Expression of lymphotoxin‐beta (LT‐β) in chronic inflammatory conditions

Abstract

Functional studies in gene‐knockout and transgenic mice systems have shown that lymphotoxin‐alpha and lymphotoxin‐beta (LT‐α and LT‐β) are of fundamental importance in peripheral lymphoid organ development, but it remains unclear what role these cytokines have to play in the adult immune response and in the pathogenesis of disease. In this study, a polyclonal anti‐serum to human LT‐β was used to investigate the distribution of LT‐β by immunohistochemistry in normal and diseased tissues. In the gut, lymph nodes, spleen, and tonsil, there was some LT‐β present on a variety of lymphoid cell types. In contrast, strong staining for LT‐β was observed on plasma cells and a subpopulation of CD4+ T cells in tissues affected by chronic inflammatory disease or infection, for example in inflammatory bowel disease, and in lymph nodes obtained from patients with sarcoidosis and tuberculosis. In tuberculous and sarcoid lymph nodes, LT‐β expression also occurred on some but not all epithelioid histiocytes within granulomas and on multi‐nucleated giant cells. These findings support a role for LT‐β in human disease and suggest that it might represent a therapeutic target in a variety of common infective or inflammatory disorders. Copyright © 2002 John Wiley & Sons, Ltd.