Articles

Loss of IRF-4–binding protein leads to the spontaneous development of systemic autoimmunity

Fanzo, Jessica C.; Yang, Wen; Jang, So Young; Gupta, Sanjay; Chen, Qinzhong; Siddiq, Ayesha; Greenberg,, Teven; Pernis, Alessandra B.

IFN regulatory factor 4–binding (IRF-4–binding) protein (IBP) is a novel type of activator of Rho GTPases that is recruited to the immunological synapse upon TCR stimulation. Here we demonstrate that loss of IBP leads to the spontaneous development of a systemic autoimmune disorder characterized by the accumulation of effector/memory T cells and IgG+ B cells, profound hypergammaglobulinemia, and autoantibody production. Similar to human SLE, this syndrome primarily affects females. T cells from IBP-deficient mice are resistant to death in vitro as well as in vivo and exhibit selective defects in effector function. In the absence of IBP, T cells respond suboptimally to TCR engagement, as demonstrated by diminished ERK1/2 activation, decreased c-Fos induction, impaired immunological synapse formation, and defective actin polymerization. Transduction of IBP-deficient T cells with a WT IBP protein, but not with an IBP mutant lacking the Dbl-like domain required for Rho GTPase activation, rescues the cytoskeletal defects exhibited by these cells. Collectively, these findings indicate that IBP, a novel regulator of Rho GTPases, is required for optimal T cell effector function, lymphocyte homeostasis, and the prevention of systemic autoimmunity.

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Also Published In

Title
Journal of Clinical Investigation
DOI
https://doi.org/10.1172/JCI24096

More About This Work

Academic Units
International Research Institute for Climate and Society
Published Here
February 7, 2024