Cell Death and Disease (Apr 2024)

Inhibition of acyl-CoA binding protein (ACBP) by means of a GABAARγ2-derived peptide

  • Gerasimos Anagnostopoulos,
  • Ester Saavedra,
  • Flavia Lambertucci,
  • Omar Motiño,
  • Jordan Dimitrov,
  • David Roiz-Valle,
  • Victor Quesada,
  • Karla Alvarez-Valadez,
  • Hui Chen,
  • Allan Sauvat,
  • Yan Rong,
  • Uxía Nogueira-Recalde,
  • Sijing Li,
  • Léa Montégut,
  • Mojgan Djavaheri-Mergny,
  • Maria Castedo,
  • Carlos Lopez-Otin,
  • Maria Chiara Maiuri,
  • Isabelle Martins,
  • Guido Kroemer

DOI
https://doi.org/10.1038/s41419-024-06633-6
Journal volume & issue
Vol. 15, no. 4
pp. 1 – 11

Abstract

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Abstract Acyl-CoA binding protein (ACBP) encoded by diazepam binding inhibitor (DBI) is an extracellular inhibitor of autophagy acting on the gamma-aminobutyric acid A receptor (GABAAR) γ2 subunit (GABAARγ2). Here, we show that lipoanabolic diets cause an upregulation of GABAARγ2 protein in liver hepatocytes but not in other major organs. ACBP/DBI inhibition by systemically injected antibodies has been demonstrated to mediate anorexigenic and organ-protective, autophagy-dependent effects. Here, we set out to develop a new strategy for developing ACBP/DBI antagonists. For this, we built a molecular model of the interaction of ACBP/DBI with peptides derived from GABAARγ2. We then validated the interaction between recombinant and native ACBP/DBI protein and a GABAARγ2-derived eicosapeptide (but not its F77I mutant) by pull down experiments or surface plasmon resonance. The GABAARγ2-derived eicosapeptide inhibited the metabolic activation of hepatocytes by recombinant ACBP/DBI protein in vitro. Moreover, the GABAARγ2-derived eicosapeptide (but not its F77I-mutated control) blocked appetite stimulation by recombinant ACBP/DBI in vivo, induced autophagy in the liver, and protected mice against the hepatotoxin concanavalin A. We conclude that peptidomimetics disrupting the interaction between ACBP/DBI and GABAARγ2 might be used as ACBP/DBI antagonists. This strategy might lead to the future development of clinically relevant small molecules of the ACBP/DBI system.