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,
Departments of
*
Pediatrics and
Immunology, and
Barbara Davis Childhood Diabetes Center, University of Colorado School of Medicine, Denver, CO 80262
Dendritic cells from the mesenteric lymph nodes (MLN) contain dense
esterase-positive inclusions that may originate in effete intestinal
epithelial cells and reach MLN without degradation. The MLN esterases
have the electrophoretic mobilities of both intestinal and mononuclear
cells. Cryptosporidium parvum
(CP)-infected mice have CP Ag-positive cells in MLN and also increased
numbers of dense esterase-positive cells, but the CP Ag-positive cells
do not stain for esterase. To characterize the handling of epithelial
cell products by dendritic cells, we analyzed mRNAs in the MLN of
control and CP-infected recombination-activating
gene-/-DO11.10 mice by oligoarrays. mRNAs for 115
proteins were increased in MLN after CP infection, of which the
principal increases in trypsin and chymotrypsin approximated to
250-fold. Colipase, reg-1, C-reactive protein-ductin, and
amyloid were also up-regulated >10-fold and all returned to baseline
by 28 days after infection. mRNAs for the same proteins were detected
in intestinal epithelial cells of infected mice by oligoarrays and
RT-PCR after infection. mRNA for CP 
-tubulin was detectable in
intestinal epithelial cells between 5 and 18 days after infection but
was not detected in the MLN throughout the observation period. It
appears that host response to CP infection includes expression of mRNA
for some pancreatic enzymes by intestinal epithelial cells and their
subsequent transport to the MLN. The esterase and trypsin, and mRNAs
for chymotrypsin, colipase, and others that may derive from uninfected
epithelial cells, appear to be transported to the MLN intact, while
mRNA for CP -tubulin that is derived from infected cells is
degraded.
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