Deficiency of C-reactive protein or human C-reactive protein transgenic treatment aggravates influenza A infection in mice

C-reactive protein (CRP) has been shown to be a potential candidate target in the immunotherapy of severe influenza A infection. However, it is unclear on the pathogenesis associated with CRP in influenza infections. Here, we used influenza A H1N1 CA04 to infect human CRP transgenic mice (KI), CRP k...

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Autores principales: Zhang, Zhuohan, Gao, Yongjun, Li, Li, Luo, Junhao, Gao, Rongbao
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9584053/
https://www.ncbi.nlm.nih.gov/pubmed/36275680
http://dx.doi.org/10.3389/fimmu.2022.1028458
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author Zhang, Zhuohan
Gao, Yongjun
Li, Li
Luo, Junhao
Gao, Rongbao
author_facet Zhang, Zhuohan
Gao, Yongjun
Li, Li
Luo, Junhao
Gao, Rongbao
author_sort Zhang, Zhuohan
collection PubMed
description C-reactive protein (CRP) has been shown to be a potential candidate target in the immunotherapy of severe influenza A infection. However, it is unclear on the pathogenesis associated with CRP in influenza infections. Here, we used influenza A H1N1 CA04 to infect human CRP transgenic mice (KI), CRP knockout mice (KO), and wild-type mice (WT), respectively, and compared the viral pathogenicity and associated immune response in those mice. The results showed that CA04 infection resulted in 100%, 80%, and 60% death in KO, KI, and WT mice, respectively. Compared to WT mice, CA04 infection resulted in higher TCID50 in lungs on day 3 after infection but lowered HI antibody titers in sera of survivors on day 21 after infection in KI mice. ELISA assay showed that IFN-γ concentration was significantly increased in sera of WT, KI, or KO mice on day 7 after infection, and IL-17 was remarkably increased in sera of WT mice but decreased in sera of KI mice while no significant change in sera of KO mice on day 3 or 7 after infection. Quantitative RT-PCR showed that the relative expression levels of immune checkpoint CTLA-4, LAIR-1, GITR, BTLA, TIM-3, or PD-1 mRNA in the lung presented decreased levels on day 3 or 7 after infection in KI or KO mice. The correlation analysis showed that mRNA expression levels of the 6 molecules positively correlated with viral TICD50 in WT mice but negatively correlated with viral TCID50 in KI or KO mice. However, only LAIR-1 presented a significant correlation in each lung tissue of WT, KI, or KO mice with CA07 infection statistically. IHC results showed that LAIR-1 positive cells could be found in WT, KO, or KI mice lung tissues with CA04 infection, and the positive cells were mainly distributed in an inflammatory dense area. Our results suggested that deficiency of CRP or human CRP transgenic treatment aggravates influenza A virus infection in mice. CRP is a double sword in immune regulation of influenza infection in which IL-17 and immune checkpoint may be involved.
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spelling pubmed-95840532022-10-21 Deficiency of C-reactive protein or human C-reactive protein transgenic treatment aggravates influenza A infection in mice Zhang, Zhuohan Gao, Yongjun Li, Li Luo, Junhao Gao, Rongbao Front Immunol Immunology C-reactive protein (CRP) has been shown to be a potential candidate target in the immunotherapy of severe influenza A infection. However, it is unclear on the pathogenesis associated with CRP in influenza infections. Here, we used influenza A H1N1 CA04 to infect human CRP transgenic mice (KI), CRP knockout mice (KO), and wild-type mice (WT), respectively, and compared the viral pathogenicity and associated immune response in those mice. The results showed that CA04 infection resulted in 100%, 80%, and 60% death in KO, KI, and WT mice, respectively. Compared to WT mice, CA04 infection resulted in higher TCID50 in lungs on day 3 after infection but lowered HI antibody titers in sera of survivors on day 21 after infection in KI mice. ELISA assay showed that IFN-γ concentration was significantly increased in sera of WT, KI, or KO mice on day 7 after infection, and IL-17 was remarkably increased in sera of WT mice but decreased in sera of KI mice while no significant change in sera of KO mice on day 3 or 7 after infection. Quantitative RT-PCR showed that the relative expression levels of immune checkpoint CTLA-4, LAIR-1, GITR, BTLA, TIM-3, or PD-1 mRNA in the lung presented decreased levels on day 3 or 7 after infection in KI or KO mice. The correlation analysis showed that mRNA expression levels of the 6 molecules positively correlated with viral TICD50 in WT mice but negatively correlated with viral TCID50 in KI or KO mice. However, only LAIR-1 presented a significant correlation in each lung tissue of WT, KI, or KO mice with CA07 infection statistically. IHC results showed that LAIR-1 positive cells could be found in WT, KO, or KI mice lung tissues with CA04 infection, and the positive cells were mainly distributed in an inflammatory dense area. Our results suggested that deficiency of CRP or human CRP transgenic treatment aggravates influenza A virus infection in mice. CRP is a double sword in immune regulation of influenza infection in which IL-17 and immune checkpoint may be involved. Frontiers Media S.A. 2022-10-06 /pmc/articles/PMC9584053/ /pubmed/36275680 http://dx.doi.org/10.3389/fimmu.2022.1028458 Text en Copyright © 2022 Zhang, Gao, Li, Luo and Gao https://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
Zhang, Zhuohan
Gao, Yongjun
Li, Li
Luo, Junhao
Gao, Rongbao
Deficiency of C-reactive protein or human C-reactive protein transgenic treatment aggravates influenza A infection in mice
title Deficiency of C-reactive protein or human C-reactive protein transgenic treatment aggravates influenza A infection in mice
title_full Deficiency of C-reactive protein or human C-reactive protein transgenic treatment aggravates influenza A infection in mice
title_fullStr Deficiency of C-reactive protein or human C-reactive protein transgenic treatment aggravates influenza A infection in mice
title_full_unstemmed Deficiency of C-reactive protein or human C-reactive protein transgenic treatment aggravates influenza A infection in mice
title_short Deficiency of C-reactive protein or human C-reactive protein transgenic treatment aggravates influenza A infection in mice
title_sort deficiency of c-reactive protein or human c-reactive protein transgenic treatment aggravates influenza a infection in mice
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9584053/
https://www.ncbi.nlm.nih.gov/pubmed/36275680
http://dx.doi.org/10.3389/fimmu.2022.1028458
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AT lili deficiencyofcreactiveproteinorhumancreactiveproteintransgenictreatmentaggravatesinfluenzaainfectioninmice
AT luojunhao deficiencyofcreactiveproteinorhumancreactiveproteintransgenictreatmentaggravatesinfluenzaainfectioninmice
AT gaorongbao deficiencyofcreactiveproteinorhumancreactiveproteintransgenictreatmentaggravatesinfluenzaainfectioninmice

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