Small amounts of superantigen, when presented on dendritic cells, are sufficient to initiate T cell responses Journal Article

   


Authors: Bhardwaj, N.; Young, J. W.; Nisanian, A. J.; Baggers, J.; Steinman, R. M.
Article Title: Small amounts of superantigen, when presented on dendritic cells, are sufficient to initiate T cell responses
Abstract: Dendritic cells are potent antigen-presenting cells for several primary immune responses and therefore provide an opportunity for evaluating the amounts of cell-associated antigens that are required for inducing T cell-mediated immunity. Because dendritic calls express very high levels of major histocompatibility complex (MHC) class II products, it has been assumed that high levels of ligands bound to MHC products (“signal one”) are needed to stimulate quiescent T cells. Here we describe quantitative aspects underlying the stimulation of human blood T cells by a bacterial superantigen, staphylococcal enterotoxin A (SEA). The advantages of superantigens for quantitative studies of signal one are that these ligands: (a) engage MHC class II and the T cell receptor but do not require processing; (b) are efficiently presented to large numbers of quiescent T cells; and (c) can be pulsed onto dendritic cells before their application to T cells. Thus one can relate amounts of dendritic cell-associated SEA to subsequent lymphocyte stimulation. Using radioiodinated SEA, we noted that dendritic cells can bind 30-200 times more superantigen than B cells and monocytes. Nevertheless, this high SEA binding does not underlie the strong potency of dendritic cells to present antigen to T cells. Dendritic cells can sensitize quiescent T cells, isolated using monoclonals to appropriate CD45R epitopes, after a pulse of SEA that occupies a maximum of 0.1% of surface MHC class II molecules. This corresponds to an average of 2,000 molecules per dendritic cell. At these low doses of bound SEA, monoclonal antibodies to CD3, CD4, and CD28 almost completely block T cell proliferation. In addition to suggesting new roles for MHC class II on dendritic ceils, especially the capture and retention of ligands at low external concentrations, the data reveal that primary T calls can generate a response to exceptionally low levels of signal one as long as these are ddivered on dendritic ceils. © 1993, Rockefeller University Press., All rights reserved.
Keywords: signal transduction; controlled study; human cell; cd3 antigen; antigen expression; lymphocyte proliferation; t-lymphocytes; cells, cultured; cell division; dendritic cell; b lymphocyte; b-lymphocytes; t lymphocyte receptor; antigen presentation; lymphocyte activation; dendritic cells; cellular immunity; antigens; major histocompatibility antigen class 2; binding sites; cd4 antigen; staphylococcus aureus; histocompatibility antigens class ii; major histocompatibility complex; t lymphocyte activation; cd28 antigen; cd45 antigen; bacterial antigen; superantigen; enterotoxins; human; priority journal; article; support, non-u.s. gov't; support, u.s. gov't, p.h.s.; staphylococcus enterotoxin
Journal Title: Journal of Experimental Medicine
Volume: 178
Issue: 2
ISSN: 0022-1007
Publisher: Rockefeller University Press  
Date Published: 1993-08-01
Start Page: 633
End Page: 642
Language: English
DOI: 10.1084/jem.178.2.633
PUBMED: 8340760
PROVIDER: scopus
PMCID: PMC2191121
DOI/URL:

https://www.scopus.com/inward/record.uri?eid=2-s2.0-0027218703&doi=10.1084%2fjem.178.2.633&partnerID=40&md5=93a49190859cd15585c356a0af898496
Notes: Article -- Export Date: 1 March 2019 -- Source: Scopus
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  1. James W Young
    318 Young
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