Published November 2015 | Version Published + Supplemental Material
Journal Article Open

Computational predictions of corroles as a class of Hsp90 inhibitors

  • 1. ROR icon California Institute of Technology
  • 2. ROR icon Technion – Israel Institute of Technology
  • 3. ROR icon Israel Corp (Israel)

Abstract

Corroles have been shown experimentally to cause cell cycle arrest, and there is some evidence that this might be attributed to an inhibitory effect of corroles on Heat shock protein 90 (Hsp90), which is known to play a vital role in cancer cell proliferation. In this study, we used molecular dynamics to examine the interaction of gallium corroles with Hsp90, and found that they can bind preferentially to the ATP-binding N-terminal site. We also found that structural variations of the corrole ring can influence the binding energies and affinities of the corrole to Hsp90. We predict that both the biscarboxylated corrole (4-Ga) and a proposed 3,17-bis-sulfonated corrole (7-Ga) are promising alternatives to Ga(III) 5,10,15-tris(pentafluorophenyl)-2,17-bis(sulfonic acid)-corrole (1-Ga) as anti-cancer agents.

Additional Information

© 2015 The Royal Society of Chemistry. Received 22nd May 2015, Accepted 31st July 2015, First published online 31 July 2015. A Caltech/COH grant (H.B.G. and Z.G.) and the AACR-Thomas J. Bardos Science Education Award (R.D.T.) are gratefully acknowledged. SSD and WAG were supported partially by NIH (R01NS073115 and R01AI040567). We would also like to thank Y. C. Lam for helpful discussions.

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Additional details

Identifiers

Eprint ID
59443
Resolver ID
CaltechAUTHORS:20150812-101036401

Funding

Caltech/City of Hope Biomedical Initiative
AACR-Thomas J. Bardos Science Education Award
NIH
R01NS073115
NIH
R01AI040567

Dates

Created
2015-08-12
Created from EPrint's datestamp field
Updated
2021-11-10
Created from EPrint's last_modified field

Caltech Custom Metadata

Other Numbering System Name
WAG
Other Numbering System Identifier
1140