1. Academic Validation
  2. An allosteric mechanism for potent inhibition of human ATP-citrate lyase

An allosteric mechanism for potent inhibition of human ATP-citrate lyase

  • Nature. 2019 Apr;568(7753):566-570. doi: 10.1038/s41586-019-1094-6.
Jia Wei 1 Silvana Leit 2 Jun Kuai 2 Eric Therrien 3 Salma Rafi 3 H James Harwood Jr 2 Byron DeLaBarre 2 Liang Tong 4
Affiliations

Affiliations

  • 1 Department of Biological Sciences, Columbia University, New York, NY, USA.
  • 2 Nimbus Therapeutics, Cambridge, MA, USA.
  • 3 Schrödinger, LLC, New York, NY, USA.
  • 4 Department of Biological Sciences, Columbia University, New York, NY, USA. ltong@columbia.edu.
Abstract

ATP-citrate lyase (ACLY) is a central metabolic Enzyme and catalyses the ATP-dependent conversion of citrate and coenzyme A (CoA) to oxaloacetate and acetyl-CoA1-5. The acetyl-CoA product is crucial for the metabolism of fatty acids6,7, the biosynthesis of Cholesterol8, and the acetylation and prenylation of proteins9,10. There has been considerable interest in ACLY as a target for anti-cancer drugs, because many Cancer cells depend on its activity for proliferation2,5,11. ACLY is also a target against dyslipidaemia and hepatic steatosis, with a compound currently in phase 3 clinical trials4,5. Many inhibitors of ACLY have been reported, but most of them have weak activity5. Here we report the development of a series of low nanomolar, small-molecule inhibitors of human ACLY. We have also determined the structure of the full-length human ACLY homo-tetramer in complex with one of these inhibitors (NDI-091143) by cryo-electron microscopy, which reveals an unexpected mechanism of inhibition. The compound is located in an allosteric, mostly hydrophobic cavity next to the citrate-binding site, and requires extensive conformational changes in the Enzyme that indirectly disrupt citrate binding. The observed binding mode is supported by and explains the structure-activity relationships of these compounds. This allosteric site greatly enhances the 'druggability' of ACLY and represents an attractive target for the development of new ACLY inhibitors.

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