IL-12-Deficient Mice Are Defective in IFNγ Production and Type 1 Cytokine Responses

Magram, Jeanne; Connaughton, Suzanne E.; Warrier, Rajeev R.; Carvajal, Daisy; Wu, Changyou; Ferrante, Jessica; Stewart, Colin L.; Sarmiento, Ulla M.; Faherty, D A; Gately, Maurice K.

doi:10.1016/s1074-7613(00)80413-6

Cited by 932 publications

(643 citation statements)

References 44 publications

(19 reference statements)

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“…A similar requirement has been demonstrated in vivo (9), and the "third signal" acts as a switch that determines whether exposure to Ag results in tolerance vs full activation and development of memory (10,11). IL-12 cannot be the only source of signal 3 since CTL responses can occur in IL-12-deficient mice (9,12). As shown in this study, type I IFN can also provide the third signal for clonal expansion and differentiation of naive CD8 T cells and does so by acting directly on the T cell.…”

mentioning

confidence: 78%

Cutting Edge: Type I IFNs Provide a Third Signal to CD8 T Cells to Stimulate Clonal Expansion and Differentiation

Curtsinger

Valenzuela

Agarwal

et al. 2005

The Journal of Immunology

540

492

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In this study, we show that IFN-αβ can have a direct role in linking innate and adaptive responses by providing the “third signal” needed by naive CD8 T cells responding to Ag and costimulatory ligands. Stimulation of CD8 T cells in the absence of a third signal leads to proliferation, but clonal expansion is limited by poor survival and effector functions do not develop. We show that IFN-αβ can provide the third signal directly to CD8 T cells via a STAT4-dependent pathway to stimulate survival, development of cytolytic function, and production of IFN-γ. Provision of the third signal by either IFN-αβ or IL-12 results in regulation of the expression of a number of genes, including several that encode proteins critical for effector function.

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mentioning

confidence: 78%

Cutting Edge: Type I IFNs Provide a Third Signal to CD8 T Cells to Stimulate Clonal Expansion and Differentiation

Curtsinger

Valenzuela

Agarwal

et al. 2005

The Journal of Immunology

540

492

View full text Add to dashboard Cite

show abstract

“…CD40 and CD40L interactions play important roles in the priming, differentiation and effector function of helper and cytotoxic T cells [23]. IL-12 is an inducible cytokine composed of 35-and 40-kDa subunits and is crucial to promoting the development of Th1 cells and cell-mediated immunity [24][25][26]. DC are major IL-12 producers [27,28], and IL-12 production after cognate interaction with CD4 + T cells is largely dependent on CD40/CD40L interaction [29].…”

Section: Discussionmentioning

confidence: 99%

Small interference RNA modulation of IL‐10 in human monocyte‐derived dendritic cells enhances the Th1 response

Liu

Akasaki

et al. 2004

Eur J Immunol

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RNA interference technology has been used to modulate dendritic cell (DC) function by targeting the expression of genes such as IL-12 and NF-kB. In this paper, we demonstrate that transfection of DC with IL-10-specific double strands of small interference RNA (siRNA) resulted in potent suppression of IL-10 gene expression without inducing DC apoptosis or blocking DC maturation. Inhibition of IL-10 by siRNA was accompanied by increased CD40 expression and IL-12 production after maturation, which endowed DC with the ability to significantly enhance allogeneic T cell proliferation. IL-10 siRNA transfection did not affect MHC class II, CD86, CD83, or CD54 expression in mature DC. To further test the ability of IL-10 siRNA-treated DC to induce a T cell response, naive CD4 T cells were stimulated by autologous DC pulsed with KLH. The results indicated that IL-10 siRNA-transfected DC enhanced Th1 responses by increasing IFN-+ and decreasing IL-4 production. These findings suggest the potential for a novel immunotherapeutic strategy of using IL-10 siRNAtransfected antigen-presenting cells as vaccine delivery agents to boost the Th1 response against pathogens and tumors that are controlled by Th1 immunity.

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“…This has been clearly demonstrated in mice de®cient for the cytokines themselves or their receptor subunits. For example, mice de®cient for IL-12 or IL-12Rb1 chain are unable to generate Th1 cells, and mice lacking IL-4 or the IL-4Ra chain are de®cient for Th2 responses (Kopf et al, 1993;Kuhn et al, 1991;Magram et al, 1996;Noben-Trauth et al, 1997;Wu et al, 1997).…”

Section: T Helper Cell Differentiationmentioning

confidence: 99%

The biology of Stat4 and Stat6

2000

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IL-12-Deficient Mice Are Defective in IFNγ Production and Type 1 Cytokine Responses

Cited by 932 publications

References 44 publications

Cutting Edge: Type I IFNs Provide a Third Signal to CD8 T Cells to Stimulate Clonal Expansion and Differentiation

Cutting Edge: Type I IFNs Provide a Third Signal to CD8 T Cells to Stimulate Clonal Expansion and Differentiation

Small interference RNA modulation of IL‐10 in human monocyte‐derived dendritic cells enhances the Th1 response

The biology of Stat4 and Stat6

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