TREML4 Promotes Inflammatory Programs in Human and Murine Macrophages and Alters Atherosclerosis Lesion Composition in the Apolipoprotein E Deficient Mouse

The Triggering Receptor Expressed on Myeloid cells-like 4 (TREML4) is a member of the TREM receptor family, known modulators of inflammatory responses. We have previously found that TREML4 expression positively correlates with human coronary arterial calcification (CAC). However, the role of TREML4...

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Autores principales: Gonzalez-Cotto, Marieli, Guo, Liang, Karwan, Megan, Sen, Shurjo K., Barb, Jennifer, Collado, Carlos J., Elloumi, Fathi, Palmieri, Erika M., Boelte, Kimberly, Kolodgie, Frank D., Finn, Aloke V., Biesecker, Leslie G., McVicar, Daniel W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7133789/
https://www.ncbi.nlm.nih.gov/pubmed/32292401
http://dx.doi.org/10.3389/fimmu.2020.00397
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author Gonzalez-Cotto, Marieli
Guo, Liang
Karwan, Megan
Sen, Shurjo K.
Barb, Jennifer
Collado, Carlos J.
Elloumi, Fathi
Palmieri, Erika M.
Boelte, Kimberly
Kolodgie, Frank D.
Finn, Aloke V.
Biesecker, Leslie G.
McVicar, Daniel W.
author_facet Gonzalez-Cotto, Marieli
Guo, Liang
Karwan, Megan
Sen, Shurjo K.
Barb, Jennifer
Collado, Carlos J.
Elloumi, Fathi
Palmieri, Erika M.
Boelte, Kimberly
Kolodgie, Frank D.
Finn, Aloke V.
Biesecker, Leslie G.
McVicar, Daniel W.
author_sort Gonzalez-Cotto, Marieli
collection PubMed
description The Triggering Receptor Expressed on Myeloid cells-like 4 (TREML4) is a member of the TREM receptor family, known modulators of inflammatory responses. We have previously found that TREML4 expression positively correlates with human coronary arterial calcification (CAC). However, the role of TREML4 in the pathogenesis of cardiovascular disease remains incompletely defined. Since macrophages play a key role in inflammatory conditions, we investigated if activated macrophages selectively expressed TREML4 and found that carriage of either one of the eQTL SNP’s previously associated with increased TREML4 expression conferred higher expression in human inflammatory macrophages (M1) compared to alternatively activated macrophages (M2). Furthermore, we found that TREML4 expression in human M1 dysregulated several inflammatory pathways related to leukocyte activation, apoptosis and extracellular matrix degradation. Similarly, murine M1 expressed substantial levels of Treml4, as did oxLDL treated macrophages. Transcriptome analysis confirmed that murine Treml4 controls the expression of genes related to inflammation and lipid regulation pathways, suggesting a possible role in atherosclerosis. Analysis of Apoe(–/–)/Treml4(–/–) mice showed reduced plaque burden and lesion complexity as indicated by decreased stage scores, macrophage content and collagen deposition. Finally, transcriptome analysis of oxLDL-loaded murine macrophages showed that Treml4 represses a specific set of genes related to carbohydrate, ion and amino acid membrane transport. Metabolomic analysis confirmed that Treml4 deficiency may promote a beneficial relationship between iron homeostasis and glucose metabolism. Together, our results suggest that Treml4 plays a role in the development of cardiovascular disease, as indicated by Treml4-dependent dysregulation of macrophage inflammatory pathways, macrophage metabolism and promotion of vulnerability features in advanced lesions.
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spelling pubmed-71337892020-04-14 TREML4 Promotes Inflammatory Programs in Human and Murine Macrophages and Alters Atherosclerosis Lesion Composition in the Apolipoprotein E Deficient Mouse Gonzalez-Cotto, Marieli Guo, Liang Karwan, Megan Sen, Shurjo K. Barb, Jennifer Collado, Carlos J. Elloumi, Fathi Palmieri, Erika M. Boelte, Kimberly Kolodgie, Frank D. Finn, Aloke V. Biesecker, Leslie G. McVicar, Daniel W. Front Immunol Immunology The Triggering Receptor Expressed on Myeloid cells-like 4 (TREML4) is a member of the TREM receptor family, known modulators of inflammatory responses. We have previously found that TREML4 expression positively correlates with human coronary arterial calcification (CAC). However, the role of TREML4 in the pathogenesis of cardiovascular disease remains incompletely defined. Since macrophages play a key role in inflammatory conditions, we investigated if activated macrophages selectively expressed TREML4 and found that carriage of either one of the eQTL SNP’s previously associated with increased TREML4 expression conferred higher expression in human inflammatory macrophages (M1) compared to alternatively activated macrophages (M2). Furthermore, we found that TREML4 expression in human M1 dysregulated several inflammatory pathways related to leukocyte activation, apoptosis and extracellular matrix degradation. Similarly, murine M1 expressed substantial levels of Treml4, as did oxLDL treated macrophages. Transcriptome analysis confirmed that murine Treml4 controls the expression of genes related to inflammation and lipid regulation pathways, suggesting a possible role in atherosclerosis. Analysis of Apoe(–/–)/Treml4(–/–) mice showed reduced plaque burden and lesion complexity as indicated by decreased stage scores, macrophage content and collagen deposition. Finally, transcriptome analysis of oxLDL-loaded murine macrophages showed that Treml4 represses a specific set of genes related to carbohydrate, ion and amino acid membrane transport. Metabolomic analysis confirmed that Treml4 deficiency may promote a beneficial relationship between iron homeostasis and glucose metabolism. Together, our results suggest that Treml4 plays a role in the development of cardiovascular disease, as indicated by Treml4-dependent dysregulation of macrophage inflammatory pathways, macrophage metabolism and promotion of vulnerability features in advanced lesions. Frontiers Media S.A. 2020-03-30 /pmc/articles/PMC7133789/ /pubmed/32292401 http://dx.doi.org/10.3389/fimmu.2020.00397 Text en Copyright © 2020 Gonzalez-Cotto, Guo, Karwan, Sen, Barb, Collado, Elloumi, Palmieri, Boelte, Kolodgie, Finn, Biesecker and McVicar. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Gonzalez-Cotto, Marieli
Guo, Liang
Karwan, Megan
Sen, Shurjo K.
Barb, Jennifer
Collado, Carlos J.
Elloumi, Fathi
Palmieri, Erika M.
Boelte, Kimberly
Kolodgie, Frank D.
Finn, Aloke V.
Biesecker, Leslie G.
McVicar, Daniel W.
TREML4 Promotes Inflammatory Programs in Human and Murine Macrophages and Alters Atherosclerosis Lesion Composition in the Apolipoprotein E Deficient Mouse
title TREML4 Promotes Inflammatory Programs in Human and Murine Macrophages and Alters Atherosclerosis Lesion Composition in the Apolipoprotein E Deficient Mouse
title_full TREML4 Promotes Inflammatory Programs in Human and Murine Macrophages and Alters Atherosclerosis Lesion Composition in the Apolipoprotein E Deficient Mouse
title_fullStr TREML4 Promotes Inflammatory Programs in Human and Murine Macrophages and Alters Atherosclerosis Lesion Composition in the Apolipoprotein E Deficient Mouse
title_full_unstemmed TREML4 Promotes Inflammatory Programs in Human and Murine Macrophages and Alters Atherosclerosis Lesion Composition in the Apolipoprotein E Deficient Mouse
title_short TREML4 Promotes Inflammatory Programs in Human and Murine Macrophages and Alters Atherosclerosis Lesion Composition in the Apolipoprotein E Deficient Mouse
title_sort treml4 promotes inflammatory programs in human and murine macrophages and alters atherosclerosis lesion composition in the apolipoprotein e deficient mouse
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7133789/
https://www.ncbi.nlm.nih.gov/pubmed/32292401
http://dx.doi.org/10.3389/fimmu.2020.00397
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