Cell growth potential drives ferroptosis susceptibility in rhabdomyosarcoma and myoblast cell lines

Silvia Codenotti; Maura Poli; Michela Asperti; Daniela Zizioli; Francesco Marampon; Alessandro Fanzani

doi:10.1007/s00432-018-2699-0

Cell growth potential drives ferroptosis susceptibility in rhabdomyosarcoma and myoblast cell lines

J Cancer Res Clin Oncol. 2018 Sep;144(9):1717-1730. doi: 10.1007/s00432-018-2699-0. Epub 2018 Jul 3.

Authors

Silvia Codenotti¹, Maura Poli¹, Michela Asperti¹, Daniela Zizioli¹, Francesco Marampon², Alessandro Fanzani³

Affiliations

¹ Division of Biotechnology, Department of Molecular and Translational Medicine, University of Brescia, Brescia, Italy.
² Division of Radiation Oncology, Department of Biotechnological and Applied Clinical Sciences, University of L'Aquila, L'Aquila, Italy.
³ Division of Biotechnology, Department of Molecular and Translational Medicine, University of Brescia, Brescia, Italy. alessandro.fanzani@unibs.it.

PMID: 29971532
DOI: 10.1007/s00432-018-2699-0

Abstract

Purpose: Ferroptosis is a programmed form of iron-dependent cell death caused by lipid hydroperoxide accumulation, which can be prevented by glutathione peroxidase 4 (GPx4) activity. Here we investigated the effects of ferroptosis inducers called erastin and RSL3, which act by glutathione depletion and GPx4 inactivation, respectively, on muscle-derived cell lines of embryonal and alveolar rhabdomyosarcoma (RMS), and mouse normal skeletal C2C12 myoblasts.

Methods: Myogenic lines were exposed to stepwise increasing concentrations of ferroptosis inducers either alone or in combination with iron supplementation, iron chelating agents (bathophenanthrolinedisulfonic acid, BPS), antioxidant molecules (glutathione, N-acetylcysteine), lipid peroxidation inhibitors (ferrostatin-1), and chemotherapeutic agents (doxorubicin and actinomycin D). Drug susceptibility was quantified by measuring cell viability, proliferation and differentiation via neutral red assay, crystal violet assay and Giemsa staining, respectively. The detection of lipid hydroperoxide and protein levels was performed by immunofluorescence and Western blot analysis, respectively.

Results: Erastin and RSL3 increased lipid hydroperoxide levels preferentially in the embryonal U57810 and myoblast C2C12 lines, leading to ferroptosis that was accentuated by iron supplementation or prevented by co-treatment with BPS, glutathione, N-acetylcysteine and ferrostatin-1. The inhibition of extracellular regulated kinases (ERK) pathway prevented ferroptosis in U57810 and C2C12 cells, whereas its increased activation in the embryonal RD cells mediated by caveolin-1 (Cav-1) overexpression led to augmented ferroptosis susceptibility. Finally, we observed the combination of erastin or RSL3 with chemotherapeutic doxorubicin and actinomycin D agents to be effective in increasing cell death in all RMS lines.

Conclusions: Erastin and RSL3 trigger ferroptosis in highly proliferating myogenic lines through a ERK pathway-dependent fashion.

Keywords: Erastin; Ferroptosis; GPx4; Iron; RSL3; Rhabdomyosarcoma.

MeSH terms

Animals
Carbolines / pharmacology
Cell Death / drug effects
Cell Death / physiology*
Cell Line
Cell Line, Tumor
Cell Proliferation / drug effects
Cell Proliferation / physiology*
Cyclohexylamines / pharmacology
Dactinomycin / pharmacology
Doxorubicin / pharmacology
Glutathione / metabolism
Glutathione Peroxidase / metabolism
Humans
Lipid Peroxidation / drug effects
Lipid Peroxidation / physiology
Mice
Myoblasts / drug effects
Myoblasts / metabolism
Myoblasts / pathology*
Phenylenediamines / pharmacology
Piperazines / pharmacology
Rhabdomyosarcoma / drug therapy
Rhabdomyosarcoma / metabolism
Rhabdomyosarcoma / pathology*

Substances

Carbolines
Cyclohexylamines
Phenylenediamines
Piperazines
RSL3 compound
erastin
ferrostatin-1
Dactinomycin
Doxorubicin
Glutathione Peroxidase
Glutathione