Inhibition of BUB1 Kinase by BAY 1816032 Sensitizes Tumor Cells Toward Taxanes, ATR, and PARP Inhibitors and

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2018 Nov 16

PMID 30429199

Citations 39

Authors

Gerhard Siemeister

Anne Mengel

Amaury E Fernandez-Montalvan

Wilhelm Bone

Jens Schroder

Sabine Zitzmann-Kolbe

Hans Briem

Stefan Prechtl

Simon J Holton

Ursula Monning

Oliver von Ahsen

Sandra Johanssen

Arwed Cleve

Vera Putter

Marion Hitchcock

Franz von Nussbaum

Michael Brands

Karl Ziegelbauer

Dominik Mumberg

Affiliations

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Abstract

Purpose: The catalytic function of BUB1 is required for chromosome arm resolution and positioning of the chromosomal passenger complex for resolution of spindle attachment errors and plays only a minor role in spindle assembly checkpoint activation. Here, we present the identification and preclinical pharmacologic profile of the first BUB1 kinase inhibitor with good bioavailability.

Experimental Design: The Bayer compound library was screened for BUB1 kinase inhibitors and medicinal chemistry efforts to improve target affinity and physicochemical and pharmacokinetic parameters resulting in the identification of BAY 1816032 were performed. BAY 1816032 was characterized for kinase selectivity, inhibition of BUB1 signaling, and inhibition of tumor cell proliferation alone and in combination with taxanes, ATR, and PARP inhibitors. Effects on tumor growth were evaluated using human triple-negative breast xenograft models.

Results: The highly selective compound BAY 1816032 showed long target residence time and induced chromosome mis-segregation upon combination with low concentrations of paclitaxel. It was synergistic or additive in combination with paclitaxel or docetaxel, as well as with ATR or PARP inhibitors in cellular assays. Tumor xenograft studies demonstrated a strong and statistically significant reduction of tumor size and excellent tolerability upon combination of BAY 1816032 with paclitaxel or olaparib as compared with the respective monotherapies.

Conclusions: Our findings suggest clinical proof-of-concept studies evaluating BAY 1816032 in combination with taxanes or PARP inhibitors to enhance their efficacy and potentially overcome resistance.

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