PIM1 Kinase Regulates Cell Death, Tumor Growth and Chemotherapy Response in Triple-negative Breast Cancer

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2016 Nov 8

PMID 27775704

Citations 122

Authors

Fara Braso-Maristany

Simone Filosto

Steven Catchpole

Rebecca Marlow

Jelmar Quist

Erika Francesch-Domenech

Darren A Plumb

Leila Zakka

Patrycja Gazinska

Gianmaria Liccardi

Pascal Meier

Albert Gris-Oliver

Maggie Chon U Cheang

Anna Perdrix-Rosell

Manar Shafat

Elodie Noel

Nirmesh Patel

Kristen McEachern

Maurizio Scaltriti

Pau Castel

Farzana Noor

Richard Buus

Sumi Mathew

Johnathan Watkins

Violeta Serra

Pierfrancesco Marra

Anita Grigoriadis

Andrew N Tutt

Affiliations

Soon will be listed here.

Abstract

Triple-negative breast cancers (TNBCs) have poor prognosis and lack targeted therapies. Here we identified increased copy number and expression of the PIM1 proto-oncogene in genomic data sets of patients with TNBC. TNBC cells, but not nonmalignant mammary epithelial cells, were dependent on PIM1 for proliferation and protection from apoptosis. PIM1 knockdown reduced expression of the anti-apoptotic factor BCL2, and dynamic BH3 profiling of apoptotic priming revealed that PIM1 prevents mitochondrial-mediated apoptosis in TNBC cell lines. In TNBC tumors and their cellular models, PIM1 expression was associated with several transcriptional signatures involving the transcription factor MYC, and PIM1 depletion in TNBC cell lines decreased, in a MYC-dependent manner, cell population growth and expression of the MYC target gene MCL1. Treatment with the pan-PIM kinase inhibitor AZD1208 impaired the growth of both cell line and patient-derived xenografts and sensitized them to standard-of-care chemotherapy. This work identifies PIM1 as a malignant-cell-selective target in TNBC and the potential use of PIM1 inhibitors for sensitizing TNBC to chemotherapy-induced apoptotic cell death.

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