Modulation of ceramide-induced cell death and superoxide production by mitochondrial DNA-encoded respiratory chain defects in Rattus xenocybrid mouse cells

doi:10.1016/j.bbabio.2013.03.012

Biochimica et Biophysica Acta (BBA) - Bioenergetics

Volume 1827, Issue 7, July 2013, Pages 817-825

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Highlights

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Mouse fibroblasts with rat mtDNA (Rn xenocybrids) exhibit multiple OXPHOS defects.
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Ceramide inhibits complex III activity in Rn xenocybrids, inducing ROS production.
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Rn xenocybrids exhibit increased sensitivity to ceramide-induced cell death.

Abstract

Mitochondria play an integral role in cell death signaling, yet how mitochondrial defects disrupt this important function is not well understood. We have used a mouse L-cell fibroblast model harboring Rattus norvegicus mtDNA (Rn xenocybrids) to examine the effects of multiple oxidative phosphorylation (OXPHOS) defects on reactive oxygen species (ROS) generation and cell death signaling. Blue native-PAGE analyses of Rn xenocybrids revealed defects in OXPHOS complex biogenesis with reduced steady-state levels of complexes I, III and IV. Isolated Rn xenocybrid mitochondria exhibited deficiencies in complex II + III and III activities, with CIII-stimulated ROS generation 66% higher than in control mitochondria. Rn xenocybrid cells were resistant to staurosporine-induced cell death, but exhibited a four-fold increase in sensitivity to ceramide-induced cell death that was caspase-3 independent and did not induce chromosomal DNA degradation. Furthermore, ceramide directly inhibited Rn xenocybrid complex II + III activity by 97%, although this inhibition could be completely abolished by exogenous decylubiquinone. Ceramide also induced a further increase in ROS output from Rn xenocybrid complex III by 42%. These results suggest that the interaction of ceramide with OXPHOS complex III is significantly enhanced by the presence of the xenotypic Rattus cytochrome b in complex III, likely due to the increased affinity for ceramide at the ubiquinone binding site. We propose a novel mechanism of altered mitochondrial cell death signaling due to mtDNA mutations whereby ceramide directly induces OXPHOS complex ROS generation to initiate cell death pathways.

Abbreviations

mtDNA

mitochondrial DNA

OXPHOS

oxidative phosphorylation

ROS

reactive oxygen species

DCFH

2′,7′-dichlorodihydrofluoroscein

Rattus norvegicus

BN-PAGE

Blue native polyacrylamide gel electrophoresis

Keywords

Oxidative phosphorylation

Reactive oxygen species

Mitochondrial DNA

Ceramide

Mouse fibroblast

Mitochondrial disease

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¹: These authors contributed equally.