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Aspirin-like drugs prime human T cells. Modulation of intracellular calcium concentrations.

E Flescher, D Fossum, P J Gray, G Fernandes, M J Harper and N Talal
J Immunol April 15, 1991, 146 (8) 2553-2559;
E Flescher
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D Fossum
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P J Gray
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G Fernandes
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M J Harper
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N Talal
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Abstract

Aspirin-like drugs (ALD) enhance T cell proliferation by suppressing PG production in monocytes. Normal human T cells do not produce any eicosanoids. Therefore we studied whether ALD would affect purified T cells directly. We found that ALD enhanced the proliferation and IL-2 production of T cells in the absence of monocytes. This effect did not depend on arachidonic acid metabolism as no lipoxygenase products and only nonsuppressive levels of cyclooxygenase products were detected in T cell cultures. Several possible mechanisms of the ALD effect were ruled out including 1) enhanced mitogen binding, 2) induction of activation markers (IL-2R, transferrin receptor, HLA-DR) on the cell surface, 3) down-regulation of suppressor cells. ALD caused a rise in [Ca2+]i which appeared to reflect an influx of Ca2+ from the extracellular milieu and was more pronounced in CD4+ cells. The rise in intracellular levels of Ca2+, that is considered a necessary second messenger for T cell activation, may prime these cells for an enhanced response to mitogens. In addition, ALD increased T cell membrane fluidity but only at higher concentrations than those found to enhance proliferation. The pharmacologic effect of ALD on T cells presents a possible new immunoenhancing potential of these drugs and may have therapeutic use in immunosuppressed individuals.

  • Copyright © 1991 by American Association of Immunologists
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The Journal of Immunology
Vol. 146, Issue 8
15 Apr 1991
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Aspirin-like drugs prime human T cells. Modulation of intracellular calcium concentrations.
E Flescher, D Fossum, P J Gray, G Fernandes, M J Harper, N Talal
The Journal of Immunology April 15, 1991, 146 (8) 2553-2559;

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Aspirin-like drugs prime human T cells. Modulation of intracellular calcium concentrations.
E Flescher, D Fossum, P J Gray, G Fernandes, M J Harper, N Talal
The Journal of Immunology April 15, 1991, 146 (8) 2553-2559;
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Print ISSN 0022-1767        Online ISSN 1550-6606