Nature Communications (Apr 2023)

Allosteric role of the citrate synthase homology domain of ATP citrate lyase

  • Xuepeng Wei,
  • Kollin Schultz,
  • Hannah L. Pepper,
  • Emily Megill,
  • Austin Vogt,
  • Nathaniel W. Snyder,
  • Ronen Marmorstein

DOI
https://doi.org/10.1038/s41467-023-37986-9
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 11

Abstract

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Abstract ATP citrate lyase (ACLY) is the predominant nucleocytosolic source of acetyl-CoA and is aberrantly regulated in many diseases making it an attractive therapeutic target. Structural studies of ACLY reveal a central homotetrameric core citrate synthase homology (CSH) module flanked by acyl-CoA synthetase homology (ASH) domains, with ATP and citrate binding the ASH domain and CoA binding the ASH-CSH interface to produce acetyl-CoA and oxaloacetate products. The specific catalytic role of the CSH module and an essential D1026A residue contained within it has been a matter of debate. Here, we report biochemical and structural analysis of an ACLY-D1026A mutant demonstrating that this mutant traps a (3S)-citryl-CoA intermediate in the ASH domain in a configuration that is incompatible with the formation of acetyl-CoA, is able to convert acetyl-CoA and OAA to (3S)-citryl-CoA in the ASH domain, and can load CoA and unload acetyl-CoA in the CSH module. Together, this data support an allosteric role for the CSH module in ACLY catalysis.