[HTML][HTML] Suppression of GLI sensitizes medulloblastoma cells to mitochondria-mediated apoptosis

Z Lin, S Li, H Sheng, M Cai, LYS Ma, L Hu, S Xu… - Journal of cancer …, 2016 - Springer
Z Lin, S Li, H Sheng, M Cai, LYS Ma, L Hu, S Xu, LS Yu, N Zhang
Journal of cancer research and clinical oncology, 2016Springer
Purpose The sonic hedgehog (SHH) signalling pathway plays the important role in
medulloblastoma (MB). Altered GLI expression plays a key role in these processes, and the
inhibition of GLI may be a good cancer-targeted therapy. This study aimed to investigate
whether GANT61, a GLI inhibitor, may inhibit the SHH signalling pathway promoting cell
mitochondria-mediated apoptosis and enhance cisplatin apoptosis antineoplastic therapy.
Methods In our study, we determined the effect of GANT61-mediated inhibition of GLI in …
Purpose
The sonic hedgehog (SHH) signalling pathway plays the important role in medulloblastoma (MB). Altered GLI expression plays a key role in these processes, and the inhibition of GLI may be a good cancer-targeted therapy. This study aimed to investigate whether GANT61, a GLI inhibitor, may inhibit the SHH signalling pathway promoting cell mitochondria-mediated apoptosis and enhance cisplatin apoptosis antineoplastic therapy.
Methods
In our study, we determined the effect of GANT61-mediated inhibition of GLI in Daoy MB cells. Cells were treated with different concentrations of GANT61 alone or in combination with cisplatin. Cell proliferation was assessed with CCK-8 assays, and cell invasion and migration were performed using 8-µm transwell inserts. Cell apoptosis was assessed with flow cytometric analysis and rhodamine 123. qPCR was used to complete RNA experiments. Protein expression was assessed with Western blotting.
Results
The GANT61 significantly inhibited cell proliferation. GANT61 decreased the cell migration and invasion, impairing these crucial steps in tumour progression. Cell apoptosis was significantly increased in Daoy cells. Rhodamine 123 assay showed that GANT61 could decrease the mitochondrial membrane potential promoting cell mitochondria-mediated apoptosis. GANT61 inhibited the expression of GLI and Bcl-2 at both the mRNA and protein levels and might affect the expression of Bax, caspase-3 and caspase-9 to promote cell intrinsic apoptosis. Furthermore, GANT61 could enhance cisplatin-induced apoptosis to decrease the IC50 value of cisplatin. Finally, data suggest that GANT61 could enhance cisplatin-induced apoptosis through promoting the expression of Bax, caspase-3 and caspase-9 protein levels.
Conclusion
Our data suggest that the SHH signalling pathway plays an important role in MB. GLI is an oncogenic transcription factor in the SHH pathway, and targeting GLI with GANT61 results in favourable antitumour activity and targeted therapy.
Springer