On the Synthesis and Anticancer Testing of alpha,beta-Unsaturated Ketones as Analogs of Combretastatin-A4

Document Type

Article

Publication Date

10-2009

Publication Source

Letters in Drug Design and Discovery

Volume Number

6

Issue Number

7

First Page

531

Last Page

537

Publisher

Bentham Science Publishers

ISSN

1570-1808

Abstract

Twenty- one alpha,beta-unsaturated ketone analogs of combretastatin-A4 (CA-4) that were designed for good solubility in aqueous media were synthesized. Compounds defined as Type A were derived from phenylacetone, in which subclass I contained ortho-, meta- or no substituents, sub-class II contained para-substituents, and sub-class III consisted of two substituents. Type B compounds were derived from cyclopropyl 2-fluorobenzyl ketone. The cis-configuration of the target compounds was ascertained through a single crystal X-ray crystallographic analysis of the fluorine-containing compound 8f. Five of the analogs, 8c, 8j and 8l of Type A and 9d and 9i of Type B, were shown to display modest cytotoxic potency (IC50 in the 3.8 - 21 mu M range) against the growth of murine melanoma (B16) and leukemia (L1210) cells in culture. Compounds 8j, 8l and 9i were further tested against MDA-MB-435 human melanoma cells. The cyclopropane-containing compound 9i was the most potent; with an IC50 value of 2.4 mu M. Even though no appreciable effects on interphase microtubules were observed when A-10 cells were treated with 30 mu M 8j or 8l, compound 9i caused extensive microtubule depolymerization at this concentration. These results suggest that compound 9i of Type B has a similar mechanism of action as CA-4 whilst compounds 8j and 8l of Type B are likely to have a different mechanism of action.

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