Innate Immune Training of Human Macrophages by Cathelicidin Analogs
van Dijk, Albert; Anten, Jennifer; Bakker, Anne; Evers, Noah; Hoekstra, Anna T; Chang, Jung-Chin; Scheenstra, Maaike R; Veldhuizen, Edwin J A; Netea, Mihai G; Berkers, Celia R; Haagsman, Henk P
(2022) Frontiers in Immunology, volume 13, pp. 1 - 18
(Article)
Abstract
Trained innate immunity can be induced in human macrophages by microbial ligands, but it is unknown if exposure to endogenous alarmins such as cathelicidins can have similar effects. Previously, we demonstrated sustained protection against infection by the chicken cathelicidin-2 analog DCATH-2. Thus, we assessed the capacity of cathelicidins to induce
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trained immunity. PMA-differentiated THP-1 (dTHP1) cells were trained with cathelicidin analogs for 24 hours and restimulated after a 3-day rest period. DCATH-2 training of dTHP-1 cells amplified their proinflammatory cytokine response when restimulated with TLR2/4 agonists. Trained cells displayed a biased cellular metabolism towards mTOR-dependent aerobic glycolysis and long-chain fatty acid accumulation and augmented microbicidal activity. DCATH-2-induced trained immunity was inhibited by histone acetylase inhibitors, suggesting epigenetic regulation, and depended on caveolae/lipid raft-mediated uptake, MAPK p38 and purinergic signaling. To our knowledge, this is the first report of trained immunity by host defense peptides.
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Keywords: Seahorse analysis, cathelicidin, host defense peptide, immunomodulation, macrophage, metabolomics, trained immunity, Immunology and Allergy, Immunology
ISSN: 1664-3224
Publisher: Frontiers Media S.A.
Note: Funding Information: We kindly thank Dr. Richard Wubbolts and Dr. Soledad Ordonez from the Center for Cell Imaging (CCI), Faculty of Veterinary Medicine, Utrecht University for analysis of confocal data, Miranda van Triest from Universitair Medisch Centrum Utrecht (UMC Utrecht) for assistance with the Seahorse assay and the Utrecht Sequencing Facility (USEQ) for providing sequencing service and data. Funding Information: This work was supported by the Dutch Ministry of Economic Affairs via the Immuno Valley Alternatives to Antibiotics (ALTANT) program (Animal-Specific Immunomodulatory Antimicrobials 2 project), NWO-TTW grant 14924 to the Bac-Vactory program and a TKI-LSH allowance grant (project no. LSHM18040). MN was supported by an ERC Advanced Grant (#833247) and a Spinoza grant of the Netherlands Organization for Scientific Research. Publisher Copyright: Copyright © 2022 van Dijk, Anten, Bakker, Evers, Hoekstra, Chang, Scheenstra, Veldhuizen, Netea, Berkers and Haagsman.
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