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Mitochondrial F-ATP Synthase Co-Migrating Proteins and Ca 2+ -Dependent Formation of Large Channels.

Anna B NikiforovaYulia L BaburinaMarina P BorisovaAlexey K SurinEkaterina S KharechkinaOlga V KrestininaMaria Y SuvorinaSvetlana A KruglovaAlexey G Kruglov
Published in: Cells (2023)
Monomers, dimers, and individual F O F 1 -ATP synthase subunits are, presumably, involved in the formation of the mitochondrial permeability transition pore (PTP), whose molecular structure, however, is still unknown. We hypothesized that, during the Ca 2+ -dependent assembly of a PTP complex, the F-ATP synthase (subunits) recruits mitochondrial proteins that do not interact or weakly interact with the F-ATP synthase under normal conditions. Therefore, we examined whether the PTP opening in mitochondria before the separation of supercomplexes via BN-PAGE will increase the channel stability and channel-forming capacity of isolated F-ATP synthase dimers and monomers in planar lipid membranes. Additionally, we studied the specific activity and the protein composition of F-ATP synthase dimers and monomers from rat liver and heart mitochondria before and after PTP opening. Against our expectations, preliminary PTP opening dramatically suppressed the high-conductance channel activity of F-ATP synthase dimers and monomers and decreased their specific "in-gel" activity. The decline in the channel-forming activity correlated with the reduced levels of as few as two proteins in the bands: methylmalonate-semialdehyde dehydrogenase and prohibitin 2. These results indicate that proteins co-migrating with the F-ATP synthase may be important players in PTP formation and stabilization.
Keyphrases
  • oxidative stress
  • heart failure
  • small molecule
  • atrial fibrillation
  • protein protein