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IL-10 deficiency unleashes an influenza-specific Th17 response and enhances survival against high-dose challenge.


ABSTRACT: We examined the expression and influence of IL-10 during influenza infection. We found that IL-10 does not impact sublethal infection, heterosubtypic immunity, or the maintenance of long-lived influenza Ag depots. However, IL-10-deficient mice display dramatically increased survival compared with wild-type mice when challenged with lethal doses of virus, correlating with increased expression of several Th17-associated cytokines in the lungs of IL-10-deficient mice during the peak of infection, but not with unchecked inflammation or with increased cellular responses. Foxp3(-) CD4 T cell effectors at the site of infection represent the most abundant source of IL-10 in wild-type mice during high-dose influenza infection, and the majority of these cells coproduce IFN-gamma. Finally, compared with predominant Th1 responses in wild-type mice, virus-specific T cell responses in the absence of IL-10 display a strong Th17 component in addition to a strong Th1 response and we show that Th17-polarized CD4 T cell effectors can protect naive mice against an otherwise lethal influenza challenge and utilize unique mechanisms to do so. Our results show that IL-10 expression inhibits development of Th17 responses during influenza infection and that this is correlated with compromised protection during high-dose primary, but not secondary, challenge.

SUBMITTER: McKinstry KK 

PROVIDER: S-EPMC2724021 | biostudies-literature | 2009 Jun

REPOSITORIES: biostudies-literature

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IL-10 deficiency unleashes an influenza-specific Th17 response and enhances survival against high-dose challenge.

McKinstry K Kai KK   Strutt Tara M TM   Buck Amanda A   Curtis Jonathan D JD   Dibble John P JP   Huston Gail G   Tighe Michael M   Hamada Hiromasa H   Sell Stewart S   Dutton Richard W RW   Swain Susan L SL  

Journal of immunology (Baltimore, Md. : 1950) 20090601 12


We examined the expression and influence of IL-10 during influenza infection. We found that IL-10 does not impact sublethal infection, heterosubtypic immunity, or the maintenance of long-lived influenza Ag depots. However, IL-10-deficient mice display dramatically increased survival compared with wild-type mice when challenged with lethal doses of virus, correlating with increased expression of several Th17-associated cytokines in the lungs of IL-10-deficient mice during the peak of infection, b  ...[more]

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