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SGLT6 - A pharmacological target for the treatment of obesity?


ABSTRACT: Despite increased knowledge of nutrient intake regulation and energy homeostasis, treatment options for obesity remain limited. Food reward consists of two branches: gustatory and post-ingestive nutritive information. Drosophila lacking dSLC5A11 (sodium/glucose cotransporter 6-SGLT6) prefer L-glucose over D-glucose independently of their state of satiety. Human SGLT6 is an active transporter of myo-inositol and D-glucose. We investigated expression of SGLT6 in human tissue and found a significant expression in the small intestine and brain. The preference between a metabolizable and a non-metabolizable sugar was tested in 3 mouse models with a selective and potent SGLT6 inhibitor. No influence on sugar preference was seen with SGLT6 inhibition. These studies suggest that SGLT6 does not play a significant role in nutrient sensing in mammals.

SUBMITTER: Baader-Pagler T 

PROVIDER: S-EPMC6768193 | biostudies-literature | 2018

REPOSITORIES: biostudies-literature

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SGLT6 - A pharmacological target for the treatment of obesity?

Baader-Pagler Tamara T   Eckhardt Matthias M   Himmelsbach Frank F   Sauer Achim A   Stierstorfer Birgit E BE   Hamilton Bradford S BS  

Adipocyte 20181011 4


Despite increased knowledge of nutrient intake regulation and energy homeostasis, treatment options for obesity remain limited. Food reward consists of two branches: gustatory and post-ingestive nutritive information. Drosophila lacking dSLC5A11 (sodium/glucose cotransporter 6-SGLT6) prefer L-glucose over D-glucose independently of their state of satiety. Human SGLT6 is an active transporter of myo-inositol and D-glucose. We investigated expression of SGLT6 in human tissue and found a significan  ...[more]

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