Long-term cultivation using ineffective MDM2 inhibitor concentrations alters the drug sensitivity profiles of PL21 leukaemia cells

Martin Michaelis; Florian Rothweiler; Constanze Schneider; Tamara Rothenburger; Marco Mernberger; Andrea Nist; Thorsten Stiewe; Jindrich Cinatl; Michael Nevels

doi:10.1017/exp.2019.1

Experimental Results (Jan 2020)

Long-term cultivation using ineffective MDM2 inhibitor concentrations alters the drug sensitivity profiles of PL21 leukaemia cells

Martin Michaelis,
Florian Rothweiler,
Constanze Schneider,
Tamara Rothenburger,
Marco Mernberger,
Andrea Nist,
Thorsten Stiewe,
Jindrich Cinatl,
Michael Nevels

Affiliations

Martin Michaelis: Industrial Biotechnology Centre and School of Biosciences, University of Kent, CanterburyCT2 7NJ, UK
Florian Rothweiler: Institut für Medizinische Virologie, Klinikum der Goethe-Universität, Paul Ehrlich-Str. 40, 60596Frankfurt am Main, Germany
Constanze Schneider: Institut für Medizinische Virologie, Klinikum der Goethe-Universität, Paul Ehrlich-Str. 40, 60596Frankfurt am Main, Germany
Tamara Rothenburger: Institut für Medizinische Virologie, Klinikum der Goethe-Universität, Paul Ehrlich-Str. 40, 60596Frankfurt am Main, Germany
Marco Mernberger: Institute of Molecular Oncology, Philipps-University, 35037Marburg, Germany
Andrea Nist: Genomics Core Facility, Philipps-University, 35037Marburg, Germany
Thorsten Stiewe: Institute of Molecular Oncology, Philipps-University, 35037Marburg, Germany Genomics Core Facility, Philipps-University, 35037Marburg, Germany
Jindrich Cinatl: Institut für Medizinische Virologie, Klinikum der Goethe-Universität, Paul Ehrlich-Str. 40, 60596Frankfurt am Main, Germany
Michael Nevels: University of St Andrews, Biomolecular Sciences Building, Fife, United Kingdom of Great Britain and Northern Ireland, KY16 9ST

DOI: https://doi.org/10.1017/exp.2019.1
Journal volume & issue: Vol. 1

Abstract

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Acquired MDM2 inhibitor resistance is commonly caused by loss-of-function TP53 mutations. In addition to the selection of TP53-mutant cells by MDM2 inhibitors, MDM2 inhibitor-induced DNA damage may promote the formation of TP53 mutations. Here, we cultivated 12 sublines of the intrinsically MDM2 inhibitor-resistant TP53 wild-type acute myeloid leukaemia cell line PL21 for 52 passages in the presence of ineffective concentrations of the MDM2 inhibitor nutlin-3 but did not observe loss-of-function TP53 mutations. This suggests that MDM2 inhibitors select TP53-mutant cells after mutations have occurred, but do not directly promote TP53 mutations. Unexpectedly, many sublines displayed increased sensitivity to the anti-cancer drugs cytarabine, doxorubicin, or gemcitabine. Consequently, therapies can affect the outcome of next-line treatments, even in the absence of a therapy response. This finding is conceptually novel. A better understanding of such processes will inform the design of improved therapy protocols in the future.

Published in Experimental Results

ISSN: 2516-712X (Online)
Publisher: Cambridge University Press
Country of publisher: United Kingdom
LCC subjects: Technology; Medicine; Science
Website: https://www.cambridge.org/core/journals/experimental-results

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