ALCHAB, Faten; ETTOUATI, Laurent; BOUAZIZ, Zouhair; BOLLACKE, Andre; DELCROS, Jean-Guy; GERTZEN, Christoph G W; GOHLKE, Holger; PINAUD, Noël; MARCHIVIE, Mathieu; GUILLON, Jean; FENET, Bernard; JOSE, Joachim; BORGNE, Marc Le

doi:10.3390/ph8020279

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ALCHAB, Faten
Molécules bioactives et chimie médicinale [B2MC]

ETTOUATI, Laurent
Molécules bioactives et chimie médicinale [B2MC]

BOUAZIZ, Zouhair
Molécules bioactives et chimie médicinale [B2MC]

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Pharmaceuticals. 2015-06-08, vol. 8, n° 2, p. 279-302

MDPI

Résumé en anglais

Due to their system of annulated 6-5-5-6-membered rings, indenoindoles have sparked great interest for the design of ATP-competitive inhibitors of human CK2. In the present study, we prepared twenty-one indeno[1,2-b]indole derivatives, all of which were tested in vitro on human CK2. The indenoindolones 5a and 5b inhibited human CK2 with an IC50 of 0.17 and 0.61 µM, respectively. The indeno[1,2-b]indoloquinone 7a also showed inhibitory activity on CK2 at a submicromolar range (IC50 = 0.43 µM). Additionally, a large number of indenoindole derivatives was evaluated for their cytotoxic activities against the cell lines 3T3, WI-38, HEK293T and MEF.< Réduire

Mots clés en anglais

inhibitory activity

synthesis

protein kinase CK2

2-b]indoles

indeno[1

cytotoxicity

molecular modeling

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Synthesis, Biological Evaluation and Molecular Modeling of Substituted Indeno[1,2-b]indoles as Inhibitors of Human Protein Kinase CK2.

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