The pathological effects of CCR2+ inflammatory monocytes are amplified by an IFNAR1-triggered chemokine feedback loop in highly pathogenic influenza infection

BACKGROUND: Highly pathogenic influenza viruses cause high levels of morbidity, including excessive infiltration of leukocytes into the lungs, high viral loads and a cytokine storm. However, the details of how these pathological features unfold in severe influenza infections remain unclear. Accumula...

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Autores principales: Lin, Sue-Jane, Lo, Ming, Kuo, Rei-Lin, Shih, Shin-Ru, Ojcius, David M, Lu, Jean, Lee, Chien-Kuo, Chen, Hui-Chen, Lin, Meei Yun, Leu, Chuen-Miin, Lin, Chia-Ni, Tsai, Ching-Hwa
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4243311/
https://www.ncbi.nlm.nih.gov/pubmed/25407417
http://dx.doi.org/10.1186/s12929-014-0099-6
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author Lin, Sue-Jane
Lo, Ming
Kuo, Rei-Lin
Shih, Shin-Ru
Ojcius, David M
Lu, Jean
Lee, Chien-Kuo
Chen, Hui-Chen
Lin, Meei Yun
Leu, Chuen-Miin
Lin, Chia-Ni
Tsai, Ching-Hwa
author_facet Lin, Sue-Jane
Lo, Ming
Kuo, Rei-Lin
Shih, Shin-Ru
Ojcius, David M
Lu, Jean
Lee, Chien-Kuo
Chen, Hui-Chen
Lin, Meei Yun
Leu, Chuen-Miin
Lin, Chia-Ni
Tsai, Ching-Hwa
author_sort Lin, Sue-Jane
collection PubMed
description BACKGROUND: Highly pathogenic influenza viruses cause high levels of morbidity, including excessive infiltration of leukocytes into the lungs, high viral loads and a cytokine storm. However, the details of how these pathological features unfold in severe influenza infections remain unclear. Accumulation of Gr1 + CD11b + myeloid cells has been observed in highly pathogenic influenza infections but it is not clear how and why they accumulate in the severely inflamed lung. In this study, we selected this cell population as a target to investigate the extreme inflammatory response during severe influenza infection. RESULTS: We established H1N1 IAV-infected mouse models using three viruses of varying pathogenicity and noted the accumulation of a defined Gr1 + CD11b + myeloid population correlating with the pathogenicity. Herein, we reported that CCR2+ inflammatory monocytes are the major cell compartments in this population. Of note, impaired clearance of the high pathogenicity virus prolonged IFN expression, leading to CCR2+ inflammatory monocytes amplifying their own recruitment via an interferon-α/β receptor 1 (IFNAR1)-triggered chemokine loop. Blockage of IFNAR1-triggered signaling or inhibition of viral replication by Oseltamivir significantly suppresses the expression of CCR2 ligands and reduced the influx of CCR2+ inflammatory monocytes. Furthermore, trafficking of CCR2+ inflammatory monocytes from the bone marrow to the lung was evidenced by a CCR2-dependent chemotaxis. Importantly, leukocyte infiltration, cytokine storm and expression of iNOS were significantly reduced in CCR2−/− mice lacking infiltrating CCR2+ inflammatory monocytes, enhancing the survival of the infected mice. CONCLUSIONS: Our results indicated that uncontrolled viral replication leads to excessive production of inflammatory innate immune responses by accumulating CCR2+ inflammatory monocytes, which contribute to the fatal outcomes of high pathogenicity virus infections.
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spelling pubmed-42433112014-11-26 The pathological effects of CCR2+ inflammatory monocytes are amplified by an IFNAR1-triggered chemokine feedback loop in highly pathogenic influenza infection Lin, Sue-Jane Lo, Ming Kuo, Rei-Lin Shih, Shin-Ru Ojcius, David M Lu, Jean Lee, Chien-Kuo Chen, Hui-Chen Lin, Meei Yun Leu, Chuen-Miin Lin, Chia-Ni Tsai, Ching-Hwa J Biomed Sci Research BACKGROUND: Highly pathogenic influenza viruses cause high levels of morbidity, including excessive infiltration of leukocytes into the lungs, high viral loads and a cytokine storm. However, the details of how these pathological features unfold in severe influenza infections remain unclear. Accumulation of Gr1 + CD11b + myeloid cells has been observed in highly pathogenic influenza infections but it is not clear how and why they accumulate in the severely inflamed lung. In this study, we selected this cell population as a target to investigate the extreme inflammatory response during severe influenza infection. RESULTS: We established H1N1 IAV-infected mouse models using three viruses of varying pathogenicity and noted the accumulation of a defined Gr1 + CD11b + myeloid population correlating with the pathogenicity. Herein, we reported that CCR2+ inflammatory monocytes are the major cell compartments in this population. Of note, impaired clearance of the high pathogenicity virus prolonged IFN expression, leading to CCR2+ inflammatory monocytes amplifying their own recruitment via an interferon-α/β receptor 1 (IFNAR1)-triggered chemokine loop. Blockage of IFNAR1-triggered signaling or inhibition of viral replication by Oseltamivir significantly suppresses the expression of CCR2 ligands and reduced the influx of CCR2+ inflammatory monocytes. Furthermore, trafficking of CCR2+ inflammatory monocytes from the bone marrow to the lung was evidenced by a CCR2-dependent chemotaxis. Importantly, leukocyte infiltration, cytokine storm and expression of iNOS were significantly reduced in CCR2−/− mice lacking infiltrating CCR2+ inflammatory monocytes, enhancing the survival of the infected mice. CONCLUSIONS: Our results indicated that uncontrolled viral replication leads to excessive production of inflammatory innate immune responses by accumulating CCR2+ inflammatory monocytes, which contribute to the fatal outcomes of high pathogenicity virus infections. BioMed Central 2014-11-18 /pmc/articles/PMC4243311/ /pubmed/25407417 http://dx.doi.org/10.1186/s12929-014-0099-6 Text en © Lin et al.; licensee BioMed Central Ltd. 2014 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Lin, Sue-Jane
Lo, Ming
Kuo, Rei-Lin
Shih, Shin-Ru
Ojcius, David M
Lu, Jean
Lee, Chien-Kuo
Chen, Hui-Chen
Lin, Meei Yun
Leu, Chuen-Miin
Lin, Chia-Ni
Tsai, Ching-Hwa
The pathological effects of CCR2+ inflammatory monocytes are amplified by an IFNAR1-triggered chemokine feedback loop in highly pathogenic influenza infection
title The pathological effects of CCR2+ inflammatory monocytes are amplified by an IFNAR1-triggered chemokine feedback loop in highly pathogenic influenza infection
title_full The pathological effects of CCR2+ inflammatory monocytes are amplified by an IFNAR1-triggered chemokine feedback loop in highly pathogenic influenza infection
title_fullStr The pathological effects of CCR2+ inflammatory monocytes are amplified by an IFNAR1-triggered chemokine feedback loop in highly pathogenic influenza infection
title_full_unstemmed The pathological effects of CCR2+ inflammatory monocytes are amplified by an IFNAR1-triggered chemokine feedback loop in highly pathogenic influenza infection
title_short The pathological effects of CCR2+ inflammatory monocytes are amplified by an IFNAR1-triggered chemokine feedback loop in highly pathogenic influenza infection
title_sort pathological effects of ccr2+ inflammatory monocytes are amplified by an ifnar1-triggered chemokine feedback loop in highly pathogenic influenza infection
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4243311/
https://www.ncbi.nlm.nih.gov/pubmed/25407417
http://dx.doi.org/10.1186/s12929-014-0099-6
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