Sucralose, an activator of the glucose-sensing receptor, increases ATP by calcium-dependent and -independent mechanisms

Sucralose is an artificial sweetener and activates the glucose-sensing receptor expressed in pancreatic β-cells. Although sucralose does not enter β-cells nor acts as a substrate for glucokinase, it induces a marked elevation of intracellular ATP ([ATP]c). The present study was conducted to identify...

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Published inENDOCRINE JOURNAL Vol. 63; no. 8; pp. 715 - 725
Main Authors Li, Longfei, Ohtsu, Yoshiaki, Nakagawa, Yuko, Masuda, Katsuyoshi, Kojima, Itaru
Format Journal Article
LanguageEnglish
Published Japan The Japan Endocrine Society 2016
Subjects
Adenosine Triphosphate - metabolism
Animals
ATP
Calcium
Calcium - metabolism
Calcium - pharmacology
Calcium Signaling - drug effects
Calcium Signaling - physiology
Cells, Cultured
Cyclic AMP - metabolism
Egtazic Acid - analogs & derivatives
Egtazic Acid - pharmacology
Glucose metabolism
Insulin-Secreting Cells - drug effects
Insulin-Secreting Cells - metabolism
Mice
Nifedipine - pharmacology
Sucrose - analogs & derivatives
Sucrose - pharmacology
Sweet taste receptor
Sweetening Agents - pharmacology
β-cell
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Summary:Sucralose is an artificial sweetener and activates the glucose-sensing receptor expressed in pancreatic β-cells. Although sucralose does not enter β-cells nor acts as a substrate for glucokinase, it induces a marked elevation of intracellular ATP ([ATP]c). The present study was conducted to identify the signaling pathway responsible for the elevation of [ATP]c induced by sucralose. Previous studies have shown that sucralose elevates cyclic AMP (cAMP), activates phospholipase C (PLC) and stimulates Ca2+ entry by a Na+-dependent mechanism in MIN6 cells. The addition of forskolin induced a marked elevation of cAMP, whereas it did not affect [ATP]c. Carbachol, an activator of PLC, did not increase [ATP]c. In addition, activation of protein kinase C by dioctanoylglycerol did not affect [ATP]c. In contrast, nifedipine, an inhibitor of the voltage-dependent Ca2+ channel, significantly reduced [ATP]c response to sucralose. Removal of extracellular Na+ nearly completely blocked sucralose-induced elevation of [ATP]c. Stimulation of Na+ entry by adding a Na+ ionophore monensin elevated [ATP]c. The monensin-induced elevation of [ATP]c was only partially inhibited by nifedipine and loading of BAPTA, both of which completely abolished elevation of [Ca2+]c. These results suggest that Na+ entry is critical for the sucralose-induced elevation of [ATP]c. Both calcium-dependent and -independent mechanisms are involved in the action of sucralose.
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ISSN:0918-8959
1348-4540
DOI:10.1507/endocrj.EJ16-0217