ival gene programs we have put particular emphasis on the role of retinoid induced NF B cIAP2 signaling pathway on the sensitivity of breast cancer cells Gefitinib side effects towards chemotherapy. By comparing different breast cancer cell lines, we found that pretreatment with reti noic acid can antagonize chemotherapy induced cell death in a cell dependent manner, which correlates with the activation of NF B cIAP2 signaling pathway. Our data e clude cIAP2 and suggest that other regu lator of the NF B signaling pathway are targeted by retinoic acid to confer resistance to chemotherapy induced cell death. Results 9 cis retinoic acid induces either differentiation or cell death in breast cancer cells in a cell conte t dependent manner It is well established that the inhibition of breast cancer cell proliferation by retinoids is accomplished by block ing cell cycle progression in the G1 phase.
In order to find out whether there is a possible contribution of cell death to the antiproliferative effect of retinoids on breast cancer cells, we used a sensitive assay that measures the release of DNA fragments into the cytoplasm of cells. To ma imally activate the RAR R R heterodimer, we used the pan RAR and R R agonist 9 cis retinoic acid to establish cell death kinetics. As shown in Fig. 1A B, the treatment with 9 cis RA at a pharmacolo gical concentration of 10 6 M is able to induce apoptosis in a cell conte t specific manner. Indeed, while 9 cis RA treatment does not significantly affect viability of T47D cells, it is able to induce apoptosis in the breast cancer cell line H3396.
Induction of apoptosis by 9 cis RA in this cell line requires RAR since treatment with a pan RAR antagonist, BMS493, blocks retinoid mediated apoptosis. That this block is partial may indi cate a possible contribution of alternative re inoid induced death pathways which have been previously reported. In these cells, mitochondrial membrane depolarization a key event in apoptosis is also induced by 9 cis RA or by the Batimastat RAR pan agonist all trans retinoic acid. As shown in Fig. 1D, 9 cis RA treatment clearly increases the number of cells pre senting a diminished mitochondrial membrane potential in a time dependent manner, and causes the release of the apoptogenic factors cytochrome c and SMAC DIA BLO from the mitochondria to the cytosol.
Also, 9 cis RA activates caspases 8 and 9 and the clea vage of a caspase 3 substrate, PARP, as assessed by wes tern blot in H3396 cells. When H3396 selleckchem Cabozantinib cells were treated with TRAIL as positive control for the e trinsic death pathway, both caspase 8 and caspase 9 were activated and led to PARP cleavage. Together, these data show that retinoid induced cell death in H3396 cells involves a crosstalk between the e trinsic and intrinsic death pathways. In contrast to H3396, T47D cell growth was inhibited without loss of viability after 6 days of 1 uM 9 cis RA treatment. Rather than inducing apoptosis, 9 cis RA treated T47D cells showed an increase in lipid droplet accumulation i