| Literature DB >> 30400014 |
Eun-Young Lee1, Xilin Zhang1, Junki Miyamoto2, Ikuo Kimura2, Tomoaki Taknaka3, Kenichi Furusawa4, Takahito Jomori4, Kosuke Fujimoto5,6, Satoshi Uematsu5,6, Takashi Miki1.
Abstract
Mechanisms of carbohydrate-induced secretion of the two incretins namely glucagon-like peptide 1 (GLP-1) and glucose-dependent insulinotropic polypeptide (GIP) are considered to be mostly similar. However, we found that mice exhibit opposite secretory responses in response to co-administration of maltose plus an α-glucosidase inhibitor miglitol (maltose/miglitol), stimulatory for GLP-1, as reported previously, but inhibitory for GIP. Gut microbiota was shown to be involved in maltose/miglitol-induced GIP suppression, as the suppression was attenuated in antibiotics (Abs)-treated mice and abolished in germ-free mice. In addition, maltose/miglitol administration increased plasma levels of short-chain fatty acids (SCFAs), carbohydrate-derived metabolites, in the portal vein. GIP suppression by maltose/miglitol was not observed in mice lacking a SCFA receptor Ffar3, but it was normally seen in Ffar2-deficient mice. Similar to maltose/miglitol administration, co-administration of glucose plus a sodium glucose transporter inhibitor phloridzin (glucose/phloridzin) induced GIP suppression, which was again cancelled by Abs treatment. In conclusion, oral administration of carbohydrates with α-glucosidase inhibitors suppresses GIP secretion through a microbiota/SCFA/FFAR3 pathway.Entities:
Keywords: FFAR3; GIP secretion; SCFA (short chain fatty acid); microbiota; α-glucosidase
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Year: 2018 PMID: 30400014 DOI: 10.1530/JOE-18-0241
Source DB: PubMed Journal: J Endocrinol ISSN: 0022-0795 Impact factor: 4.286