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Publication : Intestinal microbiota programming of alveolar macrophages influences severity of respiratory viral infection.

First Author  Ngo VL Year  2024
Journal  Cell Host Microbe Volume  32
Issue  3 Pages  335-348.e8
PubMed ID  38295788 Mgi Jnum  J:345954
Mgi Id  MGI:7610120 Doi  10.1016/j.chom.2024.01.002
Citation  Ngo VL, et al. (2024) Intestinal microbiota programming of alveolar macrophages influences severity of respiratory viral infection. Cell Host Microbe
abstractText  Susceptibility to respiratory virus infections (RVIs) varies widely across individuals. Because the gut microbiome impacts immune function, we investigated the influence of intestinal microbiota composition on RVI and determined that segmented filamentous bacteria (SFB), naturally acquired or exogenously administered, protected mice against influenza virus (IAV) infection. Such protection, which also applied to respiratory syncytial virus and severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), was independent of interferon and adaptive immunity but required basally resident alveolar macrophages (AMs). In SFB-negative mice, AMs were quickly depleted as RVI progressed. In contrast, AMs from SFB-colonized mice were intrinsically altered to resist IAV-induced depletion and inflammatory signaling. Yet, AMs from SFB-colonized mice were not quiescent. Rather, they directly disabled IAV via enhanced complement production and phagocytosis. Accordingly, transfer of SFB-transformed AMs into SFB-free hosts recapitulated SFB-mediated protection against IAV. These findings uncover complex interactions that mechanistically link the intestinal microbiota with AM functionality and RVI severity.
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