Polo-like-kinase 1 (PLK-1) and c-myc inhibition with the dual kinase-bromodomain inhibitor volasertib in aggressive lymphomas.

Carlos Murga-Zamalloa,Nathanael G Bailey,Pinki Chowdhury,Avery Polk,Ryan A Wilcox,Tianjiao Wang,Tycel Phillips,Sumana Devata,Pradeep Poonnen,Kedar V Inamdar,Juan Gomez-Gelvez,Noah Brown,Alexandra C Hristov,Walter Hanel

doi:10.18632/oncotarget.22967

Carlos Murga-Zamalloa, Nathanael G Bailey + Show 12 more

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https://doi.org/10.18632/oncotarget.22967

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Survival following anthracycline-based chemotherapy remains poor among patients with most T-cell lymphoproliferative disorders. This may be attributed, at least in part, to cell-autonomous mechanisms of chemotherapy resistance observed in these lymphomas, including the loss of important tumor suppressors and the activation of signaling cascades that culminate in the expression and activation of transcription factors promoting cell growth and survival. Therefore, the identification of novel therapeutic targets is needed. In an effort to identify novel tumor dependencies, we performed a loss-of-function screen targeting ≈500 kinases and identified polo-like kinase 1 (PLK-1). This kinase has been implicated in the molecular cross-talk with important oncogenes, including c-Myc, which is itself an attractive therapeutic target in subsets of T-cell lymphomas and in high-grade (“double hit”) diffuse large B-cell lymphomas. We demonstrate that PLK-1 expression is prevalent among these aggressive lymphomas and associated with c-myc expression. Importantly, PLK-1 inhibtion with the PLK-1 inhibitor volasertib significantly reduced downstream c-myc phosphorylation and impaired BRD4 binding to the c-myc gene, thus inhibiting c-myc transcription. Therefore, volasertib led to a nearly complete loss of c-myc expression in cell lines and tumor xenografts, induced apoptosis, and thus warrants further investigation in these aggressive lymphomas.

Highlights

Progression-free survival following anthracyclinebased multi-agent chemotherapy remains poor among patients with most T-cell lymphoproliferative disorders and high-risk subsets of aggressive B-cell lymphomas
We demonstrate that pololike kinase 1 (PLK-1) expression is prevalent among these aggressive lymphomas and associated with c-myc expression
This may be attributed, at least in part, to cell-autonomous mechanisms of chemotherapy resistance observed in these lymphomas, including the loss of important tumor suppressors and the activation of signaling cascades that culminate in the activation of transcription factors that instigate the expression of genes that promote cell growth and survival, and confer resistance to chemotherapy

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Introduction

Progression-free survival following anthracyclinebased multi-agent chemotherapy remains poor among patients with most T-cell lymphoproliferative disorders and high-risk subsets of aggressive B-cell lymphomas. This may be attributed, at least in part, to cell-autonomous mechanisms of chemotherapy resistance observed in these lymphomas, including the loss of important tumor suppressors and the activation of signaling cascades that culminate in the expression and activation of transcription factors promoting cell growth and survival.

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