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Departments of Physiology, Human Morphology, and Internal Medicine, American University of Beirut, Beirut, Lebanon
It was recently
shown that vasoactive intestinal polypeptide (VIP) inhibits rat jejunal
alanine absorption, an effect that was significantly reduced by
vagotomy. This study assesses the role of capsaicin-sensitive primary
afferents (CSPA) and the myenteric plexus in the inhibition of rat
jejunal alanine absorption by VIP. Continuous intravenous infusion of
VIP (11.2 ng · kg
1 · min
1)
reduced alanine absorption by 60% in sham control rats and by 20% in
rats neonatally treated with capsaicin
(P < 0.01). In in vitro
experiments, VIP decreased alanine uptake by jejunal strips isolated
from sham control rats in a dose-dependent manner. In the presence of
40 nM VIP, alanine uptake by full-thickness jejunal strips was reduced
by 54% in sham control rats and by 25% in rats neonatally treated
with capsaicin (P < 0.001). On the
other hand, VIP reduced alanine uptake by mucosal scrapings by 25% in
sham rats compared with 9% reduction in neonatally treated rats.
Chemical ablation of the extrinsic innervation and jejunal myenteric
plexuses by pretreatment with benzalkonium chloride significantly
(P < 0.001) reduced basal alanine
absorption and the inhibitory effect of VIP. Moreover, incubation of
intestinal strips with tetrodotoxin and atropine reduced significantly
(P < 0.05) the inhibitory effect of
VIP on alanine absorption. These data suggest that VIP exerts its
inhibitory effect on alanine absorption through the CSPA fibers and the
myenteric plexus. The neuronal circuitry of this inhibitory process may
involve cholinergic muscarinic mechanisms.
capsaicin-sensitive primary afferents; myenteric plexus; intestinal absorption
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