| Literature DB >> 33711270 |
Benjamin H Gern1, Kristin N Adams2, Courtney R Plumlee2, Caleb R Stoltzfus3, Laila Shehata3, Albanus O Moguche3, Kathleen Busman-Sahay4, Scott G Hansen4, Michael K Axthelm4, Louis J Picker4, Jacob D Estes4, Kevin B Urdahl5, Michael Y Gerner6.
Abstract
CD4 T cell effector function is required for optimal containment of Mycobacterium tuberculosis (Mtb) infection. IFNɣ produced by CD4 T cells is a key cytokine that contributes to protection. However, lung-infiltrating CD4 T cells have a limited ability to produce IFNɣ, and IFNɣ plays a lesser protective role within the lung than at sites of Mtb dissemination. In a murine infection model, we observed that IFNɣ production by Mtb-specific CD4 T cells is rapidly extinguished within the granuloma but not within unaffected lung regions, suggesting localized immunosuppression. We identified a signature of TGFβ signaling within granuloma-infiltrating T cells in both mice and rhesus macaques. Selective blockade of TGFβ signaling in T cells resulted in an accumulation of terminally differentiated effector CD4 T cells, improved IFNɣ production within granulomas, and reduced bacterial burdens. These findings uncover a spatially localized immunosuppressive mechanism associated with Mtb infection and provide potential targets for host-directed therapy.Entities:
Keywords: IFNɣ; Mycobacterium tuberculosis; T cell function; TGFβ; adaptive immunity; granuloma; immune cell trafficking; immune suppression; lung inflammation; quantitative imaging
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Year: 2021 PMID: 33711270 PMCID: PMC8624870 DOI: 10.1016/j.chom.2021.02.005
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023