Objective:

To determine whether co-inhibition of CK1ε and PIK3CB/p110β is an effective therapeutic treatment for Glioblastoma (GBM).

Background:

GBM remains the most common and malignant brain cancer in adults with dismal prognosis, largely due to lack of effective treatments. CK1ε and PIK3CB/p110β have been identified as GBM survival kinase genes. CK1ε promotes growth of GBM cells by inhibiting β-catenin. However, blocking CK1ε alone fails to completely block tumor growth perhaps because β-catenin can be regulated by other kinases, including PIK3CB/p110β. It is possible that blocking either CK1ε or PIK3CB/p110β alone does not substantially activate β-catenin to induce massive GBM cell death, thus limiting their therapeutic efficacy as a single agent. It is therefore imperative to investigate if co-targeting CK1ε and PIK3CB/p110β yields synergistic inhibitory effects on GBM cell growth.

Design/Methods:

GBM cells were treated with either DMSO (control), IC261 (chemical inhibitor of CK1ε), GSK2636771 (chemical inhibitor of PIK3CB/p110β), or both IC261 and GSK2636771. Cell viability was measured using the MTS viability assay.

Results:

Cell viability for the treatment groups were as follows: GSK2636771 (95.76%), IC261 (61.84%), and combination of GSK2636771+IC261 (41.70%). Statistical analysis of drug synergy using the Bliss independence model yielded an Excess Over Bliss score greater than 0%, indicating a synergistic effect.

Conclusions: