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Institute of Immunology and Transfusion Medicine, University of Lübeck School of Medicine, Lübeck, Germany
2To whom correspondence should be addressed.
Although the intriguing role of zinc as an essential trace element for
immune function is well established, particular progress in determining
the molecular principles of action of this ion was made recently.
Leukocyte responsiveness is delicately regulated by zinc concentration.
Zinc deficiency as well as supraphysiologic levels impair immune
function. Furthermore, the activities of many immunostimulants
frequently used in immunologic studies are influenced by zinc
concentration. Therefore, our knowledge from in vitro studies is widely
dependent on the zinc concentration, and when not in physiologic range,
immunologic responses are artificially low. Decreased
production of TH1 cytokines and interferon-
by leukocytes in the
healthy elderly person is correlated with low zinc serum level. The
defect in interferon- production is reconstituted by the addition of
physiologic amounts of zinc in vitro. Interestingly, zinc induces
cytokine production by isolated leukocytes. Zinc induces monocytes to
produce interleukin-1, interleukin-6 and tumor necrosis factor- in
peripheral blood mononuclear cells and separated monocytes. This effect
is higher in serum-free medium. However, only in the presence of
serum does zinc also induce T cells to produce lymphokines. This effect
on T cells is mediated by cytokines produced by monocytes. Stimulation
also requires cell-to-cell contact of monocytes and T cells.
Information is presented to illustrate the concepts that the zinc
concentration must be taken into account whenever in vitro studies are
made or complex alterations of immune functions are observed in
vivo.
KEY WORDS: • trace elements • immunology • cell biology • human • review
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