Further, treatment of CD133+ liver CSCs with the AKT1 inhibitor,

Further, treatment of CD133+ liver CSCs with the AKT1 inhibitor, along with doxorubicin or 5-fluorouracil, led to the complete inhibition of the preferential survival effect induced by CD133+ liver CSCs.30 Recently, Yamashita and colleagues have also identified a mechanism by which EpCAM+ liver CSCs are rendered sensitive to 5-fluorouracil chemotherapy. The receptor of oncostatin M (OSM), an interleukin 6-related cytokine that is known to induce the differentiation

of hepatoblasts into hepatocytes, was detected Doxorubicin in the majority of EpCAM+ liver CSCs. Based on this finding, the authors investigated the effect of OSM on EpCAM+ liver CSCs. The treatment of these cells find more with OSM enhanced the hepatocytic differentiation of EpCAM+ liver CSCs by inducing Stat3 activation, as determined by a decrease in the stem-cell related gene expression and a decrease in EpCAM, alpha fetoprotein and cytokeratin 19 protein expression, which was concomitant with an increase in albumin protein expression. Further, OSM-treated EpCAM+ liver CSCs showed enhanced cell proliferation with an expansion of the EpCAM- non-CSC population. The combination

of OSM treatment with 5-fluorouracil, which eradicated the EpCAM- non-CSCs, dramatically increased the number of apoptotic cells in vitro and suppressed tumor growth in vivo, when compared with either OSM or 5-fluorouracil treatment alone. Findings from the study suggest that OSM could be effectively used for the differentiation and active cell division of OSM receptor-positive EpCAM+ liver CSCs and that the combination of OSM and 5-fluorouracil can efficiently eliminate HCC by targeting both CSCs and non-CSCs subpopulations.31 Using chemotherapeutic drugs to select drug-resistant cancer cells in HCC, Wang et al. have demonstrated that chemoresistant cells display CSC-like features, including increased self-renewal ability, increased cell motility, PJ34 HCl resistance to multiple chemotherapeutic drugs, enhanced tumorigenic potential and elevated

expression of CD90+ cells. In addition, the expression of Oct4, a transcription factor essential in embryonic stem cells, was also strongly upregulated in the chemoresistant HCC cell subpopulation. The authors demonstrated that Oct4 plays a role in cancer cell chemoresistance through the following findings: (i) chemoresistant cancer cells displayed an enhanced expression of Oct4 through gene demethylation processes; (ii) the overexpression of Oct4 significantly increased, whereas the knockdown of Oct4 reduced the drug resistance of liver cancer cells in vitro and in vivo; and (iii) the overexpression of Oct4 induced the activation of TCL1, AKT and ABCG2 to mediate the chemoresistance.

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