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Merck

Multidrug resistance reversal by 3-formylchromones in human colon cancer and human mdr1 gene-transfected mouse lymphoma cells.

In vivo (Athens, Greece) (2006-11-10)
Zoltán Baráth, Rita Radics, Gabriella Spengler, Imre Ocsovszki, Masami Kawase, Noboru Motohashi, Yoshiaki Shirataki, Anamik Shah, József Molnár
RÉSUMÉ

Several new 3-formylchromone derivatives proved to be modifiers of multidrug resistance in mouse lymphoma cells and in human Colo320 colon cancer cells. There is apparently a structure-activity relationship between the antiproliferative multidrug resistance-reversing effect and the chemical structure of the 3-formylchromones. The total polar surface areas and the ground state dipole moments of the molecules are presumed to play a key role in the multidrug resistance-reversing effect. The log P values can provide an adequate explanation for the selective cytotoxicity against cancer cells.

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Sigma-Aldrich
3-Formyl-6-methylchromone, 97%
Sigma-Aldrich
3-Formyl-6-nitrochromone, 99%
Sigma-Aldrich
6-Bromo-3-formylchromone, 99%