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AARS1 and AARS2 sense l-lactate to regulate cGAS as global lysine lactyltransferases.

Authors :
Li, Heyu
Liu, Chao
Li, Ran
Zhou, Lili
Ran, Yu
Yang, Qiqing
Huang, Huizhe
Lu, Huasong
Song, Hai
Yang, Bing
Ru, Heng
Lin, Shixian
Zhang, Long
Source :
Nature; Oct2024, Vol. 634 Issue 8036, p1229-1237, 9p
Publication Year :
2024

Abstract

l-lactate modifies proteins through lactylation1, but how this process occurs is unclear. Here we identify the alanyl-tRNA synthetases AARS1 and AARS2 (AARS1/2) as intracellular l-lactate sensors required for l-lactate to stimulate the lysine lactylome in cells. AARS1/2 and the evolutionarily conserved Escherichia coli orthologue AlaRS bind to l-lactate with micromolar affinity and they directly catalyse l-lactate for ATP-dependent lactylation on the lysine acceptor end. In response to l-lactate, AARS2 associates with cyclic GMP–AMP synthase (cGAS) and mediates its lactylation and inactivation in cells and in mice. By establishing a genetic code expansion orthogonal system for lactyl-lysine incorporation, we demonstrate that the presence of a lactyl moiety at a specific cGAS amino-terminal site abolishes cGAS liquid-like phase separation and DNA sensing in vitro and in vivo. A lactyl mimetic knock-in inhibits cGAS, whereas a lactyl-resistant knock-in protects mice against innate immune evasion induced through high levels of l-lactate. MCT1 blockade inhibits cGAS lactylation in stressed mice and restores innate immune surveillance, which in turn antagonizes viral replication. Thus, AARS1/2 are conserved intracellular l-lactate sensors and have an essential role as lactyltransferases. Moreover, a chemical reaction process of lactylation targets and inactivates cGAS.The tRNA synthases AARS1 and AARS2 are identified as evolutionarily conserved sensors of intracellular l-lactate to mediate the global lysine lactylome. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
00280836
Volume :
634
Issue :
8036
Database :
Complementary Index
Journal :
Nature
Publication Type :
Academic Journal
Accession number :
180649976
Full Text :
https://doi.org/10.1038/s41586-024-07992-y