Nature Communications (May 2024)

Active site remodeling in tumor-relevant IDH1 mutants drives distinct kinetic features and potential resistance mechanisms

  • Matthew Mealka,
  • Nicole A. Sierra,
  • Diego Avellaneda Matteo,
  • Elene Albekioni,
  • Rachel Khoury,
  • Timothy Mai,
  • Brittany M. Conley,
  • Nalani J. Coleman,
  • Kaitlyn A. Sabo,
  • Elizabeth A. Komives,
  • Andrey A. Bobkov,
  • Andrew L. Cooksy,
  • Steve Silletti,
  • Jamie M. Schiffer,
  • Tom Huxford,
  • Christal D. Sohl

DOI
https://doi.org/10.1038/s41467-024-48277-2
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 16

Abstract

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Abstract Mutations in human isocitrate dehydrogenase 1 (IDH1) drive tumor formation in a variety of cancers by replacing its conventional activity with a neomorphic activity that generates an oncometabolite. Little is understood of the mechanistic differences among tumor-driving IDH1 mutants. We previously reported that the R132Q mutant unusually preserves conventional activity while catalyzing robust oncometabolite production, allowing an opportunity to compare these reaction mechanisms within a single active site. Here, we employ static and dynamic structural methods and observe that, compared to R132H, the R132Q active site adopts a conformation primed for catalysis with optimized substrate binding and hydride transfer to drive improved conventional and neomorphic activity over R132H. This active site remodeling reveals a possible mechanism of resistance to selective mutant IDH1 therapeutic inhibitors. This work enhances our understanding of fundamental IDH1 mechanisms while pinpointing regions for improving inhibitor selectivity.