Deregulated T Cell Activation and Autoimmunity in Mice Lacking Interleukin-2 Receptor β

Haruhiko Suzuki; Thomas M. Kündig; Caren Furlonger; Andrew Wakeham; Emma Timms; T. Matsuyama; Rudolf Schmits; John Simard; Pamela S. Ohashi; Henrik Griesser; Tadatsugu Taniguchi; Christopher J. Paige; Tak W. Mak

doi:10.1126/science.7770771

Deregulated T Cell Activation and Autoimmunity in Mice Lacking Interleukin-2 Receptor β

Haruhiko Suzuki(Ontario Institute for Cancer Research), Thomas M. Kündig(Ontario Institute for Cancer Research), Caren Furlonger(Wellesley Institute), Andrew Wakeham(Ontario Institute for Cancer Research), Emma Timms(Ontario Institute for Cancer Research), T. Matsuyama(Ontario Institute for Cancer Research), Rudolf Schmits(Ontario Institute for Cancer Research), John Simard(Ontario Institute for Cancer Research), Pamela S. Ohashi(Ontario Institute for Cancer Research), Henrik Griesser(University of Toronto), Tadatsugu Taniguchi(The University of Osaka), Christopher J. Paige(Wellesley Institute), Tak W. Mak(Ontario Institute for Cancer Research)

Science

June 9, 1995

10.1126/science.7770771

Cited by 858

Abstract

In mice lacking the interleukin-2 receptor beta chain (IL-2R beta), T cells were shown to be spontaneously activated, resulting in exhaustive differentiation of B cells into plasma cells and the appearance of high serum concentrations of immunoglobulins G1 and E as well as autoantibodies that cause hemolytic anemia. Marked infiltrative granulocytopoiesis was also apparent, and the animals died after about 12 weeks. Depletion of CD4+ T cells in mutant mice rescued B cells without reversion of granulocyte abnormalities. T cells did not proliferate in response to polyclonal activators, nor could antigen-specific immune responses be elicited. Thus, IL-2R beta is required to keep the activation programs of T cells under control, to maintain homeostasis, and to prevent autoimmunity.

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