The effects of VIP on intestinal motility study onex vivo perfused isolated canine jejunal loops

Kachelhoffer, J; Mendel, Carl M.; Dauchel, J; Hohmatter, D.; Grenier, J F

doi:10.1007/bf01071907

Cited by 43 publications

(10 citation statements)

References 18 publications

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“…These alterations took place within about 5 min. Thereafter, motility recurred to normal patterns despite ongoing VIP infusion (23). Consequently, protracted VIP infusion over several hours might have obscured an initial inhibitory effect in our experiments and we may have missed potential effects of short-lasting VIP infusion on human small intestinal motility.…”

Section: Effects Of Increased Vip Plasma Levels On Human Small Intestcontrasting

confidence: 49%

“…In vivo studies investigating the effect of VIP infusion on human gastrointestinal motility are lacking, so far, but there are several studies performed in rats, dogs, and pigs which have yielded conflicting results: disruption of the migrating motor complex (19,20), reduction of antral and duodenal motility (15)(16)(17)(18)22) or even induction of motor quiescence (19,20), shortening of small intestinal MMC interval (22), and retardation of small intestinal transit (21) have been observed in response to high doses of VIP. However, there are also several studies failing to show (major) effects of VIP infusion on gastrointestinal motility (4,18,22,23). Using isolated muscle preparations from various regions of the gastrointestinal tract in pigs, Mandrek and Milenov demonstrated that VIP potently inhibits tonic contractions of the duodenal circular muscle layer but has no effect on the contractility of the longitudinal muscle layer (29).…”

Section: Vip and Gastrointestinal Motilitymentioning

confidence: 96%

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Do Elevated Plasma Vasoactive Intestinal Polypeptide (VIP) Levels Cause Small Intestinal Motor Disturbances in Humans?

et al. 2005

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Increased VIP plasma levels cause severe secretory diarrhea. Moreover, VIP is a major regulator of human intestinal motility. We hypothesized that VIP-mediated intestinal motility disturbances contribute to symptoms in elevated plasma VIP. Ten healthy volunteers were intubated twice with an orojejunal multilumen tube for duodenal manometry, jejunal perfusion of electrolyte and marker solution, and aspiration 10 and 40 cm more distally. All subjects randomly received intravenous infusion of saline and 300 pmol/kg x hr VIP for 5 hr. Results showed that VIP but not saline infusion induced netjejunal sodium secretion, watery diarrhea, and cardiovascular effects (P < 0.04). VIP did not alter intestinal motor activity or the mean duration of the interdigestive motility cycle or of phases I and II but nearly halved the duration of phase III (P = 0.0002). We conclude that increased plasma VIP markedly shortens human phase III activity without influencing other motility parameters. Hence, it is unlikely that VIP-mediated small intestinal motor disturbances cause symptoms in VIPOMA. Yet VIP may contribute to terminate phase III motility.

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Section: Effects Of Increased Vip Plasma Levels On Human Small Intestcontrasting

confidence: 49%

Section: Vip and Gastrointestinal Motilitymentioning

confidence: 96%

Do Elevated Plasma Vasoactive Intestinal Polypeptide (VIP) Levels Cause Small Intestinal Motor Disturbances in Humans?

et al. 2005

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“…An excitatory effect of VIP has been reported in the small intestine (Kachelhoffer et al 1976, Cohen & Landry 1980 and bladder (Johns 1979). Some of these results may have been caused by contamination of the VIP with histamine (Said & Mutt 1970).…”

Section: Discussionmentioning

confidence: 99%

“…Some of these results may have been caused by contamination of the VIP with histamine (Said & Mutt 1970). or by the stimulation of cholinergic (Cohen & Landry 1980) or non-cholinergic excitatory fibers (Kachelhoffer et al 1976). In order to evaluate the involvement of other receptors the effect of VIP was investigated in the presence of the muscarinic receptor blocker, atropine, the aand P-adrenergic blocking agents, (phentolamine, propranolol).…”

Section: Discussionmentioning

confidence: 99%

Vasoactive intestinal polypeptide (VIP): Effect on rabbit uterine smooth muscle in vivo and in vitro

Ottesen

1981

Acta Physiologica Scandinavica

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The effect of vasoactive intestinal polypeptide (VIP) on uterine smooth muscle electrical and mechanical activity in non-pregnant estradiol-treated rabbits was investigated using in vivo and in vitro methods. The studies were performed on spontaneous, oxytocin-, carbachol-, and prostaglandin-42 alpha-induced activity. VIP had a dose-related inhibitory effect on both myoelectrical and mechanical activity. The concentration needed for 50% inhibition (ID50) was 2 x 10(-10) mol VIP . 1(-1) (in vivo), an 6 x 10(-8) mol VIP . 1(-1) (in vitro). This inhibition was unaffected by the presence of atropine (10(-5) mol . 1(-1)), propranolol (10(-5)), phentolamine (10(-5)), naloxone (10(-5)), apamin (10(-5)), and tetrodotoxin (10(-5)). These findings indicate that VIP may act via a specific receptor on the smooth muscle and supports the hypothesis that VIP may be a neurotransmitter involved in the local nervous control of uterine smooth muscle activity.

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“…VIP is known to have powerful relaxant effects on many smooth muscles, including that of the gastrointestinal tract (Piper, Said & Vane, 1970;Kachelhoffer, Mendel, Dauchel, Hohmatter & Grenier, 1976), and it has been suggested that the peptide serves an important functional role as an inhibitory neurotransmitter (Fahrenkrug, Haglund, Jodal, Lundgren, Olbe & Schaffalitzky de Muckadell, 1978;. A long-standing, unanswered question concerns the identity of the final mediator of the descending inhibitory component of the peristaltic reflex (Hirst & McKirdy, 1974).…”

Section: Introductionmentioning

confidence: 99%

Electrophysiology and morphology of vasoactive‐intestinal‐peptide‐immunoreactive neurones of the guinea‐pig ileum.

Katayama¹,

Lees²,

Pearson³

1986

The Journal of Physiology

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Simultaneous intracellular staining and electrophysiological recording techniques have been applied to neurones of guinea-pig myenteric plexus-longitudinal muscle preparations. With micro-electrodes filled with a solution of the fluorescent dye Lucifer Yellow, neurones were first characterized morphologically and electrophysiologically, and subsequently subjected to an indirect immunohistochemical method for the detection of vasoactive intestinal peptide (VIP)-like immunoreactivity. Cross-correlations of morphology, electrophysiology and VIP immunoreactivity were successfully achieved in a total of 164 neurones. Sixty-three had the slow after-hyperpolarization characteristic of AH neurones; 101 cells displayed fast excitatory post-synaptic potentials (e.p.s.p.s) in response to transmural or focal stimulation and were therefore, by definition, S neurones. Unequivocal VIP immunoreactivity was observed in 25 (25%) S neurones, which, with only one exception, had Dogiel Type I morphology (i.e. many short soma processes and a single long process). In contrast, AH neurones had Dogiel Type II morphology (i.e. smooth soma with several long processes) and none showed VIP immunoreactivity. In addition to cholinergic fast e.p.s.p.s., non-cholinergic slow synaptic inputs were evoked in seventeen of the twenty-two VIP-immunoreactive S neurones tested. Both the fast and slow e.p.s.p.s could be elicited by stimulation of the preparation, oral or aboral to the site of recording. These observations demonstrate that, in the guinea-pig ileum, myenteric plexus neurones showing VIP immunoreactivity are of a single electrophysiological type (S neurones) and belong to essentially one morphological class (Dogiel Type I).

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The effects of VIP on intestinal motility study onex vivo perfused isolated canine jejunal loops

Cited by 43 publications

References 18 publications

Do Elevated Plasma Vasoactive Intestinal Polypeptide (VIP) Levels Cause Small Intestinal Motor Disturbances in Humans?

Do Elevated Plasma Vasoactive Intestinal Polypeptide (VIP) Levels Cause Small Intestinal Motor Disturbances in Humans?

Vasoactive intestinal polypeptide (VIP): Effect on rabbit uterine smooth muscle in vivo and in vitro

Electrophysiology and morphology of vasoactive‐intestinal‐peptide‐immunoreactive neurones of the guinea‐pig ileum.

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