Laura Emionite, Fabia Galmozzi, Myriam Grattarola, Francesco Boccardo, Laura Vergani, Salvatore Toma
Index: Anticancer Res. 24(6) , 4019-24, (2004)
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Solid tumors develop resistance to retinoids during carcinogenesis. One of the strategies to overcome this resistance may include the combination of these molecules with other differentiating, cytotoxic or chromatin-remodelling agents. We analysed the anti-proliferative activity of two histone-deacetylase inhibitors (HDACIs), Trichostatin A (TSA) and sodium phenylbutyrate (PB), alone or combined with retinoids, all-trans retinoic acid (ATRA) and Ro 41-5253, on two human breast cancer cell lines: the hormone-dependent MCF-7 and the hormone-independent MDA-MB-231. These lines responded differently to retinoids: MCF-7 were sensitive, whilst MDA-MB-231 were rather resistant. When the retinoids were combined with HDACIs, these molecules potentiated the retinoid activity on growth inhibition, especially for the association Ro 41-5253 and TSA. By FACS analysis, we observed that the anti-proliferative effects were only partially due to pro-apopotic mechanisms, suggesting a cell-cycle block. The efficacy of the retinoids/HDACIs combinations could represent a new strategy in breast cancer chemotherapy, allowing inhibition of both ER + and ER- cell populations.
Structure | Name/CAS No. | Molecular Formula | Articles |
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Ro 41-5253
CAS:144092-31-9 |
C28H36O5S |
Effect of all-trans-retinoic acid on enterovirus 71 infectio...
2014-05-01 [Br. J. Nutr. 111(9) , 1586-93, (2014)] |
Retinoic acid inhibits in vivo interleukin-2 gene expression...
2009-04-01 [Immunology 126(4) , 514-22, (2009)] |
Overexpression of mucin genes induced by interleukin-1 beta,...
2002-06-01 [Exp. Lung Res. 28(4) , 315-32, (2002)] |
Retinoic acid signaling is necessary for the development of ...
1999-09-01 [Dev. Biol. 213(1) , 180-93, (1999)] |
Retinoids and human breast cancer: in vivo effects of an ant...
2005-02-28 [Cancer Lett. 219(1) , 27-31, (2005)] |
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