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secretion
Department of Medicine, University of Illinois and Chicago Veterans Affairs Medical Center, West Side Division, Chicago, Illinois 60612
Galanin is a peptide hormone widely expressed in
the central nervous system and gastrointestinal (GI) tract. Within the
GI tract galanin is present in enteric nerve terminals where it is known to modulate intestinal motility by altering smooth muscle contraction. Recent studies also show that galanin can alter intestinal short-circuit current
(Isc) but with
differing results observed in rats, rabbits, guinea pigs, and pigs. In
contrast, nothing is known about the ability of galanin to alter ion
transport in human intestinal epithelial tissues. By RT-PCR, we
determined that these tissues express only the galanin-1 receptor
(Gal1-R) subtype. To evaluate Gal1-R pharmacology and physiology, we
studied T84 cells. Gal1-R expressed by these cells bound galanin
rapidly (half time 1-2 min) and with high affinity (inhibitor
constant 0.7 ± 0.2 nM). T84 cells were then studied in
a modified Ussing chamber and alterations in
Isc, a measure of
all ion movement across the tissue, were determined. Maximal increases
in Isc were observed in a concentration-dependent manner around 2 min after stimulation with peptide, with 1 µM galanin causing
Isc to rise more
than eightfold and return to baseline occurring within 10 min. The
increase in galanin-induced
Isc was shown by
125I efflux studies to be due to
Cl
secretion, which
occurred independently of alterations in cAMP and phospholipase C. Rather, Cl
secretion is
mediated via a Ca2+-dependent,
pertussis toxin-sensitive mechanism. These data suggest that galanin
released by enteric nerves may act as a secretagogue in the human colon
by activating Gal1-R.
diarrhea; pharmacology
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