Cutting Edge: Enhancement of Antibody Responses Through Direct Stimulation of B and T Cells by Type I IFN

Agnès Le Bon(Jenner Institute), Clare Thompson(Jenner Institute), Elisabeth Kamphuis(Paul Ehrlich Institut), Vanessa Durand(Jenner Institute), Cornelia Rossmann(Jenner Institute), Ulrich Kalinke(Paul Ehrlich Institut), David F. Tough(Jenner Institute)
The Journal of Immunology
February 1, 2006
Cited by 351Open Access
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Abstract

Type I IFN (IFN-alphabeta) is induced rapidly by infection and plays a key role in innate antiviral defense. IFN-alphabeta also exerts stimulatory effects on the adaptive immune system and has been shown to enhance Ab and T cell responses. We have investigated the importance of B and T cells as direct targets of IFN-alphabeta during IFN-alpha-mediated augmentation of the Ab response against a soluble protein Ag. Strikingly, the ability of IFN-alpha to stimulate the Ab response and induce isotype switching was markedly reduced in mice in which B cells were selectively deficient for the IFN-alphabetaR. Moreover, IFN-alpha-mediated enhancement of the Ab response was also greatly impaired in mice in which T cells were selectively IFN-alphabetaR-deficient. These results indicate that IFN-alphabetaR signaling in both B and T cells plays an important role in the stimulation of Ab responses by IFN-alphabeta.


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