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Mitochondrial damage-associated molecular patterns trigger arginase-dependent lymphocyte immunoregulation

Lauren P. Westhaver, Sarah Nersesian, Adam Nelson, Leah K. MacLean, Emily B. Carter, Derek Rowter, Jun Wang, Boris Gala-López, Andrew W. Stadnyk, Brent Johnston, Jeanette E. Boudreau

2022Cell Reports22 citationsDOIOpen Access PDF

Abstract

Tissue damage leads to loss of cellular and mitochondrial membrane integrity and release of damage-associated molecular patterns, including those of mitochondrial origin (mitoDAMPs). Here, we describe the lymphocyte response to mitoDAMPs. Using primary cells from mice and human donors, we demonstrate that natural killer (NK) cells and T cells adopt regulatory phenotypes and functions in response to mitoDAMPs. NK cell-mediated cytotoxicity, interferon gamma (IFN-γ) production, T cell proliferation, and in vivo anti-viral T cell activation are all interrupted in the presence of mitoDAMPs or mitoDAMP-rich irradiated cells in in vitro and in vivo assays. Mass spectrometry analysis of mitoDAMPs demonstrates that arginase and products of its enzymatic activity are prevalent in mitoDAMP preparations. Functional validation by arginase inhibition and/or arginine add-back shows that arginine depletion is responsible for the alteration in immunologic polarity. We conclude that lymphocyte responses to mitoDAMPs reflect a highly conserved mechanism that regulates inflammation in response to tissue injury.

Topics & Concepts

ArginaseLymphocyteBiologyMitochondrionCell biologyImmunologyGeneticsArginineAmino acidImmune cells in cancerTryptophan and brain disordersImmune Response and Inflammation
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