The benzophenanthridine alkaloid sanguinarine perturbs microtubule assembly dynamics through tubulin binding. A possible mechanism for its antiproliferative activity.

Manu Lopus, Dulal Panda

School of Biosciences and Bioengineering, Indian Institute of Technology Bombay, India.

Journal Article: FEBS Journal (impact factor: 3.04). 05/2006; 273(10):2139-50. DOI: 10.1111/j.1742-4658.2006.05227.x

Abstract

Sanguinarine has been shown to inhibit proliferation of several types of human cancer cell including multidrug-resistant cells, whereas it has minimal cytotoxicity against normal cells such as neutrophils and keratinocytes. By analyzing the antiproliferative activity of sanguinarine in relation to its effects on mitosis and microtubule assembly, we found that it inhibits cancer cell proliferation by a novel mechanism. It inhibited HeLa cell proliferation with a half-maximal inhibitory concentration of 1.6 +/- 0.1 microM. In its lower effective inhibitory concentration range, sanguinarine depolymerized microtubules of both interphase and mitotic cells and perturbed chromosome organization in mitotic HeLa cells. At concentrations of 2 microM, it induced bundling of interphase microtubules and formation of granular tubulin aggregates. A brief exposure of HeLa cells to sanguinarine caused irreversible depolymerization of the microtubules, inhibited cell proliferation, and induced cell death. However, in contrast with several other microtubule-depolymerizing agents, sanguinarine did not arrest cell cycle progression at mitosis. In vitro, low concentrations of sanguinarine inhibited microtubule assembly. At higher concentrations (> 40 microM), it altered polymer morphology. Further, it induced aggregation of tubulin in the presence of microtubule-associated proteins. The binding of sanguinarine to tubulin induces conformational changes in tubulin. Together, the results suggest that sanguinarine inhibits cell proliferation at least in part by perturbing microtubule assembly dynamics.

Source: PubMed

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Keywords

brief exposure
 
granular tubulin aggregates
 
higher concentrations
 
human cancer cell
 
induced cell death
 
inhibited cell proliferation
 
interphase microtubules
 
irreversible depolymerization
 
low concentrations
 
microtubule-associated proteins
 
microtubules
 
mitotic HeLa cells
 
multidrug-resistant cells
 
novel mechanism
 
perturbed chromosome organization
 
perturbing microtubule assembly dynamics
 
sanguinarine depolymerized microtubules
 
sanguinarine inhibited microtubule assembly
 
sanguinarine inhibits cell proliferation
 
tubulin induces conformational changes