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Vol. 299, Issue 3, 915-920, December 2001
B, Attenuates Bacterial Peptidoglycan Polysaccharide-Induced
Colitis in Rats
GI Inflammation Laboratory, Otsuka Maryland Research Institute,
Rockville, Maryland
Caffeic acid phenethyl ester (CAPE) is an anti-inflammatory component
of propolis (honeybee resin). CAPE is reportedly a specific inhibitor
of nuclear factor-
B (NF-
B). The aims of our study were 1) to
evaluate the effect of CAPE on cytokine production, NF-
B, and
apoptosis in two cell lines; 2) to assess the effect of CAPE on NF-
B
in rats with peptidoglycan-polysaccharide (PG-PS)-induced colitis; and
3) to evaluate the efficacy of CAPE against this colitis. In vitro
experiments used rat macrophage (NR8383) and colonic epithelial cell
(SW620) lines. NF-
B was evaluated by electrophoretic mobility shift
assay. Cytokines and apoptosis were measured by enzyme-linked
immunosorbent assay. Colitis was induced by intramural
injections of PG-PS into the distal colon. CAPE (30 mg/kg) or vehicle
was administered once daily to rats by intraperitoneal injection, for 1 week. Various macroscopic and biochemical indices were measured on day
21. CAPE (30 µg/ml) significantly inhibited NF-
B and TNF-
production in the macrophage cell line. In macrophages, CAPE
significantly increased DNA fragmentation. CAPE exhibited generally
similar effects in the colonic epithelial cell line. CAPE treatment
reduced the mean level of colonic NF-
B in rats. CAPE also induced a
significant reduction in gross colonic injury. Moreover, colonic
cytokine levels (TNF-
and IL-1
) were significantly reduced in
CAPE-treated rats. In summary, CAPE inhibits NF-
B, causes a
reduction of pro-inflammatory cytokine production, and induces
apoptosis in macrophages. These mechanisms likely contributed to the
attenuation of PG-PS-induced colitis by CAPE.
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