Abstract

Abstract Stimulation of the type 1 IL-1R (IL-1R1) and the IL-18R by their cognate ligands induces recruitment of the IL-1R-associated kinase (IRAK). Activation of IRAK leads in turn to nuclear translocation of NF-κB, which directs expression of innate and adaptive immune response genes. To study IRAK function in cytokine signaling, we generated cells and mice lacking the IRAK protein. IRAK-deficient fibroblasts show diminished activation of NF-κB when stimulated with IL-1. Immune effector cells without IRAK exhibit a defective IFN-γ response to costimulation with IL-18. Furthermore, mice lacking the Irak gene demonstrate an attenuated response to injected IL-1. Deletion of Irak, however, does not affect the ability of mice to develop delayed-type hypersensitivity or clear infection with the intracellular parasite, Listeria monocytogenes. These results demonstrate that although IRAK participates in IL-1 and IL-18 signal transduction, residual cytokine responsiveness operates through an IRAK-independent pathway.

Keywords

BiologySignal transductionImmune systemCytokineCell biologyEffectorInnate immune systemAcquired immune systemKinaseImmunology

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Year
1999
Type
article
Volume
163
Issue
2
Pages
978-984
Citations
280
Access
Closed

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James A. Thomas, Jerry L. Allen, May F. Tsen et al. (1999). Impaired Cytokine Signaling in Mice Lacking the IL-1 Receptor-Associated Kinase. The Journal of Immunology , 163 (2) , 978-984. https://doi.org/10.4049/jimmunol.163.2.978

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DOI
10.4049/jimmunol.163.2.978