PuSH - Publication Server of Helmholtz Zentrum München: Antioxidant defense in quiescent cells determines selectivity of electron transport chain inhibition-induced cell death.

Navigation

Home

Deutsch

Research

Advanced Search

Browse by ...

... Journal

... Publication Type

... Research Data

... Publication Year

Publication overview

Support & Contact

Contact persons

Help

Data protection

Blecha, J.* ; Novais, S.M.* ; Rohlenova, K.* ; Novotna, E.* ; Lettlova, S.* ; Schmitt, S.* ; Zischka, H. ; Neuzil, J.* ; Rohlena, J.*

Antioxidant defense in quiescent cells determines selectivity of electron transport chain inhibition-induced cell death.

Free Radical Biol. Med. 112, 253-266 (2017)

DOI

PMC

Open Access Green as soon as Postprint is submitted to ZB.

Abstract
Metrics
Extra information

Mitochondrial electron transport chain (ETC) targeting shows a great promise in cancer therapy. It is particularly effective in tumors with high ETC activity where ETC-derived reactive oxygen species (ROS) are efficiently induced. Why modern ETC-targeted compounds are tolerated on the organismal level remains unclear. As most somatic cells are in non-proliferative state, the features associated with the ETC in quiescence could account for some of the specificity observed. Here we report that quiescent cells, despite increased utilization of the ETC and enhanced supercomplex assembly, are less susceptible to cell death induced by ETC disruption when glucose is not limiting. Mechanistically, this is mediated by the increased detoxification of ETC-derived ROS by mitochondrial antioxidant defense, principally by the superoxide dismutase 2 - thioredoxin axis. In contrast, under conditions of glucose limitation, cell death is induced preferentially in quiescent cells and is correlated with intracellular ATP depletion but not with ROS. This is related to the inability of quiescent cells to compensate for the lost mitochondrial ATP production by the upregulation of glucose uptake. Hence, elevated ROS, not the loss of mitochondrially-generated ATP, are responsible for cell death induction by ETC disruption in ample nutrients condition, e.g. in well perfused healthy tissues, where antioxidant defense imparts specificity. However, in conditions of limited glucose, e.g.in poorly perfused tumors, ETC disruption causes rapid depletion of cellular ATP, optimizing impact towards tumor-associated dormant cells. In summary, we propose that antioxidant defense in quiescent cells is aided by local glucose limitations to ensure selectivity of ETC inhibition-induced cell death.

Altmetric

Additional Metrics?

[➜Log in]

Edit extra informations Login

Publication type Article: Journal article

Document type Scientific Article

Corresponding Author

Keywords Electron Transport Chain ; Sod2 ; Antioxidant Defense ; Supercomplexes ; Thioredoxin; Manganese Superoxide-dismutase; Alpha-tocopheryl Succinate; Pancreatic-cancer Cells; Thioredoxin Reductase; Oxidative Stress; Respiratory Supercomplexes; Mitochondrial Thioredoxin; Glutathione-peroxidase; Cultured-cells; Apoptosis

ISSN (print) / ISBN 0891-5849

e-ISSN 1873-4596

Journal Free Radical Biology and Medicine

Quellenangaben Volume: 112, Pages: 253-266

Publisher Elsevier

Publishing Place New York, NY

Non-patent literature Publications

Reviewing status Peer reviewed

Institute(s) Institute of Molecular Toxicology and Pharmacology (TOXI)