Characterization of acquired nutlin-3 resistant non-small cell lung cancer cells

Deben, Christophe; Freire Boullosa, Laurie; Domen, Andreas; Wouters, An; Cuypers, Bart; Laukens, Kris; Lardon, Filip; Pauwels, Patrick

doi:10.20517/CDR.2020.91

Title

Characterization of acquired nutlin-3 resistant non-small cell lung cancer cells

Author

Deben, Christophe

Freire Boullosa, Laurie

Domen, Andreas

Wouters, An

Cuypers, Bart

Laukens, Kris

Lardon, Filip

Pauwels, Patrick

Abstract

Aim: The purpose of this manuscript is to study the potential characteristics of acquired nutlin-3 resistant non-small cell lung cancer cells (NSCLC). Nutlin-3 is an inhibitor of the murine-double minute 2 protein, the main negative regulator of wild type p53, of which several derivatives are currently in clinical development. Methods: A549 NSCLC cells were exposed to increasing concentrations of nutlin-3 for a period of 18 weeks. Monoclonal derivates were cultured, and the most resistance subclone was selected for whole transcriptome analysis. Gene set enrichment analysis was performed on differentially expressed genes between A549 nutlin-3 resistant cancer cells and the parental A549 p53 wild type cancer cells. Relevant findings were validated at the gene, protein and/or functional level. Results: All nutlin-3 resistant subclones acquired mutations in the TP53 gene, resulting in overexpression of the mutant p53 protein. The most resistant subclone was enriched for genes related to epithelial to mesenchymal transition (EMT), resulting in increased migratory and invasive potential. Furthermore, these cells were enriched in genes related to inflammation, tissue remodelling, and angiogenesis. Importantly, expression of several immune checkpoints, including PD-L1 and PD-L2, was significantly upregulated, and cisplatin-induced cell death was reduced. Conclusion: Transcriptome analysis of a highly nutlin-3 resistant A549 subclone shows the relevance of studying (1) resistance to standard of care chemotherapy; (2) secretion of immunomodulating chemo- and cytokines; (3) immune checkpoint expression; and (4) EMT and invasion in nutlin-3 resistant cancer cells in addition to acquired mutations in the TP53 gene.

Language

English

Publication

2021

DOI

10.20517/CDR.2020.91

Volume/pages

4 :1 (2021) , p. 233-243

ISI

000848730500013

Pubmed ID

35582010

Full text (Publisher's DOI)

https://doi.org/10.20517/CDR.2020.91

Full text (open access)

Licensed under a CC BY Attribution license

Faculty/Department				Faculty of Sciences. Mathematics and Computer Science Faculty of Medicine and Health Sciences

Research group				ADReM Data Lab (ADReM) Center for Oncological Research (CORE)
Project info				Exploring the potential and underlying mechanisms of therapeutic activation of p53 in combination with immunotherapy to stimulate an innate immune response against non-small cell lung cancer. Targeting Polo-like kinase 1 for treatment of NSCLC patients: focus on the induction of cellular senescence, the TP53 status and hypoxia.
Publication type				A1 Journal article

Subject				Human medicine

Affiliation				Publications with a UAntwerp address

Web of Science

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Identifier

Creation

16.02.2021

Last edited

30.08.2024

To cite this reference

https://hdl.handle.net/10067/1754270151162165141