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G Tosato, J Miller, G Marti and SE Pike
Division of Biochemistry and Biophysics, Food and Drug Administration,
National Institutes of Health, Bethesda, MD 20892.
Two monocyte-derived cytokines, interleukin-1 (IL-1) and interleukin-6
(IL-6), have been reported to costimulate monocyte-depleted T cell
populations in the presence of mitogen, and this effect has been attributed
to an accessory function of these molecules. We have now examined further
the accessory function potential of IL-1 plus IL-6, and examined how these
cytokines promote T cell growth with mitogen. Together, IL-1 and IL-6
additively and, to a small degree, synergistically promote the
proliferation of highly purified human peripheral blood T cells with
phytohemagglutinin (PHA). However, maximum costimulation by IL-1 plus IL-6
over a wide range of concentrations is significantly smaller than that
induced by optimal numbers of monocytes. Also, in contrast to monocytes
that costimulate equally effectively T4 positive and T8 positive cells,
IL-1 plus IL-6 costimulate T4 positive lymphocytes in marked preference to
T8 positive cells. IL-1 plus IL-6 induces IL-2 secretion in T cell cultures
costimulated with PHA, and an antibody to the IL-2 receptor, anti-Tac,
markedly inhibits PHA-activated T cells costimulated by IL-1 plus IL-6. In
addition, IL-1 plus IL-6 enhances the expression of surface IL-2 receptors.
Because the costimulatory effect of IL-1 plus IL-6 is quantitatively
smaller than that of monocytes, and it is preferentially directed toward T4
positive as opposed to T8 positive T cells, IL-1 plus IL-6, together,
appear to represent a selective set of monocyte- derived accessory signals.
This article has been cited by other articles:
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| Copyright © 1990 by American Society of Hematology Online ISSN: 1528-0020 | |||||||||
