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Departments of Medicine and Pathology, University of California San Diego, La Jolla, California 92093-0623
The intestinal epithelium produces and responds
to cytokines and lipid mediators that play a key role in the induction
and regulation of mucosal inflammation. The lipid mediator
platelet-activating factor (PAF) can be produced and degraded by the
human intestinal epithelium and is known to mediate a range of
proinflammatory and other biological effects in the intestinal mucosa.
In the studies herein, we assessed whether or not human intestinal
epithelial cells express cell surface or intracellular PAF receptors
(PAF-R), whether expression of these receptors can be regulated, and
whether human intestinal epithelial cells respond to PAF. Several human colon epithelial cell lines (HT-29, Caco-2, T84, HCT-8, HCA-7, I407,
and LS-174T) were shown by RT-PCR to constitutively express mRNA for
PAF-R. In addition, PAF-R expression was demonstrated by immunoblot
analysis and PAF-R was shown to be constitutively expressed on the cell
surface of several of these cell lines, as assessed by flow cytometry.
PAF-R expression by human colon epithelial cells was upregulated by
stimulation with retinoic acid but not by stimulation with PAF,
proinflammatory agonists (tumor necrosis factor-
, interleukin-1,
interferon-
), or transforming growth factor-
. PAF-R on intestinal
epithelial cells were functional, as PAF stimulation of the cells
increased tyrosine phosphorylation of several cellular proteins,
including proteins of 75 and 125 kDa, and this response was blocked by
a PAF-R antagonist. Consistent with the findings using cell lines,
PAF-R were also constitutively expressed by normal human colon and
small intestinal epithelium in vivo, as shown by immunohistology. The
constitutive and regulated expression of functional PAF-R by human
intestinal epithelium suggests PAF produced by the intestinal
epithelial cells or cells underlying the epithelium has autocrine or
paracrine effects on intestinal epithelial cells.
colon; colon epithelial cell lines; platelet-activating factor receptor exon 2; small intestine; tyrosine phosphorylation; retinoic acid
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