Antimycin A mimics a cell-death-inducing Bcl-2 homology domain 3

Abstract

The Bcl-2-related survival proteins confer cellular resistance to a wide range of agents. Bcl-x_L-expressing hepatocyte cell lines are resistant to tumour necrosis factor and anti-cancer drugs, but are more sensitive than isogenic control cells to antimycin A, an inhibitor of mitochondrial electron transfer. Computational molecular docking analysis predicted that antimycin A interacts with the Bcl-2 homology domain 3 (BH3)-binding hydrophobic groove of Bcl-x_L. We demonstrate that antimycin A and a Bak BH3 peptide bind competitively to recombinant Bcl-2. Antimycin A and BH3 peptide both induce mitochondrial swelling and loss of ΔΨ_m on addition to mitochondria expressing Bcl-x_L. The 2-methoxy derivative of antimycin A₃ is inactive as an inhibitor of cellular respiration but still retains toxicity for Bcl-x_L⁺ cells and mitochondria. Finally, antimycin A inhibits the pore-forming activity of Bcl-x_L in synthetic liposomes, demonstrating that a small non-peptide ligand can directly inhibit the function of Bcl-2-related proteins.