Sugar-activated ion transport in canine lingual epithelium. Implications for sugar taste transduction.

Open Access

1 July 1988

journal article
research article
Published by Rockefeller University Press in The Journal of general physiology

Vol. 92 (1) , 87-111
https://doi.org/10.1085/jgp.92.1.87

Abstract

There is good evidence indicating that ion-transport pathways in the apical regions of lingual epithelial cells, including taste bud cells, may play a role in salt taste reception. In this article, we present evidence that, in the case of the dog, there also exists a sugar-activated ion-transport pathway that is linked to sugar taste transduction. Evidence was drawn from two parallel lines of experiments: (a) ion-transport studies on the isolated canine lingual epithelium, and (b) recordings from the canine chorda tympani. The results in vitro showed that both mono- and disaccharides in the mucosal bath stimulate a dose-dependent increase in the short-circuit current over the concentration range coincident with mammalian sugar taste responses. Transepithelial current evoked by glucose, fructose, or sucrose in either 30 mM NaCl or in Krebs-Henseleit buffer (K-H) was partially blocked by amiloride. Among current carriers activated by saccharides, the current response was greater with Na than with K. Ion flux measurements in K-H during stimulation with 3-O-methylglucose showed that the sugar-evoked current was due to an increase in the Na influx. Ouabain or amiloride reduced the sugar-evoked Na influx without effect on sugar transport as measured with tritiated 3-O-methyl-glucose. Amiloride inhibited the canine chorda tympai response to 0.5 M NaCl by 70-80% and the response to 0.5 M KCl by .apprx. 40%. This agreed with the percent inhibition by amiloride of the short-circuit current supported in vitro by NaCl and KCl. Amiloride also partially inhibited the chorda tympani responses to sucrose and to fructose. The results indicate that in the dog: (a) the ion transporter subserving Na taste also subserves part of the response to K, and (b) a sugar-activated, Na-preferring ion-transport system is one mechanism mediating sugar taste transduction. Results in the literature indicate a similar sweet taste mechanism for humans.

This publication has 23 references indexed in Scilit:

Amiloride reduces the taste intensity of Na+ and Li+ salts and sweeteners.
Proceedings of the National Academy of Sciences, 1983
Increases in guinea pig small intestinal transepithelial resistance induced by osmotic loads are accompanied by rapid alterations in absorptive-cell tight-junction structure.
The Journal of cell biology, 1983
Multiple receptor sites mediate sweetness: Evidence from cross adaptation
Pharmacology Biochemistry and Behavior, 1981
Vascular anatomy and tissue osmolality in the filiform and fungiform papillae of the cat's tongue
Acta Physiologica Scandinavica, 1979
Sweet taste of dilute NaCl: Psychophysical evidence for a sweet stimulus
Physiology & Behavior, 1978
Studies on the mechanism of intestinal absorption of sugars VIII. Cation inhibition of active sugar transport and 22Na influx into hamster small intestine, in vitro
Biochimica et Biophysica Acta (BBA) - Biophysics including Photosynthesis, 1965
A Comparison of Neural and Psychophysical Responses to Taste Stimuli in Man
Acta Physiologica Scandinavica, 1965
Ion Transport in Isolated Rabbit Ileum
The Journal of general physiology, 1964
Electrophysiological Investigation of the Gustatory Effect of Various Biological Sugars
Acta Physiologica Scandinavica, 1962
Species Differences in Taste Responses
American Journal of Physiology-Legacy Content, 1955