The regulation of T cell homeostasis and autoimmunity by T cell–derived LIGHT
Jing Wang, … , Lieping Chen, Yang-Xin Fu
Jing Wang, … , Lieping Chen, Yang-Xin Fu
Published December 15, 2001
Citation Information: J Clin Invest. 2001;108(12):1771-1780. https://doi.org/10.1172/JCI13827.
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Article

The regulation of T cell homeostasis and autoimmunity by T cell–derived LIGHT

Abstract

Costimulatory molecules on antigen-presenting cells (APCs) play an important role in T cell activation and expansion. However, little is known about the surface molecules involved in direct T-T cell interaction required for their activation and expansion. LIGHT, a newly discovered TNF superfamily member (TNFSF14), is expressed on activated T cells and immature dendritic cells. Here we demonstrate that blockade of LIGHT activity can reduce anti-CD3–mediated proliferation of purified T cells, suggesting that T cell–T cell interaction is essential for this proliferation. To test the in vivo activity of T cell–derived LIGHT in immune homeostasis and function, transgenic (Tg) mice expressing LIGHT in the T cell lineage were generated. LIGHT Tg mice have a significantly enlarged T cell compartment and a hyperactivated peripheral T cell population. LIGHT Tg mice spontaneously develop severe autoimmune disease manifested by splenomegaly, lymphadenopathy, glomerulonephritis, elevated autoantibodies, and severe infiltration of various peripheral tissues. Furthermore, the blockade of LIGHT activity ameliorates the severity of T cell–mediated diseases. Collectively, these findings establish a crucial role for this T cell–derived costimulatory ligand in T cell activation and expansion; moreover, the dysregulation of T cell–derived LIGHT leads to altered T cell homeostasis and autoimmune disease.

Authors

Jing Wang, James C. Lo, Amy Foster, Ping Yu, Helen M. Chen, Yang Wang, Koji Tamada, Lieping Chen, Yang-Xin Fu

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Renal pathological analysis and the elevated autoantibodies and rheumato...
Renal pathological analysis and the elevated autoantibodies and rheumatoid factor levels in LIGHT Tg mice. Representative pictures from WT (a, c, e, and g) and Tg (b, d, f, and h) mice at 5–8 months of age are shown. (a and b) H-E staining; (c and d) PAS staining; (eh) immunofluorescence staining. Original magnification is as follows: ad, ×40; eh, ×63. Glomeruli of Tg mice at 5–8 months of age were enlarged and lobulated with increased cellularity and inflammatory cell infiltration (b). The deposition of PAS-positive material was observed along the capillary wall and in mesangium in Tg mice (d). Sections of kidneys from WT and Tg mice were stained with FITC-conjugated goat anti-mouse IgG or total Ig. Strong Ig deposits were observed in the glomeruli of Tg mice (f and h). The serum levels of anti-DNA autoantibody (i, bottom panel) and total IgG (i, top panel) were determined in parallel by ELISA using the same set of WT (open circles) and Tg (filled squares) mice (n = 5). The serum level of rheumatoid factor in WT and Tg mice (n = 7) was determined by ELISA (j). Serum dilutions are indicated and data are means ± SD.