Synthesis, metabolism and in vitro cytotoxicity studies on novel lavendamycin antitumor agents

Synthesis, metabolism and in vitro cytotoxicity studies on novel lavendamycin antitumor agents

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 P...

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Veröffentlicht in:Bioorganic & medicinal chemistry 2010-03, Vol.18 (5), p.1899-1909
Hauptverfasser: Cai, Wen, Hassani, Mary, Karki, Rajesh, Walter, Ervin D., Koelsch, Katherine H., Seradj, Hassan, Lineswala, Jayana P., Mirzaei, Hamid, York, Jeremy S., Olang, Fatemeh, Sedighi, Minoo, Lucas, Jennifer S., Eads, Thomas J., Rose, Anthony S., Charkhzarrin, Sahba, Hermann, Nicholas G., Beall, Howard D., Behforouz, Mohammad
Format: Artikel
Sprache:eng
Schlagworte:
Antineoplastic Agents - chemical synthesis
Antineoplastic Agents - metabolism
Antineoplastic Agents - toxicity
Antitumor
Cell Line, Tumor
Cytotoxicity
Humans
Lavendamycin analogues
NAD(P)H Dehydrogenase (Quinone) - chemistry
NAD(P)H Dehydrogenase (Quinone) - genetics
NAD(P)H Dehydrogenase (Quinone) - metabolism
NQO1
Quinoline-5,8-diones
Recombinant Proteins - chemistry
Recombinant Proteins - genetics
Recombinant Proteins - metabolism
Streptonigrin - analogs & derivatives
Streptonigrin - chemistry
Streptonigrin - metabolism
Streptonigrin - toxicity
Structure-Activity Relationship
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Zusammenfassung: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.
ISSN:0968-0896
1464-3391
DOI:10.1016/j.bmc.2010.01.037