Endotoxin Activates T Cell Interferon-gamma Secretion in the Presence of Endothelium
Authors: Tennenberg S.D.; Weller J.J.
Source: Journal of Surgical Research, Volume 63, Number 1, June 1996 , pp. 73-76(4)
Publisher: Academic Press
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Abstract:
T lymphocytes (T cells) and their secreted lymphokine interferon-gamma (IFN-gamma) play important mediator roles in endotoxin-induced inflammation. We sought to explore the necessary conditions for and degree of LPS-induced T cell activation for IFN-gamma secretion in a human syngeneic microvascular endothelial-T cell coculture system. Human peripheral blood T cells, with or without monocytes, were cocultured in the presence or absence of a syngeneic human adipose microvascular endothelial cell (HAMVEC) monolayer. Cocultures were stimulated with LPS (1 mug/ml) and 3-day coculture supernatants assayed for IFN-gamma and IL-2 by ELISA. In the absence of HAMVEC, LPS-induced T cell activation for IFN-gamma secretion was only minimally demonstrated in the presence of monocytes. However, in the presence of HAMVEC, LPS activated T cells for IFN-gamma secretion in the absence of monocytes and markedly augmented the response in the presence of monocytes. A subset of donor cocultures showed no IFN-gamma response to LPS. IL-2 was not secreted as part of the LPS-induced T cell activation response. Our data support a hypothesis that endothelium serves as an accessory cell for T cell IFN-gamma secretion in endotoxin-induced inflammation. T cell-endothelial interactions may play a crucial role in promoting T cell activation during LPS-induced inflammation.
Language: English
Document Type: Research article
Affiliations: Allen Park Veterans Affairs Medical Center, Wayne State University School of Medicine, Detroit, Michigan, 48101:
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