AI Article Synopsis
- Curcumin has potential anticarcinogenic properties, but its specific mechanism and target receptor remain unclear.
- Studies on curcumin analogues reveal that curcumin acts as a bifunctional ligand, with some modifications making it less effective, while a specific derivative (compound 7) demonstrates superior ability to inhibit tubulin self-assembly.
- Fluorescence spectroscopy indicates that curcumin binds to tubulin away from the known colchicine-binding site, with docking studies suggesting a closer proximity to the vinblastine-binding site, while compound 7's tridented structure accounts for its stronger binding affinity.
Article Abstract
Although curcumin is known for its anticarcinogenic properties, the exact mechanism of its action or the identity of the target receptor is not completely understood. Studies on a series of curcumin analogues, synthesized to investigate their tubulin binding affinities and tubulin self-assembly inhibition, showed that: (i) curcumin acts as a bifunctional ligand, (ii) analogues with substitution at the diketone and acetylation of the terminal phenolic groups of curcumin are less effective, (iii) a benzylidiene derivative, compound 7, is more effective than curcumin in inhibiting tubulin self-assembly. Cell-based studies also showed compound 7 to be more effective than curcumin. Using fluorescence spectroscopy we show that curcumin binds tubulin 32 Å away from the colchicine-binding site. Docking studies also suggests that the curcumin-binding site to be close to the vinblastine-binding site. Structure-activity studies suggest that the tridented nature of compound 7 is responsible for its higher affinity for tubulin compared to curcumin.
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| http://dx.doi.org/10.1021/jm2004046 | DOI Listing |
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