RESUMO
The aim of the present study was to demonstrate that ivermectin preferentially inhibited cancer stemlike cells (CSC) in breast cancer cells and downregulated the expression of 'stemness' genes. Computational searching of DrugBank, a database of approved drugs, was performed using the principles of twodimensional similarity searching; the chemical structure of salinomycin was used as a query. Growth inhibition of the breast cancer cell lin e MDAMB231 by ivermectin was investigated in the total cell population, in cell spheroids and in sorted cells that expressed cluster of differentiation (CD)44+/CD24. The effects of ivermectin treatment on the expression of pluripotency and selfrenewal transcription factors, such as homeobox protein nanog (nanog), octamerbinding protein 4 (oct4) and SRYbox 2 (sox2), were evaluated by reverse transcriptionquantitative polymerase chain reaction and western blotting. Ivermectin exhibited a similarity value of 0.78 in reference to salinomycin. Ivermectin demonstrated an inhibitory effect upon the growth of MDAMB231 cells in the range of 0.28 µM. Ivermectin preferentially inhibits the viability of CSCenriched populations (CD44+/CD24 and cells growing in spheroids) compared with the total cell population. The opposite pattern was observed with paclitaxel treatment. Ivermectin exposure reduced the expression of nanog, oct4 and sox2 at the mRNA and protein levels. Ivermectin preferentially inhibited the CSC subpopulation in the MDAMB231 cells and downregulated the expression of genes involved in the maintenance of pluripotency and selfrenewal.