Synthetic seco Forms of (-)-Diazonamide A.

Li, Jing; Chen, Xin; Burgett, Anthony W G; Harran, Patrick G

Li, Jing; Chen, Xin; Burgett, Anthony W G; Harran, Patrick G.

Afiliación

Li J; Department of Biochemistry University of Texas, Southwestern Medical Center at Dallas Dallas, TX 75390-9038 (USA) Fax: (+1) 214-648-6455.
Chen X; Department of Biochemistry University of Texas, Southwestern Medical Center at Dallas Dallas, TX 75390-9038 (USA) Fax: (+1) 214-648-6455.
Burgett AWG; Department of Biochemistry University of Texas, Southwestern Medical Center at Dallas Dallas, TX 75390-9038 (USA) Fax: (+1) 214-648-6455.
Harran PG; Department of Biochemistry University of Texas, Southwestern Medical Center at Dallas Dallas, TX 75390-9038 (USA) Fax: (+1) 214-648-6455.

Angew Chem Int Ed Engl ; 40(14): 2682-2685, 2001 Jul 16.

Article en En | MEDLINE | ID: mdl-29712335

RESUMEN

One bond and a water molecule separate title compound 1 from the potently bioactive peptide metabolite diazonamide A. Compositionally similar, yet topographically distinct, diazonamide A and 1 are both toxic towards cultured human cancer cells although the mechanisms underlying their actions likely differ. The quest towards completely synthetic diazonamides continues.

Palabras clave

antitumor agents; fluorescence spectroscopy; natural products; nitrogen heterocycles; transesterification

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