Controlling biochemical pathways through chemically designed modulators may provide novel opportunities to develop therapeutic drugs and chemical tools. The underlying challenge is to design new molecular entities able to act as allosteric chemical switches that selectively turn on/off functions by modulating the conformational dynamics of their target protein. We examine the origins of the stimulation of ATPase and closure kinetics in the molecular chaperone Hsp90 by allosteric modulators through atomistic molecular dynamics (MD) simulations and analysis of protein-ligand interactions. In particular, we focus on the cross-talk between allosteric ligands and protein conformations and its effect on the dynamic properties of the chaperone's active state. We examine the impact of different allosteric modulators on the stability, structural and internal dynamics properties of Hsp90 closed state. A critical aspect of this study is the development of a quantitative model that correlates Hsp90 activation to the presence of a certain compound, making use of information on the dynamic adaptation of protein conformations to the presence of the ligand, which allows to capture conformational states relevant in the activation process. We discuss the implications of considering the conformational dialogue between allosteric ligands and protein conformations for the design of new functional modulators.

Molecular dynamics simulations reveal the mechanisms of allosteric activation of Hsp90 by designed ligands / V. G., M. E., S. Sattin, T. J., A. D. A., A. Bernardi, C. G.. - In: SCIENTIFIC REPORTS. - ISSN 2045-2322. - 6(2016), pp. 23830.1-23830.13. [10.1038/srep23830]

Molecular dynamics simulations reveal the mechanisms of allosteric activation of Hsp90 by designed ligands

S. Sattin;A. Bernardi
Penultimo
;
2016

Abstract

Controlling biochemical pathways through chemically designed modulators may provide novel opportunities to develop therapeutic drugs and chemical tools. The underlying challenge is to design new molecular entities able to act as allosteric chemical switches that selectively turn on/off functions by modulating the conformational dynamics of their target protein. We examine the origins of the stimulation of ATPase and closure kinetics in the molecular chaperone Hsp90 by allosteric modulators through atomistic molecular dynamics (MD) simulations and analysis of protein-ligand interactions. In particular, we focus on the cross-talk between allosteric ligands and protein conformations and its effect on the dynamic properties of the chaperone's active state. We examine the impact of different allosteric modulators on the stability, structural and internal dynamics properties of Hsp90 closed state. A critical aspect of this study is the development of a quantitative model that correlates Hsp90 activation to the presence of a certain compound, making use of information on the dynamic adaptation of protein conformations to the presence of the ligand, which allows to capture conformational states relevant in the activation process. We discuss the implications of considering the conformational dialogue between allosteric ligands and protein conformations for the design of new functional modulators.
English
shock-protein 90; heat-shock-protein-70 HSP70 inhibitor; ATP hydrolysis; conformational dynamics; substrate recognition; Escherichia-Coli; drug discovery; chaperone; enzymes; principles
Settore CHIM/06 - Chimica Organica
Articolo
Esperti anonimi
Ricerca di base
Pubblicazione scientifica
   Chemical Control of signalling pathway by modulation of hub proteins
   CHECOSP
   FONDAZIONE CARIPLO
   2011-1800
2016
6
23830
1
13
13
Pubblicato
Periodico con rilevanza internazionale
crossref
pubmed
Aderisco
info:eu-repo/semantics/article
Molecular dynamics simulations reveal the mechanisms of allosteric activation of Hsp90 by designed ligands / V. G., M. E., S. Sattin, T. J., A. D. A., A. Bernardi, C. G.. - In: SCIENTIFIC REPORTS. - ISSN 2045-2322. - 6(2016), pp. 23830.1-23830.13. [10.1038/srep23830]
open
Prodotti della ricerca::01 - Articolo su periodico
7
262
Article (author)
no
V. G., M. E., S. Sattin, T. J., A. D. A., A. Bernardi, C. G.
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/378525
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