Cholinergic regulation of epithelial ion transport in the mammalian intestine

Open Access

1 November 2006

journal article
review article
Published by Wiley in British Journal of Pharmacology

Vol. 149 (5) , 463-479
https://doi.org/10.1038/sj.bjp.0706889

Abstract

Acetylcholine (ACh) is critical in controlling epithelial ion transport and hence water movements for gut hydration. Here we review the mechanism of cholinergic control of epithelial ion transport across the mammalian intestine. The cholinergic nervous system affects basal ion flux and can evoke increased active ion transport events. Most studies rely on measuring increases in short‐circuit current (I_SC= active ion transport) evoked by adding ACh or cholinomimetics to intestinal tissue mounted in Ussing chambers. Despite subtle species and gut regional differences, most data indicate that, under normal circumstances, the effect of ACh on intestinal ion transport is mainly an increase in Cl^‐secretion due to interaction with epithelial M₃muscarinic ACh receptors (mAChRs) and, to a lesser extent, neuronal M₁mAChRs; however, AChR pharmacology has been plagued by a lack of good receptor subtype‐selective compounds. Mice lacking M₃mAChRs display intact cholinergically‐mediated intestinal ion transport, suggesting a possible compensatory mechanism. Inflamed tissues often display perturbations in the enteric cholinergic system and reduced intestinal ion transport responses to cholinomimetics. The mechanism(s) underlying this hyporesponsiveness are not fully defined. Inflammation‐evoked loss of mAChR‐mediated control of epithelial ion transport in the mouse reveals a role for neuronal nicotinic AChRs, representing a hitherto unappreciated braking system to limit ACh‐evoked Cl^‐secretion. We suggest that: i) pharmacological analyses should be supported by the use of more selective compounds and supplemented with molecular biology techniques targeting specific ACh receptors and signalling molecules, and ii) assessment of ion transport in normal tissue must be complemented with investigations of tissues from patients or animals with intestinal disease to reveal control mechanisms that may go undetected by focusing on healthy tissue only.British Journal of Pharmacology(2006)149, 463–479. doi:10.1038/sj.bjp.0706889

Keywords

This publication has 226 references indexed in Scilit:

Disturbances in epithelial ionic secretion in different experimental models of colitis
Life Sciences, 2005
From structure to disease: the evolving tale of aquaporin biology
Nature Reviews Molecular Cell Biology, 2004
Aquaporins in the digestive system
Medical Molecular Morphology, 2004
Nicotinic acetylcholine receptor α7 subunit is an essential regulator of inflammation
Nature, 2002
Immunological localization of m1–m5 muscarinic acetylcholine receptors in peripheral tissues and brain
Published by Elsevier ,2002
The identification and chemical coding of cholinergic neurons in the small and large intestine of the mouse
The Anatomical Record, 1998
Immunohistochemical localization of nicotinic acetylcholine receptors in the guinea pig bowel and pancreas
Journal of Comparative Neurology, 1998
Affinities of muscarinic drugs for [3H]N-methylscopolamine (NMS) and [3H]oxotremorine (OXO) binding to a mixture of M1−M4 muscarinic receptors: Use of NMS/OXO-M ratios to group compounds into potential agonist, partial agonist, and antagonist classes
Neurochemical Research, 1995
Epithelial and mucosal preparations of canine proximal colon in ussing chambers: Comparison of responses
Life Sciences, 1986
Electrical activity of an intestinal epithelial cell line: Hyperpolarizing responses to intestinal secretagogues
The Journal of Membrane Biology, 1984