Author:
Herrle Niklas,Malacarne Pedro F.,Warwick Timothy,Cabrera-Orefice Alfredo,Chen Yiheng,Gheisari Maedeh,Chatterjee Souradeep,Leisegang Matthias S.,Sarakpi Tamim,Wionski Sarah,Lopez Melina,Koch Ina,Keßler Marcus,Klein Sabine,Uschner Frank Erhard,Trebicka Jonel,Brunst Steffen,Proschak Ewgenij,Günther Stefan,Rosas-Lemus Mónica,Baumgarten Nina,Klatt Stephan,Speer Thimoteus,Wittig Ilka,Schulz Marcel H.,Richards J. Brent,Gilsbach Ralf,Denton Travis T.,Fleming Ingrid,Hannibal Luciana,Brandes Ralf P.,Rezende Flávia
Abstract
SummaryOxidative stress is caused by short-lived molecules and metabolic changes belong to the fastest cellular responses. Here we studied how the endothelial cell metabolome reacts to acute oxidative challenges (menadione or H2O2) to identify redox-sensitive metabolic enzymes. H2O2selectively increased α-ketoglutaramate (αKGM), a largely uncharacterized metabolite produced by glutamine transamination and a yet unrecognized intermediate of endothelial glutamine catabolism. The enzyme nitrilase-like 2 ω-amidase (NIT2) converts αKGM to α-ketoglutarate (αKG). Reversible oxidation of specific cysteine in NIT2 by H2O2inhibited its catalytic activity. Furthermore, a variant in theNIT2gene that decreases its expression is associated with high plasma αKGM level in humans. Endothelial-specific knockout mice of NIT2 exhibited increased levels of αKGM and impaired angiogenesis. Knockout of NIT2 impaired endothelial cell proliferation and sprouting and induced senescence. In conclusion, we show that the glutamine transaminase-ω-amidase pathway is a metabolic switch in which NIT2 is the redox-sensitive enzyme. The pathway is modulated in humans and functionally important for endothelial glutamine metabolism.
Publisher
Cold Spring Harbor Laboratory