CHK1-targeted therapy to deplete DNA replication-stressed, p53-deficient, hyperdiploid colorectal cancer stem cells

Gwenola Manic; Michele Signore; Antonella Sistigu; Giorgio Russo; Francesca Corradi; Silvia Siteni; Martina Musella; Sara Vitale; Maria Laura De Angelis; Matteo Pallocca; Carla Azzurra Amoreo; Francesca Sperati; Simone Di Franco; Sabina Barresi; Eleonora Policicchio; Gabriele De Luca; Francesca De Nicola; Marcella Mottolese; Ann Zeuner; Maurizio Fanciulli; Giorgio Stassi; Marcello Maugeri-Saccà; Marta Baiocchi; Marco Tartaglia; Ilio Vitale; Ruggero De Maria

doi:10.1136/gutjnl-2016-312623

CHK1-targeted therapy to deplete DNA replication-stressed, p53-deficient, hyperdiploid colorectal cancer stem cells

Gut. 2018 May;67(5):903-917. doi: 10.1136/gutjnl-2016-312623. Epub 2017 Apr 7.

Authors

Gwenola Manic^#¹, Michele Signore^#², Antonella Sistigu^#³, Giorgio Russo^{3

4}, Francesca Corradi¹, Silvia Siteni^{3

5}, Martina Musella^{3

6}, Sara Vitale⁴, Maria Laura De Angelis², Matteo Pallocca⁷, Carla Azzurra Amoreo⁸, Francesca Sperati⁹, Simone Di Franco¹⁰, Sabina Barresi¹¹, Eleonora Policicchio^{2

12}, Gabriele De Luca², Francesca De Nicola⁷, Marcella Mottolese⁸, Ann Zeuner², Maurizio Fanciulli⁷, Giorgio Stassi¹⁰, Marcello Maugeri-Saccà¹³, Marta Baiocchi², Marco Tartaglia¹¹, Ilio Vitale^#^{1

3}, Ruggero De Maria^#⁴

Affiliations

¹ Department of Biology, University of Rome "Tor Vergata", Rome, Italy.
² Department of Oncology and Molecular Medicine, Istituto Superiore di Sanità, Rome, Italy.
³ Department of Research, Advanced Diagnostics and Technological Innovation, Regina Elena National Cancer Institute, Rome, Italy.
⁴ Institute of General Pathology, Catholic University and A. Gemelli Polyclinic, Rome, Italy.
⁵ Department of Science, University "Roma Tre", Rome, Italy.
⁶ Department of Molecular Medicine, University "La Sapienza", Rome, Italy.
⁷ SAFU, Department of Research, Advanced Diagnostics, and Technological Innovation, Translational Research Area, Regina Elena National Cancer Institute, Rome Italy.
⁸ Department of Pathology, Regina Elena National Cancer Institute, Rome, Italy.
⁹ Biostatistical Unit, Regina Elena National Cancer Institute, Rome, Italy.
¹⁰ Department of Surgical Oncological and Stomatological Sciences, University of Palermo, Palermo, Italy.
¹¹ Genetics and Rare Diseases Research Division, Ospedale Pediatrico "Bambino Gesù", Rome, Italy.
¹² Department of Experimental Medicine, University "La Sapienza", Rome, Italy.
¹³ Division of Medical Oncology 2, Regina Elena National Cancer Institute, Rome, Italy.

^# Contributed equally.

Abstract

Objective: Cancer stem cells (CSCs) are responsible for tumour formation and spreading, and their targeting is required for tumour eradication. There are limited therapeutic options for advanced colorectal cancer (CRC), particularly for tumours carrying RAS-activating mutations. The aim of this study was to identify novel CSC-targeting strategies.

Design: To discover potential therapeutics to be clinically investigated as single agent, we performed a screening with a panel of FDA-approved or investigational drugs on primary CRC cells enriched for CSCs (CRC-SCs) isolated from 27 patients. Candidate predictive biomarkers of efficacy were identified by integrating genomic, reverse-phase protein microarray (RPPA) and cytogenetic analyses, and validated by immunostainings. DNA replication stress (RS) was increased by employing DNA replication-perturbing or polyploidising agents.

Results: The drug-library screening led to the identification of LY2606368 as a potent anti-CSC agent acting in vitro and in vivo in tumour cells from a considerable number of patients (∼36%). By inhibiting checkpoint kinase (CHK)1, LY2606368 affected DNA replication in most CRC-SCs, including RAS-mutated ones, forcing them into premature, lethal mitoses. Parallel genomic, RPPA and cytogenetic analyses indicated that CRC-SCs sensitive to LY2606368 displayed signs of ongoing RS response, including the phosphorylation of RPA32 and ataxia telangiectasia mutated serine/threonine kinase (ATM). This was associated with mutation(s) in TP53 and hyperdiploidy, and made these CRC-SCs exquisitely dependent on CHK1 function. Accordingly, experimental increase of RS sensitised resistant CRC-SCs to LY2606368.

Conclusions: LY2606368 selectively eliminates replication-stressed, p53-deficient and hyperdiploid CRC-SCs independently of RAS mutational status. These results provide a strong rationale for biomarker-driven clinical trials with LY2606368 in patients with CRC.

Keywords: CELL CYCLE CONTROL; CHEMOTHERAPY; COLORECTAL CANCER; DNA DAMAGE; DRUG DEVELOPMENT.

Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antineoplastic Agents / pharmacology*
Cell Line, Tumor
Checkpoint Kinase 1 / drug effects*
Checkpoint Kinase 1 / genetics
Colorectal Neoplasms / drug therapy*
Colorectal Neoplasms / genetics
DNA Replication / drug effects
Humans
Immunohistochemistry
Mutation
Neoplastic Stem Cells / drug effects*
Neoplastic Stem Cells / metabolism
Oligonucleotide Array Sequence Analysis
Pyrazines / pharmacology*
Pyrazoles / pharmacology*
Tumor Suppressor Protein p53 / genetics

Substances

Antineoplastic Agents
Pyrazines
Pyrazoles
Tumor Suppressor Protein p53
prexasertib
CHEK1 protein, human
Checkpoint Kinase 1