Respiratory syncytial virus infection of newborn CX3CR1-deficient mice induces a pathogenic pulmonary innate immune response
Sudipta Das, … , Anuradha Ray, Prabir Ray
Sudipta Das, … , Anuradha Ray, Prabir Ray
Published September 7, 2017
Citation Information: JCI Insight. 2017;2(17):e94605. https://doi.org/10.1172/jci.insight.94605.
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Research Article Infectious disease Pulmonology

Respiratory syncytial virus infection of newborn CX3CR1-deficient mice induces a pathogenic pulmonary innate immune response

Abstract

Respiratory syncytial virus (RSV) infects almost all infants by 2 years of age, and severe bronchiolitis resulting from RSV infection is the primary cause of hospitalization in the first year of life. Among infants hospitalized due to RSV-induced bronchiolitis, those with a specific mutation in the chemokine receptor CX3CR1, which severely compromises binding of its ligand CX3CL1, were at a higher risk for more severe viral bronchiolitis than those without the mutation. Here, we show that RSV infection of newborn mice deficient in CX3CR1 leads to significantly greater neutrophilic inflammation in the lungs, accompanied by an increase in mucus production compared with that induced in WT mice. Analysis of innate and adaptive immune responses revealed an early increase in the number of IL-17+ γδ T cells in CX3CR1-deficient mice that outnumbered IFN-γ+ γδ T cells as well as IFN-γ+ NK cells, IFN-γ being host protective in the context of RSV infection. This bias toward IL-17+ γδ T cells persisted at a later time. The lungs of CX3CR1-deficient mice expressed higher levels of IL-1β mRNA and protein, and blockade of IL-1β signaling using IL-1 receptor antagonist significantly reduced the number of IL-17+ γδ T cells in the lungs of infected mice. Blockade of IL-17RC abolished RSV-induced lung pathology in infected CX3CR1-deficient mice. We propose that, in infants harboring mutant CX3CR1, targeting the IL-17R may minimize disease severity and hospitalization in early life.

Authors

Sudipta Das, Mahesh Raundhal, Jie Chen, Timothy B. Oriss, Rachael Huff, John V. Williams, Anuradha Ray, Prabir Ray

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Figure 5

Blocking IL-1β signaling inhibits generation of IL-17+ γδ T cells after RSV infection of CX3CR1–/– mice.

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Blocking IL-1β signaling inhibits generation of IL-17+ γδ T cells after ...
(A) Schematic representation of the experimental plan. Neonatal mice were treated with IL-1RA (anakinra) at a dose of 5 mg/kg by the intraperitoneal route every 24 hours as shown. The pups were infected with 1 × 106 PFU of RSV by the intranasal route 4 hours after the first IL-1RA treatment on day 5, and mice were sacrificed on day 7 p.i. for analysis. (BD) Flow cytometric analysis of the mentioned groups, showing (B) the total number of lung cells and γδ T cells; (C) percentages of IL-17+ and IFN-γ+ γδ T cells, with representative contour plots, and (D) the total number of IL-17+ γδ T cells and IFN-γ+γδ T cells on day 7 p.i. Analyses were performed using FlowJo software. Data shown are mean ± SEM, representative of 2 independent experiments; n = 3 (uninfected), 5 (RSV-infected), and 6 (RSV-infected + IL-1RA) mice per group per experiment. *P ≤ 0.05, **P ≤ 0.01, ****P ≤ 0.0001. 1-way ANOVA with Tukey’s post-hoc test (B–D) was used for statistical analysis.