Original Article
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World J Gastroenterol. Feb 14, 2013; 19(6): 846-854
Published online Feb 14, 2013. doi: 10.3748/wjg.v19.i6.846
Accommodation and peristalsis are functional responses to obstruction in rat hypertrophic ileum
Simona Bertoni, Francesca Saccani, Rita Gatti, Alberto Rapalli, Lisa Flammini, Vigilio Ballabeni, Elisabetta Barocelli
Simona Bertoni, Francesca Saccani, Alberto Rapalli, Lisa Flammini, Vigilio Ballabeni, Elisabetta Barocelli, Department of Pharmacological, Biological and Applied Chemical Sciences, University of Parma, 43124 Parma, Italy
Rita Gatti, Department of Experimental Medicine, University of Parma, 43125 Parma, Italy
Author contributions: Bertoni S performed the research and wrote the paper; Saccani F and Gatti R performed the immunohistochemistry studies; Rapalli A and Flammini L performed the functional studies; Ballabeni V analyzed the data; Barocelli E designed the research study and wrote the paper.
Correspondence to: Dr. Simona Bertoni, Department of Pharmacological, Biological and Applied Chemical Sciences, University of Parma, Parco Area delle Scienze 27/a, 43124 Parma, Italy. simona.bertoni@unipr.it
Telephone: +39-521-905090 Fax: +39-521-905091
Received: July 4, 2012
Revised: September 13, 2012
Accepted: September 22, 2012
Published online: February 14, 2013
Abstract

AIM: To investigate the effects of chronic obstruction on enteric reflexes evoked by electrical stimulation (EFS) or intraluminal distension of the rat hypertrophic ileum.

METHODS: Motor responses to EFS and to intraluminal distension were studied in the absence and in the presence of various inhibitors of enteric mediators. Ileum segments from operated (chronic ileal obstruction), sham-operated (control) and normal rats were horizontally mounted, connected to a pressure transducer and intraluminally perfused. The effects of selective serotonin receptor (5-HTR) blockers were investigated on distension-induced responses. The cellular localization of 5-HT3Rs was also examined in control and hypertrophic tissues through confocal microscopy.

RESULTS: In non-obstructed segments, EFS elicited tetrodotoxin (TTX)-sensitive responses with high amplitude contraction followed by weak relaxation. In hypertrophic tissues, EFS lowered the baseline pressure and evoked TTX-sensitive contractions significantly larger than normal (P < 0.01) or control (P < 0.05), and devoid of any relaxation phase (P < 0.01 vs normal). Incubation with atropine and guanethidine [non-adrenergic non-cholinergic (NANC) conditions] did not modify intestinal tone in normal and control preparations, but reversed the accommodation produced by EFS in hypertrophic tissues, and depressed the amplitude of contractions in all types of tissues. L-NAME and α-chymotrypsin blocked residual NANC motility in all tissues and augmented intraluminal pressure in hypertrophic segments (P < 0.05 vs NANC conditions). Intraluminal distension of the intestinal wall evoked non-propulsive cycles of contractions and relaxations in non-obstructed tissues. In all hypertrophic segments, strong propulsive strokes, markedly wider (P < 0.001), and larger than normal (P < 0.001) or control (P < 0.05) were elicited. Both motor patterns were blocked under NANC conditions and with simultaneous incubation with L-NAME and α-chymotrypsin. In all types of tissues, incubation with ketanserin or GR125487 did not modify distension-induced motility. In contrast, blockade of 5-HT3Rs by ondansetron concentration-dependently inhibited motor responses in normal and control tissues, but only slightly impaired enteric reflexes in the hypertrophic preparations. Finally, confocal microscopy did not reveal a different cellular distribution of 5-HT3Rs in control and hypertrophic ileum.

CONCLUSION: Accommodation and distension-induced peristalsis of rat hypertrophic ileum are controlled by cholinergic and peptidergic transmission and are negligibly affected by 5-HT3Rs, which modulate distension-induced motility in non-obstructed tissues.

Keywords: 5-HT3 receptor, Intestinal obstruction, Peristalsis, Rat intestinal motility, Serotonin