Author/Authors :
Wen Cai، نويسنده , , Mary Hassani، نويسنده , , Rajesh Karki، نويسنده , , Ervin D. Walter، نويسنده , , Katherine H. Koelsch، نويسنده , , Hassan Seradj، نويسنده , , Jayana P. Lineswala، نويسنده , , Hamid Mirzaei، نويسنده , , Jeremy S. York، نويسنده , , Fatemeh Olang، نويسنده , , Minoo Sedighi، نويسنده , , Jennifer S. Lucas، نويسنده , , Thomas J. Eads، نويسنده , , Anthony S. Rose، نويسنده , , Sahba Charkhzarrin، نويسنده , , Nicholas G. Hermann، نويسنده , , Howard D. Beall، نويسنده , , Mohammad Behforouz، نويسنده ,
Abstract :
A series of lavendamycin analogues with two, three or four substituents at the C-6, C-7 N, C-2′, C-3′ and C-11′ positions were synthesized via short and efficient methods and evaluated as potential NAD(P)H:quinone oxidoreductase (NQO1)-directed antitumor agents. The compounds were prepared through Pictet–Spengler condensation of the desired 2-formylquinoline-5,8-diones with the required tryptophans followed by further needed transformations. Metabolism and toxicity studies demonstrated that the best substrates for NQO1 were also the most selectively toxic to NQO1-rich tumor cells compared to NQO1-deficient tumor cells.
Keywords :
Lavendamycin analogues , Quinoline-5 , 8-diones , Antitumor , NQO1 , Cytotoxicity
