Dolastatin 11 conformations, analogues and pharmacophore

Author:

Ali, M. A.

Bates, R. B.

Crane, Z. D.

Dicus, C. W.

Gramme, M. R.

Hamel, E.

Marcischak, J.

Martinez, D. S.

McClure, K. J.

Nakkiew, P.

Pettit, G. R.

Stessman, C. C.

Sufi, B. A.

Yarick, G. V.
Author Address

Univ Arizona, Dept Chem, Tucson, AZ 85721 USA. NCI, Frederick, MD 21702 USA. Arizona State Univ, Dept Chem & Biochem, Tempe, AZ 85287 USA. Arizona State Univ, Canc Res Inst, Tempe, AZ 85287 USA Bates, RB, Univ Arizona, Dept Chem, Tucson, AZ 85721 USA

Abstract:

Twenty analogues of the natural antitumor agent dolastatin 11, including majusculamide C, were synthesized and tested for cytotoxicity against human cancer cells and stimulation of actin polymerization. Only analogues containing the 30-membered ring were active. Molecular modeling and NMR evidence showed the low-energy conformations. The amide bonds are all trans except for the one between the Tyr and Val units, which is cis. Since an analogue restricted to negative 2-3-4-5 angles stimulated actin polymerization but was inactive in cells, the binding conformation (most likely the lowest-energy conformation in water) has a negative 2-3-4-5 angle, whereas a conformation with a positive 2-3-4-5 angle (most likely the lowest energy conformation in chloroform) goes through cell walls. The highly active R alcohol from borohydride reduction of dolastatin I I is a candidate for conversion to prodrugs. (c) 2005 Elsevier Ltd. All rights reserved

See More

Author Address