Does Oxidation of Mitochondrial Cardiolipin Trigger a Chain of Antiapoptotic Reactions?

Autor(en): Mulkidjanian, A. Y.
Shalaeva, D. N.
Lyamzaev, K. G.
Chernyak, B. V.
Stichwörter: ADP/ATP CARRIER; Biochemistry & Molecular Biology; C/CARDIOLIPIN PEROXIDASE COMPLEXES; CELL-DEATH; CYTOCHROME-C RELEASE; ELECTRON-TRANSPORT CHAIN; FATTY-ACIDS; lipid peroxidation; membrane potential; mitochondria-targeted antioxidants; mitophagy; PERMEABILITY TRANSITION; proton leak; reactive oxygen species; RESPIRATORY SUPERCOMPLEXES; TARGETED ANTIOXIDANTS; UNCOUPLING PROTEINS
Erscheinungsdatum: 2018
Volumen: 83
Ausgabe: 10
Startseite: 1263
Seitenende: 1278
Oxidative stress causes selective oxidation of cardiolipin (CL), a fourtail lipid specific for the inner mitochondrial membrane. Interaction with oxidized CL transforms cytochrome c into peroxidase capable of oxidizing even more CL molecules. Ultimately, this chain of events leads to the pore formation in the outer mitochondrial membrane and release of mitochondrial proteins, including cytochrome c, into the cytoplasm. In the cytoplasm, cytochrome c promotes apoptosome assembly that triggers apoptosis (programmed cell death). Because of this amplification cascade, even an occasional oxidation of a single CL molecule by endogenously formed reactive oxygen species (ROS) might cause cell death, unless the same CL oxidation triggers a separate chain of antiapoptotic reactions that would prevent the CL-mediated apoptotic cascade. Here, we argue that the key function of CL in mitochondria and other coupling membranes is to prevent proton leak along the interface of interacting membrane proteins. Therefore, CL oxidation should increase proton permeability through the CL-rich clusters of membrane proteins (CL islands) and cause a drop in the mitochondrial membrane potential (MMP). On one hand, the MMP drop should hinder ROS generation and further CL oxidation in the entire mitochondrion. On the other hand, it is known to cause rapid fission of the mitochondrial network and formation of many small mitochondria, only some of which would contain oxidized CL islands. The fission of mitochondrial network would hinder apoptosome formation by preventing cytochrome c release from healthy mitochondria, so that slowly working protein quality control mechanisms would have enough time to eliminate mitochondria with the oxidized CL. Because of these two oppositely directed regulatory pathways, both triggered by CL oxidation, the fate of the cell appears to be determined by the balance between the CL-mediated proapoptotic and antiapoptotic reactions. Since this balance depends on the extent of CL oxidation, mito-chondria-targeted antioxidants might be able to ensure cell survival in many pathologies by preventing CL oxidation.
ISSN: 00062979
DOI: 10.1134/S0006297918100115

Show full item record

Google ScholarTM