 4IO8, a VER-155008 complex form; and PDB code 2E8A, an AMP-PNP [adenylyl-imidodiphosphate, a non-hydrolyzable analog of ATP] bound form) to obtain a more detailed view of the binding mode of Az to HSP70 (Cho et al, 2011;Schlecht et al, 2013;Shida et al, 2010). The results of a molecular modeling study show that Az adopts a conformation that is closely overlaid with AMP-PNP in the ATP binding site of HSP70 ( Figure 2A).…”

Section: Binding Mode Of Az To Hsp70mentioning

confidence: 99%

A Small Molecule Inhibitor of ATPase Activity of HSP70 Induces Apoptosis and Has Antitumor Activities

Kim

et al. 2015

Chemistry & Biology

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The heat shock protein HSP70 plays antiapoptotic and oncogenic roles, and thus its inhibition has been recognized as a potential avenue for anticancer therapy. Here we describe the small molecule, apoptozole (Az), which inhibits the ATPase activity of HSP70 by binding to its ATPase domain and, as a result, induces an array of apoptotic phenotypes in cancer cells. Affinity chromatography provides evidence that Az binds HSP70 but not other types of heat shock proteins including HSP40, HSP60, and HSP90. We also demonstrate that Az induces cancer cell death via caspase-dependent apoptosis by disrupting the interaction of HSP70 with APAF-1. Animal studies indicate that Az treatment retards tumor growth in a xenograft mouse model without affecting mouse viability. These studies suggest that Az will aid the development of new cancer therapies and serve as a chemical probe to gain a better understanding of the diverse functions of HSP70.

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Direct inter-subdomain interactions switch between the closed and open forms of the Hsp70 nucleotide-binding domain in the nucleotide-free state

Cited by 23 publications

References 52 publications

Exploiting Protein Conformational Change to Optimize Adenosine-Derived Inhibitors of HSP70

Exploiting Protein Conformational Change to Optimize Adenosine-Derived Inhibitors of HSP70

Molecular Mechanism of Allosteric Communication in Hsp70 Revealed by Molecular Dynamics Simulations

A Small Molecule Inhibitor of ATPase Activity of HSP70 Induces Apoptosis and Has Antitumor Activities

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