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Division of Allergy and Immunology, Department of Pediatrics, and
Division of Infectious Diseases, Department of Medicine, Harbor-University of California, Los Angeles, Medical Center, Torrance, CA 90509
Eukaryotic translation initiation factor (eIF)-6 is known to be
important in ribosome biogenesis. Previously, we have discovered that
eIF-6 mRNA is induced in lung in a murine model of asthma. We also
found that there was enhanced eIF-6 expression in mast cells stimulated
with PMA plus calcium ionophore. Therefore, we hypothesized that the
induction of eIF-6 enhances the production of bioactive mediators by
mast cells upon allergic stimulation. In the current study, we found
that eIF-6 mRNA was rapidly induced in murine mast cells stimulated by
Fc
RI cross-linking, which is a major physiologic stimulant for mast
cells. eIF-6 was also induced in human mast cells upon stimulation. The
increase in eIF-6 gene expression in murine mast cells was blocked by
therapeutic agents such as dexamethasone and cyclosporin A. To
determine the location and function of eIF-6, murine mast cells were
transfected with a construct that overexpressed enhanced green
fluorescent protein-tagged eIF-6. These experiments demonstrated that
eIF-6 was localized predominantly in the nucleolus of the mast cells.
Also, overexpression of enhanced green fluorescent protein/eIF-6
enhanced the production of histamine and IL-2, but not IL-4 by
stimulated murine mast cells. These results suggest that eIF-6
regulates the production of selected bioactive mediators in allergic
diseases. This is the first demonstration of a biologic function of
eIF-6 in mammalian cells.
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