Abstract
Simple SummaryThere is a critical need to identify readily translatable adjuncts to potentiate the dismal median survivals of only 15–20 months in glioblastoma (GBM) patients after standard of care, i.e., concurrent Temozolomide (TMZ) and radiation (XRT) therapy. Here we demonstrated that the Polo-like kinase 1 (PLK1) inhibitor volasertib, which has been employed in cancer clinical trials, has activity against GBM in the contexts of both as monotherapy and as an adjunct to standard of care (SOC). In addition to corroborating the known effects of volasertib, we found novel impacts of volasertib on mitochondrial membrane potential, ROS generation, persistent DNA damage and signaling pathways such as ERK/MAPK, AMPK and glucocorticoid receptor. Together these studies support the potential importance of PLK1 inhibitors as an adjunct to GBM SOC therapy that warrants further preclinical investigation.New strategies that improve median survivals of only ~15–20 months for glioblastoma (GBM) with the current standard of care (SOC) which is concurrent temozolomide (TMZ) and radiation (XRT) treatment are urgently needed. Inhibition of polo-like kinase 1 (PLK1), a multifunctional cell cycle regulator, overexpressed in GBM has shown therapeutic promise but has never been tested in the context of SOC. Therefore, we examined the mechanistic and therapeutic impact of PLK1 specific inhibitor (volasertib) alone and in combination with TMZ and/or XRT on GBM cells. We quantified the effects of volasertib alone and in combination with TMZ and/or XRT on GBM cell cytotoxicity/apoptosis, mitochondrial membrane potential (MtMP), reactive oxygen species (ROS), cell cycle, stemness, DNA damage, DNA repair genes, cellular signaling and in-vivo tumor growth. Volasertib alone and in combination with TMZ and/or XRT promoted apoptotic cell death, altered MtMP, increased ROS and G2/M cell cycle arrest. Combined volasertib and TMZ treatment reduced side population (SP) indicating activity against GBM stem-like cells. Volasertib combinatorial treatment also significantly increased DNA damage and reduced cell survival by inhibition of DNA repair gene expression and modulation of ERK/MAPK, AMPK and glucocorticoid receptor signaling. Finally, as observed in-vitro, combined volasertib and TMZ treatment resulted in synergistic inhibition of tumor growth in-vivo. Together these results identify new mechanisms of action for volasertib that provide a strong rationale for further investigation of PLK1 inhibition as an adjunct to current GBM SOC therapy.
Highlights
Glioblastoma (GBM) is the most lethal and primary malignant brain tumor with median survivals of 15–20 months [1,2]
BT115 cells were more resistant to TMZ and volasertib compared to commercial cell lines tested (Figure 1A)
Targeted therapeutic adjuncts to enhance current standard of care (SOC) therapy for GBM are urgently needed to improve the median survivals of 15–16 months with TMZ/XRT and 20 months with the addition of tumor treating fields [3]
Summary
Glioblastoma (GBM) is the most lethal and primary malignant brain tumor with median survivals of 15–20 months [1,2]. Introduced in 2005, concurrent temozolomide (TMZ) chemotherapy and radiation (XRT) remain the current standard of care (SOC) treatment for GBM [3] This paradigm increased median survival from ~12 to months compared with XRT alone [3] while the addition of tumor treating fields improves median survivals from to 20.9 months [4]. These incremental improvements underscore the urgent need to identify new targeted approaches to potentiate genotoxic TMZ/XRT SOC therapy [5]. We investigated the activity and mechanisms of action of one such candidate, volasertib, a selective polo-like kinase 1 (PLK1) inhibitor, as a targeted adjunct to potentiate SOC therapy in GBM
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