Phenotypic and functional characterization of mice that lack the type I receptor for IL-1.

MB Glaccum, KL Stocking, K Charrier… - … (Baltimore, Md.: 1950 …, 1997 - journals.aai.org
MB Glaccum, KL Stocking, K Charrier, JL Smith, CR Willis, C Maliszewski, DJ Livingston…
Journal of immunology (Baltimore, Md.: 1950), 1997journals.aai.org
Abstract IL-1 alpha and IL-1 beta bind to receptors termed the type I and type II IL-1
receptors. The type I IL-1 receptor is responsible for specific signaling, while the type II IL-1
receptor functions as a nonsignaling decoy receptor. To determine the effect of a defect in IL-
1-mediated signaling, mice have been produced with a genetically disrupted type I IL-1
receptor gene. Mice lacking type I IL-1 receptors are of normal vigor and exhibit no overt
phenotype. B cells from type I IL-1R-/-mice activated in vitro with anti-IgM do not proliferate in …
Abstract
IL-1 alpha and IL-1 beta bind to receptors termed the type I and type II IL-1 receptors. The type I IL-1 receptor is responsible for specific signaling, while the type II IL-1 receptor functions as a nonsignaling decoy receptor. To determine the effect of a defect in IL-1-mediated signaling, mice have been produced with a genetically disrupted type I IL-1 receptor gene. Mice lacking type I IL-1 receptors are of normal vigor and exhibit no overt phenotype. B cells from type I IL-1R-/- mice activated in vitro with anti-IgM do not proliferate in response to IL-1, but do so in response to IL-4. Injection of murine IL-1 alpha does not induce detectable serum IL-6 levels in type I IL-1R-/- mice, but equivalent levels are produced in response to LPS. Type I IL-1R-/- mice have normal serum Ig levels and generate equivalent primary and secondary Ab responses as wild-type mice. In response to LPS, acute phase protein mRNA induction are equivalent in type I IL-1R-/- and wild-type mice. Type I IL-1R-/- mice do not differ from control mice in susceptibility to either a lethal challenge with D-galactosamine plus LPS or high dose LPS. Interestingly, ICE-/-/type I IL-1R-/- double mutant mice are resistant to high dose LPS. Type I IL-1R-/- mice backcrossed to the C57BL/6 background were as equally resistant as wild-type mice to Listeria monocytogenes.
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