Substance P: a potent inhibitor of the canine small intestine in vivo
- 1 January 1986
- journal article
- research article
- Published by American Physiological Society in American Journal of Physiology-Gastrointestinal and Liver Physiology
- Vol. 250 (1) , G21-G27
- https://doi.org/10.1152/ajpgi.1986.250.1.g21
Abstract
Intraarterially administration substance P inhibited neurally activated contractions of the circular muscle of canine small intestine in vivo (lowest effective dose .apprx. 10-13 mol). Excitation of intestine required higher (10-10 mol) doses. The inhibitory effect required functioning nerves, since tetrodotoxin treatment eliminated it. However, inhibition of neurogenic contraction by substance P was unaffected by nicotinic or opiate receptor antagonists or by catecholamine depletion but was reduced by a selective substance P antagonist. Since the inhibition by substance P was also greatly reduced by treatment with atropine or pirenzepine and acetylcholine given intra-arterially produced a similar inhibitory response, stimulation of release of acetylcholine to inhibitory muscarinic receptors on nerves appeared to be the mechanism of this action. Direct smooth muscle effects were ruled out; substance P did not inhibit contractions in intraarterial acetylcholine or those following tetrodotoxin. In vitro in ileal strips, no inhibition by substance P of any contractile response was found. We propose that the local release of substance P into the myenteric plexus produces inhibition and suggest that this constitutes a physiological function of the neuropeptide. This action may be absent in vitro.This publication has 15 references indexed in Scilit:
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