| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2039332 | Cell Reports | 2015 | 13 Pages |
•Mice pre-depleted of neutrophils develop more autoantibodies after pDC activation•The pDC-IFN-α/β pathway stimulates NK cells to produce IFN-γ by inducing IL-15•ROS released by neutrophils decreases IL-15 and thus inhibits IFN-γ production•Neutrophils in male NZB/W F1 mice suppress NK cell and autoimmune B cell activation
SummaryHere, we examine the mechanism by which plasmacytoid dendritic cells (pDCs) and type I interferons promote humoral autoimmunity. In an amyloid-induced experimental autoimmune model, neutrophil depletion enhanced anti-nuclear antibody development, which correlated with heightened IFN-γ production by natural killer (NK) cells. IFN-α/β produced by pDCs activated NK cells via IL-15 induction. Neutrophils released reactive oxygen species (ROS), which negatively modulated the levels of IL-15, thereby inhibiting IFN-γ production. Mice deficient in NADPH oxidase 2 produced increased amounts of IFN-γ and developed augmented titers of autoantibodies. Both the pDC-IFN-α/β pathway and IFN-γ were indispensable in stimulating humoral autoimmunity. Male NZB/W F1 mice expressed higher levels of superoxide than their female lupus-prone siblings, and depletion of neutrophils resulted in spontaneous NK cell and autoimmune B cell activation. Our findings suggest a regulatory role for neutrophils in vivo and highlight the importance of an NK-IFN-γ axis downstream of the pDC-IFN-α/β pathway in systemic autoimmunity.
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