Alveolar Type II Epithelial Cells Contribute to the Anti-Influenza A Virus Response in the Lung by Integrating Pathogen- and Microenvironment-Derived Signals

Stegemann-Koniszewski, Sabine; Jeron, Andreas; Gereke, Marcus; Geffers, Robert; Kröger, Andrea; Gunzer, Matthias; Bruder, Dunja

doi:10.1128/mbio.00276-16

Cited by 55 publications

(47 citation statements)

References 46 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…These genes included cytokines and chemokines (Cxcl9, Ccl5, IL12b, Ccl8) , IFN response genes (Ifitm6, Ifi27l2a, Ifna2, Ifit2, Ifitm5, Ifra11 ), and genes involved in processing MHC class I antigens (Psmb10, Tap2, H2-Q2, H2-K1, Psmd9, Psme2, Psme1). The significant up-regulation of host defense genes in response to PR8 in the LA4 cell line corresponds with the expression profile of murine type II alveolar epithelial cells in response to PR8 infection in mice [37]. Furthermore, strong up-regulation of immune response-related genes upon PR8 infection of mice correlates with disease severity [11].…”

Section: Resultsmentioning

confidence: 99%

“…Alveolar epithelial cells have a key role in alerting the immune system to infection by respiratory viruses and shaping immune responses [37, 56, 57]. As viruses from several different families all target respiratory epithelial cells, it is important to understand the similarities and differences in how these cells respond to a diverse set of viruses.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Lung epithelial cells have virus-specific and shared gene expression responses to infection by diverse respiratory viruses

Leuven

Ridenhour

Miller

et al. 2016

Preprint

View full text Add to dashboard Cite

The severity of respiratory viral infections is partially determined by the cellular response mounted by infected lung epithelial cells. Disease prevention and treatment is dependent on our understanding of the shared and unique responses elicited by diverse viruses, yet few studies compare host responses to viruses from different families while controlling other experimental parameters. Murine models are commonly used to study the pathogenesis of respiratory viral infections, and in vitro studies using murine cells provide mechanistic insight into the pathogenesis observed in vivo. We used microarray analysis to compare changes in gene expression of murine lung epithelial cells infected individually by three respiratory viruses causing mild (rhinovirus, RV1B), moderate (coronavirus, MHV-1), and severe (influenza A virus, PR8) disease in mice. RV1B infection caused numerous gene expression changes, but the differential effect peaked at 12 hours post-infection. PR8 altered an intermediate number of genes whose expression continued to change through 24 hours. MHV-1 had comparatively few effects on host gene expression. The viruses elicited highly overlapping responses in antiviral genes, though MHV-1 induced a lower type I interferon response than the other two viruses. Signature genes were identified for each virus and included host defense genes for PR8, tissue remodeling genes for RV1B, and transcription factors for MHV-1. Our comparative approach identified universal and specific transcriptional signatures of virus infection that can be used to distinguish shared and virus-specific mechanisms of pathogenesis in the respiratory tract.

show abstract

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Lung epithelial cells have virus-specific and shared gene expression responses to infection by diverse respiratory viruses

Leuven

Ridenhour

Miller

et al. 2016

Preprint

View full text Add to dashboard Cite

show abstract

“…These cells can be identified in enzyme-digested lung tissue using flow cytometry. We defined AT-I as CD45 À , T1a + MHC-I + , AT-II as CD45 À , T1a À , EpCAM + MHC-II high , and cilia cells as CD45 À , T1a À , EpCAM + MHC-II int as previously described (Stegemann-Koniszewski et al, 2016;Cardani et al, 2017;Hasegawa et al, 2017) ( Figure 3A). Although two recent transcriptomic studies identified an IFN gene signature in AT-II (Stegemann-Koniszewski et al, 2016;Steuerman et al, 2018), to the best of our knowledge, the IFN-response in this and other pulmonary epithelial cells has yet to be compared.…”

Section: M1red Mice Reveal That Pulmonary Epithelial Cells Exhibit DImentioning

confidence: 99%

Visualizing the Selectivity and Dynamics of Interferon Signaling In Vivo

et al. 2019

View full text Add to dashboard Cite

show abstract

“…Chemokines and chemokine receptors are critical in directing T cells to sites of infection. CXCL9 and CXCL10 from epithelial cells are strongly induced by influenza infection [14, 17]. The receptor for these chemokines, CXCR3, is expressed on activated CD8 T cells and is required for efficient infiltration of the infected respiratory tract [18].…”

Section: Resultsmentioning

confidence: 99%

Antigen and G-Protein Coupled Receptor signaling differentially control CD8 T cell motility immediately before and after virus clearance in a primary infection

Lambert-Emo

Reilly

Sportiello

et al. 2019

Preprint

View full text Add to dashboard Cite

17 In mice, experimental influenza virus infection stimulates CD8 T cell infiltration of the airways.18 Virus is cleared by day 9, and between days 8 and 9 there is an abrupt change in CD8 T cell 19 motility behavior transitioning from low velocity and high confinement on day 8, to high velocity 20 with continued confinement on day 9. We hypothesized that it is loss of virus and/or antigen 21 signals in the context of high chemokine levels that drives the T cells into a rapid surveillance 22 mode. Virus infection induces chemokine production, which may change when the virus is 23 cleared. We therefore sought to examine this period of rapid changes to the T cell environment in 24 the tissue and seek evidence on the roles of peptide-MHC and chemokine receptor interactions.25 Experiments were performed to block G protein coupled receptor (GPCR) signaling with Pertussis 26 toxin (Ptx). Ptx treatment generally reduced cell velocities and mildly increased confinement, 27 except on day 8 when velocity increased and confinement was relieved, suggesting chemokine 28 mediated arrest. Blocking specific peptide-MHC with monoclonal antibody unexpectedly 29 decreased velocities on days 7 through 9, suggesting TCR/peptide-MHC interactions promote 30 cell mobility in the tissue. Together, these results suggest the T cells are engaged with antigen 31 bearing and chemokine producing cells that affect motility in ways that vary with the day after 32 infection. The increase in velocities on day 9 were reversed by addition of specific peptide, 33 consistent with the idea that antigen signals become limiting on day 9 compared to earlier time 34 points. Thus, antigen and chemokine signals act to alternately promote and restrict CD8 T cell 35 motility until the point of virus clearance, suggesting the switch in motility behavior on day 9 may 36 be due to a combination of limiting antigen in the presence of high chemokine signals as the virus 37 is cleared. 39 Introduction40 Influenza viruses infect roughly 12 percent of the population in any given year [1]. This leads to 41 lost productivity, hospitalizations, and deaths. In the 2017-18 season there was a record 80,000 3 42 deaths in the US alone [2]. In 2018-19, the northern hemisphere experienced the longest flu 43 season in over 20 years [3]. Understanding how the immune system controls influenza infection 44 is paramount to the development of improved vaccination strategies and for understanding the 45 disease process itself. Cytotoxic CD8 T cells are responsible for the initial clearance of infected 46 cells, especially in a primary infection when there are no pre-existing antibodies or other types of 47 adaptive immunity [4, 5]. In order to reach the site of infection, the trachea and airway epithelium, 48 the CD8 T cells must traffic through the circulation, exit into the tissue, and migrate within the 49 tissue before crossing into the epithelial surface. There are many things in the tissue 50 microenvironment that the T cells must interact and communicate with, and many feature...

show abstract

Alveolar Type II Epithelial Cells Contribute to the Anti-Influenza A Virus Response in the Lung by Integrating Pathogen- and Microenvironment-Derived Signals

Cited by 55 publications

References 46 publications

Lung epithelial cells have virus-specific and shared gene expression responses to infection by diverse respiratory viruses

Lung epithelial cells have virus-specific and shared gene expression responses to infection by diverse respiratory viruses

Visualizing the Selectivity and Dynamics of Interferon Signaling In Vivo

Antigen and G-Protein Coupled Receptor signaling differentially control CD8 T cell motility immediately before and after virus clearance in a primary infection

Contact Info

Product

Resources

About