Frontiers in Molecular Biosciences (Apr 2022)

Structural Basis of Human Dimeric α-Amino-β-Carboxymuconate-ε-Semialdehyde Decarboxylase Inhibition With TES-1025

  • Michele Cianci,
  • Nicola Giacchè,
  • Lucia Cialabrini,
  • Andrea Carotti,
  • Paride Liscio,
  • Emiliano Rosatelli,
  • Francesca De Franco,
  • Massimiliano Gasparrini,
  • Janet Robertson,
  • Adolfo Amici,
  • Nadia Raffaelli,
  • Roberto Pellicciari

DOI
https://doi.org/10.3389/fmolb.2022.834700
Journal volume & issue
Vol. 9

Abstract

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Human α-amino-β-carboxymuconate-ε-semialdehyde decarboxylase (ACMSD) stands at a branch point of the de novo NAD+ synthesis pathway and plays an important role in maintaining NAD+ homeostasis. It has been recently identified as a novel therapeutic target for a wide range of diseases, including inflammatory, metabolic disorders, and aging. So far, in absence of potent and selective enzyme inhibitors, only a crystal structure of the complex of human dimeric ACMSD with pseudo-substrate dipicolinic acid has been resolved. In this study, we report the crystal structure of the complex of human dimeric ACMSD with TES-1025, the first nanomolar inhibitor of this target, which shows a binding conformation different from the previously published predicted binding mode obtained by docking experiments. The inhibitor has a Ki value of 0.85 ± 0.22 nM and binds in the catalytic site, interacting with the Zn2+ metal ion and with residues belonging to both chains of the dimer. The results provide new structural information about the mechanism of inhibition exerted by a novel class of compounds on the ACMSD enzyme, a novel therapeutic target for liver and kidney diseases.

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