The human protein Pontin, which belongs to the AAA+ (ATPases associated with various cellular activities) family, is overexpressed in several cancers and its silencing in vitro leads to tumour cell growth arrest and apoptosis, making it a good target for cancer therapy. In particular, high levels of expression were found in hepatic tumours for which the therapeutic arsenal is rather limited. The three-dimensional structure of Pontin has been resolved previously, revealing a hexameric assembly with one ADP molecule co-crystallized in each subunit. Using Vina, DrugScore and Xscore, structure-based virtual screening of 2200 commercial molecules was conducted into the ATP-binding site formed by a dimer of Pontin in order to prioritize the best candidates. Complementary to the in silico screening, a versatile and sensitive colorimetric assay was set up to measure the disruption of the ATPase activity of Pontin. This assay allowed the determination of inhibition curves for more than 20 top-scoring compounds, resulting in the identification of four ligands presenting an inhibition constant in the micromolar concentration range. Three of them inhibited tumour cell proliferation. The association of virtual screening and experimental assay thus proved successful for the discovery of the first small-molecule inhibitors of Pontin.
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Research Article|
March 27 2012
First identification of small-molecule inhibitors of Pontin by combining virtual screening and enzymatic assay
Judith Elkaim;
Judith Elkaim
*Molecular Modeling Group, IECB-CNRS-Université de Bordeaux, UMR 5248, 2 rue R. Escarpit, F-33607 Pessac, France
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Michel Castroviejo;
Michel Castroviejo
†Platform Protein Expression and Purification, CNRS, UMR 5234, 146 rue L. Saignat, F-33076 Bordeaux Cedex, France
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Driss Bennani;
Driss Bennani
*Molecular Modeling Group, IECB-CNRS-Université de Bordeaux, UMR 5248, 2 rue R. Escarpit, F-33607 Pessac, France
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Said Taouji;
Said Taouji
‡Physiopathologie du Cancer du Foie, INSERM U1053-Université de Bordeaux, 146 rue L. Saignat, F-33076 Bordeaux Cedex, France
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Nathalie Allain;
Nathalie Allain
‡Physiopathologie du Cancer du Foie, INSERM U1053-Université de Bordeaux, 146 rue L. Saignat, F-33076 Bordeaux Cedex, France
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Michel Laguerre;
Michel Laguerre
*Molecular Modeling Group, IECB-CNRS-Université de Bordeaux, UMR 5248, 2 rue R. Escarpit, F-33607 Pessac, France
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Jean Rosenbaum;
Jean Rosenbaum
‡Physiopathologie du Cancer du Foie, INSERM U1053-Université de Bordeaux, 146 rue L. Saignat, F-33076 Bordeaux Cedex, France
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Jean Dessolin;
Jean Dessolin
1
*Molecular Modeling Group, IECB-CNRS-Université de Bordeaux, UMR 5248, 2 rue R. Escarpit, F-33607 Pessac, France
1Correspondence may be addressed to either of these authors (email [email protected] for molecular modelling aspects or [email protected] for biochemical aspects).
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Patrick Lestienne
Patrick Lestienne
1
‡Physiopathologie du Cancer du Foie, INSERM U1053-Université de Bordeaux, 146 rue L. Saignat, F-33076 Bordeaux Cedex, France
1Correspondence may be addressed to either of these authors (email [email protected] for molecular modelling aspects or [email protected] for biochemical aspects).
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Publisher: Portland Press Ltd
Received:
October 05 2011
Revision Received:
January 23 2012
Accepted:
January 24 2012
Accepted Manuscript online:
January 24 2012
Online ISSN: 1470-8728
Print ISSN: 0264-6021
© The Authors Journal compilation © 2012 Biochemical Society
2012
Biochem J (2012) 443 (2): 549–559.
Article history
Received:
October 05 2011
Revision Received:
January 23 2012
Accepted:
January 24 2012
Accepted Manuscript online:
January 24 2012
Citation
Judith Elkaim, Michel Castroviejo, Driss Bennani, Said Taouji, Nathalie Allain, Michel Laguerre, Jean Rosenbaum, Jean Dessolin, Patrick Lestienne; First identification of small-molecule inhibitors of Pontin by combining virtual screening and enzymatic assay. Biochem J 15 April 2012; 443 (2): 549–559. doi: https://doi.org/10.1042/BJ20111779
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